EPIGENETIC METHODS AND NUCLEIC ACIDS FOR THE DETECTION OF BREAST CELL PROLIFERATIVE DISORDERS

Abstract

The present application provides methods and nucleic acids for the detection and differentiation of breast cell proliferative disorders. This is achieved by the analysis of the methylation of a panel of genes, or subsets thereof. The invention may be used for the detection and/or differentiation of a variety of tissue types including breast cancer and benign breast disorders as well as other cancers and tissue types.

Description

FIELD OF THE INVENTION

The present invention relates to genomic DNA sequences that exhibit altered CpG methylation patterns in disease states relative to normal. Particular embodiments provide methods, nucleic acids, nucleic acid arrays and kits useful for detecting, or for detecting and differentiating between or among breast cell proliferative disorders.

BACKGROUND

The etiology of pathogenic states is known to involve modified methylation patterns of individual genes or of the genome. 5-methylcytosine, in the context of CpG dinucleotide sequences, is the most frequent covalently modified base in the DNA of eukaryotic cells, and plays a role in the regulation of transcription, genetic imprinting, and tumorigenesis. The identification and quantification of 5-methylcytosine sites in a specific specimen, or between or among a plurality of specimens, is thus of considerable interest, not only in research, but particularly for the molecular diagnoses of various diseases.

Correlation of aberrant DNA methylation with cancer. Aberrant DNA methylation within CpG ‘islands’ is characterized by hyper- or hypomethylation of CpG dinucleotide sequences leading to abrogation or over-expression of a broad spectrum of genes, and is among the earliest and most common alterations found in, and correlated with human malignancies. Additionally, abnormal methylation has been shown to occur in CpG-rich regulatory elements in intronic and coding parts of genes for certain tumors. In colon cancer, for example, aberrant DNA methylation constitutes one of the most prominent alterations and inactivates many tumor suppressor genes such as p14ARF, p161INK4a, THBS1, MINT2, and MINT31 and DNA mismatch repair genes such as hMLH1.

In contrast to the specific hypermethylation of tumor suppressor genes, an overall hypomethylation of DNA can be observed in tumor cells. This decrease in global methylation can be detected early, far before the development of frank tumor formation. A correlation between hypomethylation and increased gene expression has been determined for many oncogenes.

Breast cancer. In American women, breast cancer is the most frequently diagnosed cancer. 1 out of 8 women will develop breast cancer during her life time. Breast cancer is the second leading cause of cancer death and in women aged 40-55, breast cancer is the leading cause of death. For 2004, 215990 new cases of breast cancer and 40110 deaths are estimated in the US alone with comparable numbers in Europe.

Breast Cancer Classification.

1. Breast Cancer

The vast majority of breast neoplasms are of epithelial origin with ductal carcinomas representing 80% of all tumors. In addition, there are several breast cancer subtypes that are less common. Medullary and lobular carcinomas are both found in about 5% of patients diagnosed with breast cancer. Other less frequent tumor histologies include pure tubular carcinoma, mucinous or colloid carcinoma, papillary carcinoma, and Paget's disease. These cancers have substantially better prognoses, especially when found in a node-negative stage. Carcinocarcinomas and adenocystic tumors occur only sporadically.

Ductal carcinoma in-situ (DCIS) is a noninvasive, precancerous condition, DCIS can progress to become invasive cancer, but estimates of the likelihood of this vary widely. Some people include DOS in breast cancer statistics. The frequency of the diagnosis of DCIS has increased markedly in the United States since the widespread use of screening mammography. In 1998, DCIS accounted for about 18% of all newly-diagnosed invasive plus noninvasive breast tumors in the United States. Very few cases of DCIS present as a palpable mass; 80% are diagnosed by mammography alone.

2. Benign Breast Conditions

The most common benign breast conditions include fibrocystic breast condition, benign breast tumors, and breast inflammation. Fibrocystic disease is the most frequent benign breast condition affecting every second woman at least once during her life time. Symptoms of fibrocystic breasts in the breast include cysts (accumulated packets of fluid), fibrosis (formation of scar-like connective tissue), lumpiness, areas of thickening, tenderness, or breast pain. Fibrocystic breasts can sometimes make breast cancer more difficult to detect with mammography.

Fibroadenomas are common benign breast tumors often too small to feel by hand, though occasionally, they may grow to be several inches in diameter. Fibroadenomas are made up of both glandular and stromal (connective) breast tissue and usually occur in women between 20-30 years of age. According to the American Cancer Society, African-American women are affected with fibroadenomas more often than women of other racial or ethnic groups. Phyllodes tumors are also benign breast tumors in the glandular and stroma breast tissues but are far less common than fibroadenomas. The difference between phyllodes tumors and fibroadenomas is that there is an overgrowth of the fibro-connective tissue in phyllodes tumors. Phyllodes tumors are usually benign but on very rare occasions, they may be malignant (cancerous) and could metastasize. Granular cell tumors are usually found in the mouth or skin but may rarely be detected in the breast as well. However, granular cell tumors do not indicate higher risk for developing breast cancer. Mastitis is an inflammation of breast tissue that commonly occurs during breast feeding.

TNM Stage

The TNM classification was devised by the International Union Against Cancer (UICC) and accepted by the American Joint Commission on Cancer Staging. TNM is based on the clinical features of tumor (T), the regional lymph nodes (N), and the presence or absence of distant metastases (M). The tumor is characterized by its size, so that a T1 is a tumor under 2 cm, a T2 is 2 to 5 cm, and a T3 is over 5 cm. Breast carcinomas in-situ are labeled Tis and distinguished in ductal carcinoma in-situ (DCIS), lobular carcinoma in-situ (LCIS) and Paget's disease. Similarly, N0 represents negative or normal regional lymph nodes and M0 absence of distant metastases, respectively. Involvement of the ipsilateral axillary lymph nodes is the most reliable and reproducible prognostic indicator for primary breast cancer. In general, 50 to 70% of patients with positive lymph nodes have a relapse, whereas only 20 to 35% of patients with all lymph nodes negative for metastatic disease have a relapse after loco-regional treatments only.

Grade

Tumor grade reflects the differentiation status of the tumor. Breast cancer differentiation is usually described as well (grade 1), moderately (grade 2) or poorly (grade 3) differentiated, respectively. Poorly differentiated tumors tend to be more aggressive. Eighty-six percent of patients having tumors of good nuclear grade survived for 8 years as opposed to 64% in whom the nuclear grade was scored as poor.

Hormone Receptor Status

Hormone receptor levels are important parameters to classify breast cancer both with respect to prognosis as well as for treatment planning. Patients with ER-positive tumor tend to have a more indolent course and to metastasize preferentially to soft tissue and bone; conversely, those with ER-negative tumors relapse earlier, and metastases to liver, lung, and central nervous system are more likely. ER-positive tumors are more often well differentiated and are associated with other favorable prognostic characteristics. Although patients with ER-positive tumors tend to have better short-term disease-free and overall survival rates than do patients with ER-negative tumors, the differences between the two groups tend to diminish or even disappear with time. PsR appeared in some studies to be a more valuable prognostic indicator than the ER. In addition, high levels of estrogen receptor expression are predictors of a favorable response to endocrine therapy.

Age and Menopausal Status

A large study with long follow-up indicated that women 45 to 49 years of age had the best prognosis and that the very young (those under age 35 years) or elderly patients had the worst breast cancer survival. However, when other, more important tumor characteristics are considered, age and menopausal status are not important prognostic indicators.

Diagnosis and Treatment.

Diagnosis

Breast cancer is often diagnosed as a palpable mass by self examination of the patient or during a clinical breast examination by a physician. The increasing use of mammography in breast cancer screening has resulted in many cancers being found already in a stage where no palpable mass is detectable. Suspicious masses are usually followed up by further imaging such as ultra sound or MRI and definitive diagnosis is confirmed by needle biopsy.

Screening

The American Cancer Society currently recommends the following guidelines for the detection of breast cancer in women who are asymptomatic:

• • Women 20 years of age and older should perform breast self-examination (BSE) every month.
  • Women 20-39 should have a physical examination of the breast (CBE or clinical breast exam) at least every three years, performed by health care professional such as a physician, physician assistant, nurse or nurse practitioner. CBE may often be received in the same appointment as a Pap smear.
  • Women 20-39 should also perform monthly BSE.
  • Women 40 and older should have a physical examination of the breast (CBE or clinical breast exam) every year, performed by a health care professional, such as a physician, physician assistant, nurse or nurse practitioner. CBE can often be performed in the same visit as a mammogram. Monthly BSE should also be performed.
  • Women 40 years of age and older should have a screening mammogram every year in addition to annual CBE and monthly BSE.

3. Breast Self Examination (BSE) and Clinical Breast Examination (CBE)

In 2001, new analyses were conducted for clinical breast exam and breast self-exam. There is no direct, but some indirect, evidence that CBE decreases breast cancer mortality. CBE has an overall sensitivity of 54%, which varies with the patient's age and size of the mass, as well as the provider's skill in clinical examination. In the absence of direct evidence, the recommendation for CBE was based on consensus opinion. Regarding breast self exam, a meta-analysis of 6 large controlled trials found no reduction in the relative risk of mortality in women performing BSE vs. those not performing BSE (0.94, 95% C.I. 0.83-1.06). Recently it was further questioned whether routine BSE reduces breast cancer mortality and might even harm. Despite this evidence breast self examination (BSE) and clinical breast examination (CBE) are both still part of the current guidelines for breast cancer screening.

4. Mammography

Mammography is currently the only exam approved by the U.S. Food and Drug Administration (FDA) to screen for breast cancer in asymptomatic women. Randomly controlled trials conducted in the US and several European countries have demonstrated that routine mammography screening can reduce breast cancer mortality by 20-40% if performed annually. On average the sensitivity of mammography is up to 85%. However, mammography is less sensitive in patients with dense breast or benign breast conditions such as fibrocystic changes or lumps. Five to 10 percent of screening mammogram results are abnormal and require more testing. False positive rates are higher in younger women due to higher density of their breasts.

In the US, mammography screening has been established for the general population. Although mammography involves low dose radiation and discomfort to the tested person, the compliance rate is around 70%. The average charge for screening mammography is $141, $101 technical, $40 for interpretation. Despite the obvious success of mammography, growing difficulty has been reported to recruit trained staff; both doctors and nurses, for mammography clinics resulting in a 8% decline of sites over the last 4 years. It was speculated that this might be due to long hours, low reimbursement, heavy regulation and fear of lawsuits.

5. MRI screening

MRI imaging is mainly used to follow up positive mammography results. MRI is very sensitive, is well suited to analyze dense breasts and younger women, but is slower, more expensive, and is more difficult to guide breast biopsies. Currently, trials are ongoing to assess MRI for screening in high risk populations such as carriers of breast cancer susceptibility gene mutations

Breast Cancer Therapy.

Due to current screening programs and the accessibility to self-examination, breast cancer is diagnosed comparatively early: in about 65% of all newly diagnosed cases, the cancer is limited to the breast and has not yet spread to the lymph nodes. Therefore, for most patients diagnosed with organ confined breast cancer the suggested primary therapeutic intervention is surgery often followed by radiation therapy.

Although the tumor can be completely removed by surgery in most early stage breast cancer patients. However, without further therapy, about one third of these will develop metastases during follow-up. It is thought that this is due to occult metastases (or micrometastases) already present at the time of surgery. Based on this observation, systemic adjuvant treatment has been introduced also for node-negative breast cancers. Systemic adjuvant therapy is administered after surgical removal of the tumor, and has been shown to reduce the risk of recurrence significantly (Early Breast Cancer Trialists' Collaborative Group, 1998). Several types of adjuvant treatment are available: endocrine treatment (for hormone receptor positive tumors), different chemotherapy regimens, and novel agents like Herceptin. The treatment regimen for the individual patient is chosen according to guidelines such as St. Gallen or NIH which are based on the pathological classification of the tumor (mainly TNM, grade, ER status).

Based on figures from the American Cancer Society, the prognosis of breast cancer is dearly correlated with cancer stage. The earlier a tumor is detected the better the prognosis for survival. Therefore, breast cancer screening tests that detect cancer at an early result in a reduction of breast cancer mortality.

Methylation and Breast Cancer.

Epigenetic regulation such as DNA methylation has been established as a frequent and early event in carcinogenesis In particular for breast cancer, the contribution of DNA methylation has been well documented. Widscbwendter and Jones (.Oncogene. 2002 Aug. 12; 21(35):5462-82.) demonstrated in a recent review that DNA methylation changes have been reported in the context of all relevant steps in breast carcinogenesis including 1) evasion of apoptosis, 2) insensitivity to antigrowth signals, 3) self-sufficiency in growth signals, 4) limitless replicative potential, 5) tissue invasion and metastasis and 6) sustained angiogenesis. Less well documented is the role of DNA methylation in early pre cancerous lesions such as DCIS and in less frequent cancerous lesions such as lobular carcinoma. Fackler et al. showed that 95% of DCIS lesions (N=44) showed hypermethylation of at least one out or 5 genes including RASSF1A, HIN-1, RAR-beta, Cyclin D2 and Twist. The same authors compared frequency of hypermethylation of these genes between ductal and lobular carcinomas and found similar methylation patterns except for TWIST which was found less hypermethylated in lobular carcinomas. Similarly, Lehmann et al. reported very early stage changes in methylation of both RASSF1A and stratifin and found more frequent inactivation of DAPK in lobular carcinomas compared with ductal carcinomas. Early stage methylation changes in DCIS for RASSF1A and stratifin were confirmed by other groups.

In order to screen an asymptomatic population, candidate molecular markers have to be detectable in remote samples in order to allow for non invasive screening assays. It is well established that DNA from breast tumors can be detected as free nucleic acid in serum and plasma. Alternatively fluids obtained directly from the breast such as nipple aspirate fluid (NAF) or ductal lavage have also been suggested as a body fluid source for molecular testing. However, since the procedures to obtain NAF and ductal lavage have been questioned for their reliability and are uncomfortable for the patient, blood based testing is clearly preferred for screening assays.

Blood based molecular cancer screening assays are faced with the challenge to detect minute omits of tumor DNA in a background of normal DNA from other tissues. Tumor markers that are based on DNA methylation can be detected using assays that amplify DNA in a methylation specific way such as MSP or HeavyMethyl™. These assays allow highly sensitive detection of few copies of methylated DNA in a background of excess normal DNA

Multifactorial approach, Cancer diagnostics has traditionally relied upon the detection of single molecular markers (e.g. gene mutations, elevated PSA levels). Unfortunately, cancer is a disease state in which single markers have typically failed to detect or differentiate many forms of the disease. Thus, assays that recognize only a single marker have been shown to be of limited predictive value, as well be discussed briefly herein. A successful approach currently being pursued in methylation based cancer diagnostics and the screening, diagnosis, and therapeutic monitoring of such diseases is the use of a selection of multiple markers. The multiplexed analytical approach is particularly well suited for cancer diagnostics since cancer is not a simple disease, this multi-factorial “panel” approach is consistent with the heterogeneous nature of cancer, both cytologically and clinically.

Key to the successful implementation of a panel approach to methylation based diagnostic tests is the design and development of optimized panels of markers that can characterize and distinguish disease states. This patent application describes an efficient and unique panel of genes the methylation analysis of one or a combination of the members of the panel enabling the detection of cell proliferative disorders of the prostate with a particularly high sensitivity, specificity and/or predictive value.

Development of medical tests. Two key evaluative measures of any medical screening or diagnostic test are its sensitivity and specificity, which measure how well the test performs to accurately detect all affected individuals without exception, and without falsely including individuals who do not have the target disease (predictive value). Historically, many diagnostic tests have been criticized due to poor sensitivity and specificity.

A true positive (TP) result is where the test is positive and the condition is present. A false positive (FP) result is where the test is positive but the condition is not present. A true negative (TN) result is where the test is negative and the condition is not present. A false negative (FN) result is where the test is negative but the condition is not present.

Sensitivity=TP/(TP+FN)

Specificity=TN/(FP+TN)

Predictive value=TP/(TP+FP)

Sensitivity is a measure of a test's ability to correctly detect the target disease in an individual being tested. A test having poor sensitivity produces a high rate of false negatives, i.e., individuals who have the disease but are falsely identified as being free of that particular disease. The potential danger of a false negative is that the diseased individual will remain undiagnosed and untreated for some period of time, during which the disease may progress to a later stage wherein treatments, if any, may be less effective. An example of a test that has low sensitivity is a protein-based blood test for HIV. This type of test exhibits poor sensitivity because it fails to detect the presence of the virus until the disease is well established and the virus has invaded the bloodstream in substantial numbers. In contrast, an example of a test that has high sensitivity is viral-load detection using the polymerase chain reaction (PCR). High sensitivity is achieved because this type of test can detect very small quantities of the virus. High sensitivity is particularly important when the consequences of missing a diagnosis are high.

Specificity, on the other hand, is a measure of a test's ability to identify accurately patients who are free of the disease state. A test having poor specificity produces a high rate of false positives, i.e., individuals who are falsely identified as having the disease. A drawback of false positives is that they force patients to undergo unnecessary medical procedures treatments with their attendant risks, emotional and financial stresses, and which could have adverse effects on the patient's health. A feature of diseases which makes it difficult to develop diagnostic tests with high specificity is that disease mechanisms, particularly in cancer, often involve a plurality of genes and proteins. Additionally, certain proteins may be elevated for reasons unrelated to a disease state. An example of a test that has high specificity is a gene-based test that can detect a p53 mutation. Specificity is important when the cost or risk associated with further diagnostic procedures or further medical intervention are very high.

Methylation analysis of breast fluids. The detectability of methylation in body fluids of breast cancer patients has been established, Silva at al. (Br J Cancer. 1999 June; 80(8):1262-4.) described the detection of methylated p16INK4a exon 1 in the plasma of five of eight tested breast cancer patients with p16INK4a axon 1 tumor methylation. The sensitivity of the analysis has since been improved by analyzing a panel of genes. Krassenstein et al. (Clin Cancer Res. 2004 Jan. 1; 10(1 Pt 1):28-32.) described the analysis of a panel of six genes (GSTP1, RARB2, p16INK4a, p14ARF, RASSF1A and DAPK) in matched tumor and nipple aspirate fluid (herein also referred to as NAF). Using a small sample set (22 tumors, 5 healthy patients and 5 benign breast patients) it was established that at least one gene of the panel was methylated in the tumor, and that this methylation could be detected in the NAF of 18 of the 22 breast cancer.

Although the study by Krassenstein et al. confirms that methylation observed in tumour tissue can be detected in breast derived fluid there are several technical problems associated with providing a body fluid based test, some of which were acknowledged but not satisfactorily resolved. Firstly, the markers used by Krassenstein were not specifically methylated in breast cancer, but were general cancer markers methylated in a range of cancers. Therefore, if said panel were to be utilized in a clinical setting it is probable that there would be an increased number of false positives, where methylated DNA from cancers of other tissues (or free-floating DNA therefrom) would be detected.

Although Krassenstein at al. aimed to provide a breast cancer screening test, patient compliance with a procedure such as NAF (or e.g. ductal lavage) would likely be low, except in the most at-risk populations. The preferred sample type for a screening test with high patient compliance would more preferably be blood based. The performance of a panel tested on tissue or NAF is no indicator as to its performance on a blood sample. Therefore, any panel would have to be validated on blood samples in order to establish that the markers were not also methylated in blood.

These issues were both shortly addressed by Evron et al. (Lancet. 2001 Apr. 28; 357(9265):1335-6.). In this study a gene panel consisting, of Cyclin D2, FARB and Twist was selected based on factors including their methylation status in white blood cells. The methylation status of these genes was then analyzed in matched tissue and ductal lavage fluid. The gene panel detected invasive breast cancer in 48 of 50 samples.

The main aim of a screening test is the detection of low grade tumors, such as DCIS, higher grade tumors are easily detected by e.g. self-examination and mammography and are harder to treat. This was not enabled by Krassenstein et al. The sample set used consisted of mostly high grade (2 and 3) tumors. There was only one grade 1 tumor. Therefore it may be concluded the suitability of the panel for the detection of low grade tumors has not been fully established, in particular as it is not possible to confirm if the NAF sample in question tested positive for methylation. Furthermore, it is generally assumed that methylation is a progressive feature of tumorigenesis. One would conclude that it is in the detection of the early stages of tumorigenesis that a highly specifically selected panel of genetic markers as opposed to a panel of markers selected for their methylation status in high grade tumor tissue would be required. The panel investigated by Evron et al. detected only 8 out of 14 cases of DCIS thus confirming that a panel suited to the detection of breast cancers is not necessarily suitable for detection of DCIS.

One can summarize the state of the art in that methylation gene panels for the analysis of breast fluids are known, however, there are deficiencies associated with all said panels. Due to these technical difficulties none of these gene panels fulfill the requirements of a breast cancer screening test, namely that the test is suitable for use in body fluids, most preferably blood and that the test be capable of detecting early stage cell proliferative disorders such as DCIS.

The use of a panel of methylation markers consisting RASSF1A, TWIST, Cyclin D2 and HIN1 for the differentiation of invasive breast carcinoma from normal breast tissue was recently described by Fackler et al. By use of a highly sensitive quantitative multiplexed methylation-specific PCR assay the study detected the presence of promoter hypermethylation of the gene panel in breast cancer (as opposed to normal breast tissue) with a sensitivity of 84% and a specificity of 94%. Therefore, the study is significant in establishing the use of methylation markers for the sensitive detection of breast cancer cells in a background of non-cancerous cells. However, the samples used by Fackler et al., were tissue based (including those extracted by means of ductal lavage), thus it has not been established whether such a sensitivity and specificity would be obtainable using body fluid based samples. Furthermore, the same panel proved unable of detecting ductal carcinoma in-situ. Therefore, the method is unsuitable for use as an early screening test.

SUMMARY OF THE INVENTION

The present invention provides novel methods for detecting and/or distinguishing between breast cell proliferative disorders. In preferred embodiments the present invention enables the screening of at-risk populations for the early detection of breast cancers. Further embodiments of the method may also be used as alternatives to cytological screening for the differentiation of breast carcinomas from benign breast cell proliferative disorders.

The invention achieves solves this longstanding need in the art by providing a panel of genes and/or genomic sequences according to Table 3, the expression of these genes are indicative of the presence or absence of breast cell proliferative disorders or features thereof. Preferred selections and combinations of genes are provided, the analysis of which enable the differentiation and detection of various classes of breast cell proliferative disorders, namely:

• • Detection of breast cell proliferative disorders.
  • Detection of early stage breast cancers, including differentiation from benign breast cell proliferative disorders.
  • Differentiation of breast cancers from other cancers
  • Detection of breast cancer cells in a background of blood or fluids derived therefrom.
  • Differentiation of DCIS from benign breast cell proliferative disorders (including healthy breast tissue).

It is particularly preferred that the expression status of said genes and/or genomic sequences is determined according to the methylation status of CpG positions thereof.

In order to enable this analysis the invention provides a method for the analysis of biological samples for genomic methylation associated with the development of breast cell proliferative disorders. Said method is characterized in that at least one nucleic acid, or a fragment thereof, from the group consisting of SEQ ID NO: 1 to SEQ ID NO; 118 is/are contacted with a reagent or series of reagents capable of distinguishing between methylated and non methylated CpG dinucleotides within the genomic sequence, or sequences of interest.

The present invention provides further methods for ascertaining genetic and/or epigenetic parameters of SEQ ID NO: 1 to SEQ ID NO: 118, including but not limited to mRNA expression analysis, protein expression analysis and methylation analysis. The method has utility for the improved diagnosis, differentiation and treatment of breast cell proliferative disorders, more specifically by enabling the improved detection of and differentiation between subclasses of said disorder. The invention presents several improvements over the State of the art. Although methylation assays for the detection of breast cancer in body fluids are known there is currently no assay that fulfills the criteria of being validated in blood and capable of detecting DOS with a suitable accuracy for commercial approval.

The source may be any suitable source, such as cell lines, histological slides, biopsies, paraffin-embedded tissue, body fluids, blood plasma, blood serum, whole blood, isolated blood cells, cells isolated from the blood and all possible combinations thereof. It is preferred that said sources of DNA are body fluids selected from the group consisting nipple aspirate fluid, lymphatic fluid, ductal lavage fluid, fine needle aspirate, blood plasma, blood serum, whole blood, isolated blood cells, cells isolated from the blood.

Specifically, the present invention provides a method for detecting breast cell proliferative disorders, comprising: obtaining a biological sample comprising genomic nucleic acid(s); contacting the nucleic acid(s), or a fragment thereof, with one reagent or a plurality of reagents sufficient for distinguishing between methylated and non methylated CpG dinucleotide sequences within a target sequence of the subject nucleic acid, wherein the target sequence comprises, or hybridizes under stringent conditions to, a sequence comprising at least 16 contiguous nucleotides of SEQ ID NO: 1 to SEQ ID NO: 118, said contiguous nucleotides comprising at least one CpG dinucleotide sequence; and determining, based at least in part on said distinguishing, the methylation state of at least one target CpG dinucleotide sequence, or an average, or a value reflecting an average methylation state of a plurality of target CpG dinucleotide sequences. Preferably, distinguishing between methylated and non methylated CpG dinucleotide sequences within the target sequence comprises methylation state-dependent conversion or non-conversion of at least one such CpG dinucleotide sequence to the corresponding converted or non-converted dinucleotide sequence within a sequence selected from the group consisting of SEQ ID NO: 493 to SEQ ID NO: 964, and contiguous regions thereof corresponding to the target sequence.

Additional embodiments provide a method for the detection of breast cell proliferative disorders, comprising: obtaining a biological sample having subject genomic DNA; extracting the genomic DNA; treating the genomic DNA, or a fragment thereof, with one or more reagents to convert 5-position unmethylated cytosine bases to uracil or to another base that is detectably dissimilar to cytosine in terms of hybridization properties; contacting the treated genomic DNA, or the treated fragment thereof, with an amplification enzyme and at least two primers comprising, in each case a contiguous sequence at least 9 nucleotides in length that is complementary to, or hybridizes under moderately stringent or stringent conditions to a sequence selected from the group consisting SEQ ID NO: 493 to SEQ ID NO: 964, and complements thereof, wherein the treated DNA or the fragment thereof is either amplified to produce an amplificate, or is not amplified; and determining, based on a presence or absence of, or on a property of said amplificate, the methylation state of at least one CpG dinucleotide sequence selected from the group consisting of SEQ ID NO: 1 to SEQ ID NO: 118, or an average, or a value reflecting an average methylation state of a plurality of CpG dinucleotide sequences thereof. Preferably, at least one such hybridizing nucleic acid molecule or peptide nucleic acid molecule is bound to a solid phase. Preferably, determining comprises use of at least one method selected from the group consisting of hybridizing at least one nucleic acid molecule comprising a contiguous sequence at least 9 nucleotides in length that is complementary to, or hybridizes under moderately stringent or stringent conditions to a sequence selected from the group consisting of SEQ ID NO; 493 to SEQ ID NO: 964, and complements thereof; hybridizing at least one nucleic acid molecule, bound to a solid phase, comprising a contiguous sequence at least 9 nucleotides in length that is complementary to, or hybridizes under moderately stringent or stringent conditions to a sequence selected from the group consisting of SEQ ID NO: 493 to SEQ ID NO: 964, and complements thereof; hybridizing at least one nucleic acid molecule comprising a contiguous sequence at least 9 nucleotides in length that is complementary to, or hybridizes under moderately stringent or stringent conditions to a sequence selected from the group consisting of SEQ ID NO: 493 to SEQ ID NO: 964, and complements thereof, and extending at least one such hybridized nucleic acid molecule by at least one nucleotide base; and sequencing of the amplificate.

Further embodiments provide a Method for the analysis of breast cell proliferative disorders, comprising: obtaining a biological sample having subject genomic DNA; extracting the genomic DNA; contacting the genomic DNA, or a fragment thereof, comprising one or more sequences selected from the group consisting of SEQ ID NO: 1 to SEQ ID NO: 118 or a sequence that hybridizes under stringent conditions thereto, with one or more methylation-sensitive restriction enzymes, wherein the genomic DNA is either digested thereby to produce digestion fragments, or is not digested thereby; and determining, based on a presence or absence of, or on property of at least one such fragment, the methylation state of at least one CpG dinucleotide sequence of one or more sequences selected from the group consisting of SEQ ID NO: 1 to SEQ ID NO: 118, or an average, or a value reflecting an average methylation state of a plurality of CpG dinucleotide sequences thereof. Preferably, the digested or undigested genomic DNA is amplified prior to said determining.

Additional embodiments provide novel genomic and chemically modified nucleic acid sequences, as well as oligonucleotides and/or PNA-oligomers for analysis of cytosine methylation patterns within sequences from the group consisting of SEQ ID NO: 1 to SEQ ID NO: 118.

In a further embodiment the present invention provides DNA markers associated with the presence of general cancers.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 4048 (Assay 1) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 2 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 22 (NR2E1) (Assay o) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 3 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 29 (Assay 2) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 4 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 90 (RASSF1A) (Assay 1) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 5 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 77 (FABP3) (Assay 1-5) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 6 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 104 (CCND2) (Assay 4) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 7 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 38 (LMX1A) (Assay 3) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 8 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 20 (PRDM6) (Assay o) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 9 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 13 (MSF) (Assay 2) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 10 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 112 (SLIT2) (Assay 2-2-5) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 11 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 98 (DAPK1) (Assay 2) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 12 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 115 (SCGB3A1) (Assay 1) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 23. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 13 provides three plots. On the left hand side are two binary distribution curves showing the analysis of SEQ ID NO: 90 (RASSF1A) (Assay 1) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 24. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 14 provides three plots. On the left hand side are two binary distribution curves showing the analysis of SEQ ID NO: 38 (LMX1A) (Assay 3) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 24. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 15 provides two plots. On the left hand side is a binary distribution curve showing the analysis of SEQ ID NO: 13 (MSF) (Assay 2) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 24. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 16 provides three plots. On the left hand side are two binary distribution curves showing the analysis of SEQ ID NO: 104 (CCND2) (Assay 4) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 24. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 17 provides three plots. On the left hand side are two binary distribution curves showing the analysis of SEQ ID NO: 77 (FABF3) (Assay 1-5) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 24. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIG. 18 provides three plots. On the left hand side are two binary distribution curves showing the analysis of SEQ ID NO: 20 (PRDM6) (Assay o) according to Example 2 by means of the quantitative assay shown in Table 22, results shown in Table 24. The Y-Axis shows the proportion of analysed samples with a methylation level greater than the quantified value shown on the X-axis. On the right hand side is a ROC plot of said assay calculated according to Example 2.

FIGS. 19-78 provide a graphical representation of the results of the microarray analysis according to Example 1. Each of said figures presents a matrix of the level of methylation of each significant oligomer, oligomers belonging to each gene or genomic sequence are grouped in one discrete block. The SEQ ID NO: of each oligomer is shown on the left hand side of the matrix, on the right hand side of the matrix the FOR corrected multivariate P-value of the oligomers belonging to each individual gene or genomic sequence is shown. The level of methylation is shown by the color of each square of the matrix, from black representing total methylation (+2) to white representing total unmethylation (−2) as shown on the scale to the right hand side of the matrix. Each vertical line of the matrix represents one sample, the type of sample is shown above the matrix.

DETAILED DESCRIPTION OF THE INVENTION

Definitions

The term “Observed/Expected Ratio” (“O/E Ratio”) refers to the frequency of CpG dinucleotides within a particular DNA sequence, and corresponds to the [number of CpG sites/(number of C bases×number of G bases)]×band length for each fragment.

The term “CpG island” refers to a contiguous region of genomic DNA that satisfies the criteria of (1) having a frequency of CpG dinucleotides corresponding to an “Observed/Expected Ratio”>0.6, and (2) having a “GC Content”>0.5. CpG islands are typically, but not always, between about 0.2 to about 1 kb, or to about 2 kb in length.

The term “methylation state” or “methylation status” refers to the presence or absence of 5-methylcytosine (“5-mCyt”) at one or a plurality of CpG dinucleotides within a DNA sequence. Methylation states at one or more particular CpG methylation sites (each having two CpG CpG dinucleotide sequences) within a DNA sequence include “unmethylated,” “fully-methylated” and “hemi-methylated.”

The term “hemi-methylation” or “hemimethylation” refers to the methylation state of a double stranded nucleic acid, wherein only the CpG positions of one strand thereof is methylated (e.g., 5′-CCMGG-3′ (top strand): 3′-GGCC-5′ (bottom strand)).

The term ‘AUC’ as used herein is an abbreviation for the area under a curve. In particular it refers to the area under a Receiver Operating Characteristic (ROC) curve. The ROC curve is a plot of the true positive rate against the false positive rate for the different possible cutpoints of a diagnostic test. It shows the trade-off between sensitivity and specificity depending on the selected cutpoint (any increase in sensitivity will be accompanied by a decrease in specificity). The area under an ROC curve (AUC) is a measure for the accuracy of a diagnostic test (the larger the area the better, optimum is 1, a random test would have a ROC curve lying on the diagonal with an area of 0.5; for reference: J. P. Egan. Signal Detection Theory and ROC Analysis, Academic Press, New York, 1975).

The term “hypermethylation” refers to the average methylation state corresponding to an increased presence of 5-mCyt at one or a plurality of CpG dinucleotides within a DNA sequence of a test DNA sample, relative to the amount of 5-mCyt found at corresponding CpG dinucleotides within a normal control DNA sample.

The term “hypomethylation” refers to the average methylation state corresponding to a decreased presence of 5-mCyt at one or a plurality of CpG dinucleotides within a DNA sequence of a test DNA sample, relative to the amount of 5-mCyt found at corresponding CpG dinucleotides within a normal control DNA sample.

The term “microarray” refers broadly to both “DNA microarrays,” and ‘DNA chip(s),’ as recognized in the art, encompasses all art-recognized solid supports, and encompasses all methods for affixing nucleic acid molecules thereto or synthesis of nucleic acids thereon.

“Genetic parameters” are mutations and polymorphisms of genes and sequences further required for their regulation. To be designated as mutations are, in particular, insertions, deletions, point mutations, inversions and polymorphisms and, particularly preferred, SNPs (single nucleotide polymorphisms).

“Epigenetic parameters” are, in particular, cytosine methylations. Further epigenetic parameters include, for example, the acetylation of histones which, however, cannot be directly analyzed using the described method but which, in turn, correlate with the DNA methylation.

The term “bisulfite reagent” refers to a reagent comprising bisulfite, disulfite, hydrogen sulfite or combinations thereof, useful as disclosed herein to distinguish between methylated and unmethylated CpG dinucleotide sequences.

The term “Methylation assay” refers to any assay for determining the methylation state of one or more CpG dinucleotide sequences within a sequence of DNA.

The term “MS.AP-PCR” (Methylation-Sensitive Arbitrarily-Primed Polymerase Chain Reaction) refers to the art-recognized technology that allows for a global scan of the genome using CO-rich primers to focus on the regions most likely to contain CpG dinucleotides, and described by Gonzalgo et al., Cancer Research 57:594-599, 1997.

The term “MethyLight™” refers to the art-recognized fluorescence-based real-time PCR technique described by Ends et al., Cancer Res. 59:2302-2306, 1999.

The term “HeavyMethyl™” assay, in the embodiment thereof implemented herein, refers to an assay, wherein methylation specific blocking probes (also referred to herein as blockers) covering CpG positions between, or covered by the amplification primers enable methylation-specific selective amplification of a nucleic acid sample. The HeavyMethyl assay has previously been described in WO02/072880 and Cottrell et al. Nucleic Acids Res. 2004 Jan. 13; 32(1):e10.

The term “HeavyMethyl™ MethyLight™ assay, in the embodiment thereof implemented herein, refers to a HeavyMethyl™ MethyLight™ assay, which is a variation of the MethyLight™ assay, wherein the MethyLight™ assay is combined with methylation specific blocking probes covering CpG positions between the amplification primers.

The term “Ms-SNuPE” (Methylation-sensitive Single Nucleotide Primer Extension) refers to the art-recognized assay described by Gonzalgo and Jones, Nucleic Acids Res. 25:2529-2531, 1997.

The term “MSP” (Methylation-specific PCR) refers to the art-recognized methylation assay described by Herman et al. Proc. Natl. Acad. Sci. USA 93:9821-9826, 1996, and by U.S. Pat. No. 5,786,146.

The term “COBRA” (Combined Bisulfite Restriction Analysis) refers to the art-recognized methylation assay described by Xiong and Laird, Nucleic Acids Res. 25:2532-2534, 1997.

The term “MCA” (Methylated CpG Island Amplification) refers to the methylation assay described by Toyota et al., Cancer Res. 59:2307-12, 1999, and in WO 00/26401 A1.

The term “hybridization” is to be understood as a bond of an oligonucleotide to a complementary sequence along the lines of the Watson-Crick base pairings in the sample DNA, forming a duplex structure.

“Stringent hybridization conditions,” as defined herein, involve hybridizing at 68° C. in 5×SSC/5×Denhardt's solution/1.0% SDS, and washing in 0.2×SSC/0.1% SDS at room temperature, or involve the art-recognized equivalent thereof (e.g., conditions in which a hybridization is carried out at 60° C. in 2.5×SSC buffer, followed by several washing steps at 37° C. in a low buffer concentration, and remains stable). Moderately stringent conditions, as defined herein, involve including washing in 3×SSC at 42° C., or the art-recognized equivalent thereof. The parameters of salt concentration and temperature can be varied to achieve the optimal level of identity between the probe and the target nucleic acid. Guidance regarding such conditions is available in the art, for example, by Sambrook et al., 1989, Molecular Cloning, A Laboratory Manual, Cold Spring Harbor Press, N.Y.; and Ausubel et al. (eds.), 1995, Current Protocols in Molecular Biology, (John Wiley and Sons, N.Y.) at Unit 2.10.

The terms “array SEQ ID NO,” “composite array SEQ ID NO,” or “composite array sequence” refer to a sequence, hypothetical or otherwise, consisting of a head-to-tail (5′ to 3′) linear composite of all individual contiguous sequences of a subject array (e.g., a head-to-tail composite of SEQ ID NO: 1-118, in that order).

The terms “array SEQ ID NO node,” “composite array SEQ ID NO node,” or “composite array sequence node” refer to a junction between any two individual contiguous sequences of the “array SEQ ID NO,” the “composite array SEQ ID NO,” or the “composite array sequence.”

In reference to composite array sequences, the phrase “contiguous nucleotides” refers to a contiguous sequence region of any individual contiguous sequence of the composite array, but does not include a region of the composite array sequence that includes a “node,” as defined herein above.

Overview:

The present invention provides for molecular genetic markers that have novel utility for the analysis of gene expression, most preferably as expressed in the methylation thereof, associated with the development of breast cell proliferative disorders. Said markers may be used for detecting and/or distinguishing between breast cell proliferative disorders, thereby providing improved means for the detection, classification and treatment of said disorders.

Bisulfite modification of DNA is an art-recognized tool used to assess CpG methylation status. 5-methylcytosine is the most frequent covalent base modification in the DNA of eukaryotic cells. It plays a role, for example, in the regulation of the transcription, in genetic imprinting, and in tumorigenesis. Therefore, the identification of 5-methylcytosine as a component of genetic information is of considerable interest. However, 5-methylcytosine positions cannot be identified by sequencing, because 5-methylcytosine has the same base pairing behavior as cytosine. Moreover, the epigenetic information carried by 5-methylcytosine is completely lost during, e.g., PCR amplification.

The most frequently used method for analyzing DNA for the presence of 5-methylcytosine is based upon the specific reaction of bisulfite with cytosine whereby, upon subsequent alkaline hydrolysis, cytosine is converted to uracil which corresponds to thymine in its base pairing behavior. Significantly, however, 5-methylcytosine remains unmodified under these conditions. Consequently, the original DNA is converted in such a manner that methylcytosine, which originally could not be distinguished from cytosine by its hybridization behavior, can now be detected as the only remaining cytosine, using standard, art-recognized molecular biological techniques, for example, by amplification and hybridization, or by sequencing. All of these techniques are based on differential base pairing properties, which can now be fully exploited.

The present invention provides for the use of the bisulfite technique, in combination with one or more methylation assays, for determination of the methylation status of CpG dinucleotide sequences within sequences from the group consisting of SEQ ID NO: 1 to SEQ ID NO: 118. According to the present invention, determination of the methylation status of CpG dinucleotide sequences within sequences from the group consisting of SEQ ID NO: 1 to SEQ ID NO: 118 has diagnostic and prognostic utility.

Methylation Assay Procedures. Various methylation assay procedures are known in the art, and can be used in conjunction with the present invention. These assays allow for determination of the methylation state of one or a plurality of CpG dinucleotides (e.g., CpG islands) within a DNA sequence. Such assays involve, among other techniques, DNA sequencing of bisulfite-treated DNA, PCR (for sequence-specific amplification), Southern blot analysis, and use of methylation-sensitive restriction enzymes.

For example, genomic sequencing has been simplified for analysis of DNA methylation patterns and 5-methylcytosine distribution by using bisulfite treatment (Frommer et al., Proc. Natl. Acad. Sci. USA 89:1827-1831, 1992). Additionally, restriction enzyme digestion of PCR products amplified from bisulfite-converted DNA is used, e.g., the method described by Sadri and Hornsby (Nucl. Acids Res. 24:5058-5059, 1996), or COBRA (Combined Bisulfite Restriction Analysis) (Xiong and Laird, Nucleic Acids Res. 25:2532-2534, 1997).

COBRA. COBRA analysis is a quantitative methylation assay useful for determining DNA methylation levels at specific gene loci in small amounts of genomic DNA (Xiong and Laird, Nucleic Acids Res. 25:2532-2534, 1997). Briefly, restriction enzyme digestion is used to reveal methylation-dependent sequence differences in PCR products of sodium bisulfite-treated DNA. Methylation-dependent sequence differences are first introduced into the genomic DNA by standard bisulfite treatment according to the procedure described by Frommer et al. (Proc. Natl. Acad. Sci. USA 89:1827-1831, 1992). PCR amplification of the bisulfite converted DNA is then performed using primers specific for the CpG islands of interest, followed by restriction endonuclease digestion, gel electrophoresis, and detection using specific, labeled hybridization probes. Methylation levels in the original DNA sample are represented by the relative amounts of digested and undigested PCR product in a linearly quantitative fashion across a wide spectrum of DNA methylation levels. In addition, this technique can be reliably applied to DNA obtained from microdissected paraffin-embedded tissue samples. Typical reagents (e.g., as might be found in a typical COBRA-based kit) for COBRA analysis may include, but are not limited to: PCR primers for specific gene (or bisulfite treated DNA sequence or CpG island); restriction enzyme and appropriate buffer; gene-hybridization oligo; control hybridization oligo; kinase labeling kit for oligo probe; and labeled nucleotides. Additionally, bisulfite conversion reagents may include: DNA denaturation buffer; sulfonation buffer; DNA recovery reagents or kits (e.g., precipitation, ultrafiltration, affinity column); desulfonation buffer; and DNA recovery components.

Preferably, assays such as “MethyLight™” (a fluorescence-based real-time PCR technique) (Eads et al., Cancer Res. 59:2302-2306, 1999), Ms-SNuPE (Methylation-sensitive Single Nucleotide Primer Extension) reactions (Gonzalgo and Jones, Nucleic Acids Res. 25:2529-2531, 1997) and methylation-specific PCR (“MSP”; Herman et al., Proc. Natl. Acad. Sci. USA 93:9821-9826, 1996; U.S. Pat. No. 5,786,146) are used alone or in combination with other of these methods.

MethyLight™. The MethyLight™ assay is a high-throughput quantitative methylation assay that utilizes fluorescence-based real-time PCR (TaqMan™) technology that requires no further manipulations after the PCR step (Eads et al., Cancer Res. 59:2302-2306, 1999). Briefly, the MethyLight™ process begins with a mixed sample of genomic DNA that is converted, in a sodium bisulfite reaction, to a mixed pool of methylation-dependent sequence differences according to standard procedures (the bisulfite process converts unmethylated cytosine residues to uracil). Fluorescence-based PCR is then performed either in an “unbiased” (with primers that do not overlap known CpG methylation sites) PCR reaction, or in a “biased” (with PCR primers that overlap known CpG dinucleotides) reaction. Sequence discrimination can occur either at the level of the amplification process or at the level of the fluorescence detection process, or both.

The MethyLight™ assay may be used as a quantitative test for methylation patterns in the genomic DNA sample, wherein sequence discrimination occurs at the level of probe hybridization. In this quantitative version, the PCR reaction provides for unbiased amplification in the presence of a fluorescent probe that overlaps a particular putative methylation site. An unbiased control for the amount of input DNA is provided by a reaction in which neither the primers, nor the probe overlie any CpG dinucleotides. Alternatively, a qualitative test for genomic methylation is achieved by probing of the biased PCR pool with either control oligonucleotides that do not “cover” known methylation sites (a fluorescence-based version of the “MSP” technique), or with oligonucleotides covering potential methylation sites.

The MethyLight™ process can by used with a “TaqMan®” probe in the amplification process. For example, double-stranded genomic DNA is treated with sodium bisulfite and subjected to one of two sets of PCR reactions using TaqMan® probes; e.g., with either biased primers and TaqMan® probe, or unbiased primers and TaqMan® probe. The TaqMan® probe is dual-labeled with fluorescent “reporter” and “quencher” molecules, and is designed to be specific for a relatively high GC content region so that it melts out at about 10° C. higher temperature in the PCR cycle than the forward or reverse primers. This allows the TaqMan® probe to remain fully hybridized during the PCR annealing/extension step. As the Taq polymerase enzymatically synthesizes a new strand during PCR, it will eventually reach the annealed TaqMan® probe. The Taq polymerase 5′ to 3′ endonuclease activity will then displace the TaqMan® probe by digesting it to release the fluorescent reporter molecule for quantitative detection of its now unquenched signal using a real-time fluorescent detection system.

Typical reagents (e.g., as might be found in a typical MethyLight™-based kit) for MethyLight™ analysis may include, but are not limited to: PCR primers for specific gene (or bisulfite treated DNA sequence or CpG island); TaqMan® probes; optimized PCR buffers and deoxynucleotides; and Taq polymerase.

Ms-SNuPE. The Ms-SNuPE technique is a quantitative method for assessing methylation differences at specific CpG sites based on bisulfite treatment of DNA, followed by single-nucleotide primer extension (Gonzalgo and Jones, Nucleic Acids. Res. 25:2529-2531, 1997). Briefly, genomic DNA is reacted with sodium bisulfite to convert unmethylated cytosine to uracil while leaving 5-methylcytosine unchanged. Amplification of the desired target sequence is then performed using PCR primers specific for bisulfite-converted DNA, and the resulting product is isolated and used as a template for methylation analysis at the CpG site(s) of interest. Small amounts of DNA can be analyzed (e.g., microdissected pathology sections), and it avoids utilization of restriction enzymes for determining the methylation status at CpG sites.

Typical reagents (e.g., as might be found in a typical Ms-SNuPE-based kit) for Ms-SNuPE analysis may include, but are not limited to: PCR primers for specific gene (or bisulfite treated DNA sequence or CpG island); optimized PCR buffers and deoxynucleotides; gel extraction kit; positive control primers; Ms-SNuPE primers for specific gene; reaction buffer (for the Ms-SNuPE reaction); and labeled nucleotides. Additionally, bisulfite conversion reagents may include: DNA denaturation buffer; sulfonation buffer; DNA recovery regents or kit (e.g., precipitation, ultrafiltration, affinity column); desulfonation buffer; and DNA recovery components.

MSP. MSP (methylation-specific PCR) allows for assessing the methylation status of virtually any group of CpG sites within a CpG island, independent of the use of methylation-sensitive restriction enzymes (Herman et al. Proc. NaCl. Acad. Sci. USA 93:9821-9826, 1996; U.S. Pat. No. 5,786,146). Briefly, DNA is modified by sodium bisulfite converting all unmethylated, but not methylated cytosines to uracil, and subsequently amplified with primers specific for methylated versus unmethylated DNA. MSP requires only small quantities of DNA, is sensitive to 0.1% methylated alleles of a given CpG island locus, and can be performed on DNA extracted from paraffin-embedded samples. Typical reagents (e.g., as might be found in a typical MSP-based kit) for MSP analysis may include, but are not limited to: methylated and unmethylated PCR primers for specific gene (or bisulfite treated DNA sequence or CpG island), optimized PCR buffers and deoxynucleotides, and specific probes.

Genomic Sequences according to SEQ ID NO: 1 to SEQ ID NO: 118, and non-naturally occurring treated variants thereof according to SEQ ID NO: 493 to SEQ ID NO: 964, were determined to have utility for the detection, classification and/or treatment of breast cell proliferative disorders.

In one embodiment the invention provides a method for detecting and/or for detecting and distinguishing between or among breast cell proliferative disorders in a subject. Said method comprises the following steps

i) contacting genomic DNA obtained from the subject with at least one reagent, or series of reagents that distinguishes between methylated and non-methylated CpG dinucleotides within at least one target region of the genomic DNA, wherein said contiguous nucleotides comprise at least one CpG dinucleotide sequence, andii) detecting, or detecting and distinguishing between or among breast cell proliferative disorders.

It is particularly preferred that said genomic DNA is isolated from body fluids of the subject. It is further preferred that said body fluid is selected from the group consisting nipple aspirate fluid, lymphatic fluid, ductal lavage fluid, fine needle aspirate, blood plasma, blood serum, whole blood, isolated blood cells, cells isolated from the blood.

Genomic DNA may be isolated by any means standard in the art, including the use of commercially available kits. Briefly, wherein the DNA of interest is encapsulated in by a cellular membrane the biological sample must be disrupted and lysed by enzymatic, chemical or mechanical means. The DNA solution may then be cleared of proteins and other contaminants e.g. by digestion with proteinase K. The genomic DNA is then recovered from the solution. This may be carried out by means of a variety of methods including salting out, organic extraction or binding of the DNA to a solid phase support. The choice of method will be affected by several factors including time, expense and required quantity of DNA.

The genomic DNA sample is then treated in such a manner that cytosine bases which are unmethylated at the 5′-position are converted to uracil, thymine, or another base which is dissimilar to cytosine in terms of hybridization behavior. This will be understood as ‘treatment’ herein.

This is preferably achieved by means of treatment with a bisulfite reagent. The term “bisulfite reagent” refers to a reagent comprising bisulfite, disulfite, hydrogen sulfite or combinations thereof, useful as disclosed herein to distinguish between methylated and unmethylated CpG dinucleotide sequences. Methods of said treatment are known in the art (e.g. PCT/EP2004/011715, which is incorporated by reference in its entirety). It is preferred that the bisulfite treatment is conducted in the presence of denaturing solvents such as but not limited to n-alkylenglycol, particulary diethylene glycol dimethyl ether (DME), or in the presence of dioxane or dioxane derivatives. In a preferred embodiment the denaturing solvents are used in concentrations between 1% and 35% (v/v). It is also preferred that the bisulfite reaction is mailed out in the presence of scavengers such as but not limited to chromane derivatives, e.g., 6-hydroxy-2,5,7,8,-tetramethylchromane 2-carboxylic acid (see: PCT/EP2004/011715 which is incorporated by reference in its entirety). The bisulfite conversion is preferably carried out at a reaction temperature between 30° C. and 70° C., whereby the temperature is increased to over 85° C. for short periods of times during the reaction (see: PCT/EP2004/011715 which is incorporated by reference in its entirety). The bisulfite treated DNA is preferably purified prior to further analysis. This may be conducted by any means known in the art, such as but not limited to ultrafiltration, preferably carried out by means of Microcon™ columns (manufactured by Millipore™). The purification is carried out according to a modified manufacturer's protocol (see; PCT/EP2004/011715 which is incorporated by reference in its entirety).

The treated DNA is then analyzed in order to determine the methylation state of one or more target gene sequences (prior to the treatment) associated with the development of breast carcinoma. It is particularly preferred that the target region comprises, or hybridizes under stringent conditions to at least 16 contiguous nucleotides of at least one gene or genomic sequence selected from the group consisting the genes and genomic sequences as listed in Table 3. It is further preferred that the sequences of said genes in Table 3 as described in the accompanying sequence listing are analyzed. The method of analysis may be selected from those known in the art, including those listed herein. Particularly preferred are MethyLight™, MSP and the use of blocking oligonucleotides as will be described herein. It is further preferred that any oligonucleotides used in such analysis (including primers, blocking oligonucleotides and detection probes) should be reverse complementary, identical, or hybridize under stringent or highly stringent conditions to an at least 16-base-pair long segment of the base sequences of one or more of SEQ ID NO: 493 to SEQ ID NO: 964 and sequences complementary thereto.

Aberrant methylation, more preferably hypermethylation of one or more genes or genomic sequences taken from those listed in Table 3 are associated with the presence of breast carcinoma. Analysis of one or a plurality of the sequences enables detecting, or detecting and distinguishing between or among breast cell proliferative disorders.

In one embodiment, the method discloses the use of one or more genes or genomic sequences selected from the group consisting of APC, ARH1/NOEY2, BRCA2, CCND2, CDKN1A, CDKN2A, SEQ ID NO: 9, DAPK1, SEQ ID NO: 2, EYA4, FHIT, GSTP1, HIC1, IGFBP7, MLH1, PGR, SERPINB5, RARB, SFN, SOD2, TGFBR2, THRB, TIMP3, TP73, NME1, CDH13, THBS1, TMS1/ASC, ESR1, IL6, APAF1, CASP8, SYK, HOXA5, FABP3, RASSF1A, SEQ ID NO: 3, RARA, TWIST, ESR2, PLAU, STAT1, SEQ ID NO: 4, BRCA1, LOT1, PRSS8, SNCG, TPM1, GPC3, CLDN7, SLC19A1, GJB2, SLIT2, IGSF4, MCT1, HS3ST2, PRDM2, ALX4, SEQ ID NO: 5, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 8, SCGB3A1, SEQ ID NO: 1, PROSTAGLANDIN E2 RECEPTOR, EP4 SUBTYPE (PROSTANOID EP4 RECEPTOR) (PGE RECEPTOR, EP4 SUBTYPE), ORPHAN NUCLEAR RECEPTOR NR5A2 (ALPHA-1-FETOPROTEIN TRANSCRIPTION FACTOR) (HEPATOCYTIC TRANSCRIPTION FACTOR) (B1-BINDING FACTOR) (HB1F) (CYP7A PROMOTER BINDING FACTOR), LIM DOMAIN KINASE 1, SASH1, S100A7, BCL11B, SEQ ID NO: 51, MGC34831, SEQ ID NO: 54, PDLIM1, MSF, SEQ ID NO: 14, SEQ ID NO: 15, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 18, SEQ ID NO: 19, PRDM6, RAP213, NR2E1, PCDH7, DKK3, RTTN, SNAP25, SEQ ID NO: 26, GIRK2, SEQ ID NO: 28, SEQ ID NO: 29, ARL7, SEQ ID NO: 31, THH, HOXB13, SEQ ID NO: 35, MGC10561, LMX1A, SENP3, GS1, TITF1, SEQ ID NO: 42, DDX51, SEQ ID NO: 117, SEQ ID NO: 45, SEQ ID NO: 46, O60279, and SEQ ID NO: 48 as markers for the detection of breast cancers.

The use of said genes and/or sequences may be enabled by means of any analysis of the expression of the gene, by means of mRNA expression analysis or protein expression analysis. However, in the most preferred embodiment of the invention, the detection of breast cell proliferative disorders is enabled by means of analysis of the methylations status of said genes or genomic sequences and their promoter or regulatory elements. Methods for the methylation analysis of genes are described herein.

It is also preferred that the expression level of only one gene or genomic sequence from the group consisting of PRDM2, PLAU, GSTP1, SLIT2, CCND2, HOXA5, RASSF1A, HS3ST2, ARH1/NOEY2, SCGB3A1, SEQ ID NO: 6, SEQ ID NO: 3, SEQ ID NO: 18, SEQ ID NO: 7, SEQ ID NO: 41, SEQ ID NO: 22, SEQ ID NO: 46, SEQ ID NO: 13, and SEQ ID NO: 31 is analyzed. It is particularly preferred that this is carried out by means of methylation analysis.

In one embodiment the method discloses the use of one or more genes or genomic sequences selected from the group consisting of ARH1/NOEY2, CCND2, CDKN1A, CDKN2A, DAPK1, SEQ ID NO: 2, EYA4, FHIT, GSTP1, HIC1, IGFBP7, SERPINB5, TERT, TGEBR2, THRB, TIMP3, TP73, NME1, CDH13, THBS1, TMS1/ASC, IL6, APAF1, SYK, HOXA5, FABP3, RASSF1A, SEQ ID NO: 3, TWIST, ESR2, PLAU, STAT1, SEQ ID NO: 4, LOT1, GPC3, CLDN7, GJB2, SLIT2, IGSF4, MCT1, PRDM2, ALX4, SEQ ID NO: 5, SEQ ID NO: 6, SEQ ID NO: 8, SCGB3A1, SEQ ID NO: 1, PROSTAGLANDIN E2 RECEPTOR, EP4 SUBTYPE (PROSTANOID EP4 RECEPTOR) (PGE RECEPTOR, EP4 SUBTYPE), LIM DOMAIN KINASE 1, MGC34831, SEQ ID NO: 54, MSF, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 18, SEQ ID NO: 19, PRDM6, NR2E1, PCDH7, RTTN, SNAP25, SEQ ID NO: 26, SEQ ID NO: 28, ARL7, SEQ ID NO: 31, THH, HOXB13, SEQ ID NO: 35, MGC10561, LMX1A, SENP3, TITF1, SEQ ID NO: 42, DDX51, SEQ ID NO: 45, O60279, SEQ ID NO: 48 as markers for the differentiation of breast cancers from other cancers. Said use of the genes and/or sequences may be enabled by means of any analysis of the expression of the gene, by means of mRNA expression analysis or protein expression analysis. However, in the most preferred embodiment of the invention, the detection of breast cell proliferative disorders is enabled by means of analysis of the methylation status of said genes or genomic sequences and their promoter or regulatory elements. Methods for the methylation analysis of genes are described herein.

In said embodiment it is further preferred that the expression level of only one gene or genomic sequence from the group consisting PRDM2, GSTP1, ALX4, HOXA5, PLAU, RASSF1A, IGSF4, SLIT2, DAPK1, CDKN1A, SEQ ID NO: 38, SEQ ID NO: 35, LIMK-1, SEQ ID NO: 39, SEQ ID NO: 10, SEQ ID NO: 26, SEQ ID NO: 8, SEQ ID NO: 22, SEQ ID NO: 18, and SEQ ID NO: 47 is analyzed. It is particularly preferred that this is carried out by means of methylation analysis.

In one embodiment the method discloses the use of one or more genes or genomic sequences selected from the group consisting of APC, ARH1/NOEY2, CCND2, CDH1, CDKN1A, CDKN2A, SEQ ID NO: 9, DAPK1, SEQ ID NO: 2, EYA4, FHIT, GSTP1, HIC1, IGFBP7, PGR, SERPINB5, RARB, SFN, SOD2, TERT, TGFBR2, THRB, TIMP3, NME1, CDH13, THBS1, TMS1/ASC, ESR1, IL6, APAF1, CASP8, SYK, HOXA5, FABP3, RASSF1A, SEQ ID NO: 3, TWIST, ESR2, PLAU, STAT1, SEQ ID NO: 4, BRCA1, LOT1, PRSS8, SNCG, GPC3, CLDN7, SLC19A1, GJB2, SLIT2, IGSF4, MCT1, HS3ST2, PRDM2, ALX4, SEQ ID NO: 5, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 8, SCGB3A1, SEQ ID NO: 1, PROSTAGLANDIN E2 RECEPTOR, EP4 SUBTYPE (PROSTANOID EP4 RECEPTOR) (PGE RECEPTOR, EP4 SUBTYPE), ORPHAN NUCLEAR RECEPTOR NR5A2 (ALPHA-1-FETOPROTEIN TRANSCRIPTION FACTOR) (HEPATOCYTIC TRANSCRIPTION FACTOR) (B1-BINDING FACTOR) (HB1F) (CYP7A PROMOTER BINDING FACTOR), LIM DOMAIN KINASE 1, SASH1, S100A7, BCL11B, SEQ ID NO: 51, MGC34831, SEQ ID NO: 54, PDLIM1, MSF, SEQ ID NO: 14, SEQ ID NO: 15, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 18, SEQ ID NO: 19, PRDM6, RAP2B, NR2E1, PCDH7, DKK3, RTTN, SNAP25, SEQ ID NO: 26, GIRK2, SEQ ID NO: 28, SEQ ID NO: 29, ARL7, SEQ ID NO: 31, THH, HOXB13, SEQ ID NO: 35, SEQ ID NO; 36, MGC10561, LMX1A, SENP3, GS1, TITF1, SEQ ID NO: 42, DDX51, SEQ ID NO: 117, SEQ ID NO: 46, O60279, and SEQ ID NO: 48 as markers for the detection of breast cancer cells within blood or blood derived fluids by differentiation of breast cancer cells from peripheral blood lymphocytes. Said use of the genes and/or sequences may be enabled by means of any analysis of the expression of the gene, by means of mRNA expression analysis or protein expression analysis. However, in the most preferred embodiment of the invention, the detection of breast cell proliferative disorders is enabled by means of analysis of the methylation status of said genes or genomic sequences and their promoter or regulatory elements. Methods for the methylation analysis of genes are described herein.

In said embodiment it is further preferred that the expression level of only one gene or genomic sequence from the group consisting FABP3, RASSF1A, MSF, PRDM6, LMX1A, SEQ ID NO: 4, SCGB3A1, SLIT2, NR2E1, EYA4, PRDM2, SERPINB5, TWIST, STAT1, ALX4, IGFBP7, DAPK1, THBS1, PLAU, SEQ ID NO: 20, SEQ ID NO: 38, SEQ ID NO: 8, SEQ ID NO: 37, SEQ ID NO: 10, SEQ ID NO: 35, SEQ ID NO: 47, SEQ ID NO: 6, LIMK-1 and SEQ ID NO: 46 is analyzed for the detection of breast cancer cells within blood or blood derived fluids by differentiation of breast cancer cells from peripheral blood lymphocytes. Said use of the genes and/or sequences may be enabled by means of any analysis of the expression of the gene, by means of mRNA expression analysis or protein expression analysis. However, in the most preferred embodiment of the invention, the detection of breast cell proliferative disorders is enabled by means of analysis of the methylation status of said genes or genomic sequences and their promoter or regulatory elements. Methods for the methylation analysis of genes are described herein.

In one embodiment the method discloses the use of one or more genes or genomic sequences selected from the group consisting of APC, ARH1/NOEY2, CCND2, CDKN1A, CDKN2A, SEQ ID NO: 9, SEQ ID NO: 2, EYA4, FHIT, GSTP1, HIC1, IGFBP7, MLH1, PGR, SERPINB5, RARB, SOD2, PERT, TGFBR2, THRB, TIMP3, TP73, CDH13, THBS1, TMS1/ASC, ESR1, APAF1, CASP8, SYK, HOXA5, FABP3, RASSF1A, SEQ ID NO: 3, RARA, TWIST, ESR2, PLAU, SEQ ID NO: 4, SNCG, SLC19A1, GJB2, SLIT2, IGSF4, MCT1, HS3ST2, PRDM2, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 8, SCGB3A1, PROSTAGLANDIN E2 RECEPTOR, EP4 SUBTYPE (PROSTANOID EP4 RECEPTOR) (PGE RECEPTOR, EP4 SUBTYPE), ORPHAN NUCLEAR RECEPTOR NR5A2 (ALPHA-1-FETOPROTEIN TRANSCRIPTION FACTOR) (HEPATOCYTIC TRANSCRIPTION FACTOR) (B1-BINDING FACTOR) (HB1F) (CYP7A PROMO BINDING FACTOR), LIM DOMAIN KINASE 1, SASH1, S100A7, BCL11B, SEQ ID NO: 51, MGC34831, SEQ ID NO: 54, PDLIM1, MSF, SEQ ID NO: 14, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 18, SEQ ID NO: 19, NR2E1, PCDH7, DKK3, RTTN, SNAP25, GIRK2, SEQ ID NO: 28, SEQ ID NO: 29, ARL7, SEQ ID NO: 31, THH, HOXB13, SEQ ID NO: 36, LMX1A, SENP3, TITF1, SEQ ID NO: 42, DDX51, SEQ ID NO: 117, SEQ ID NO: 46, O60279, and SEQ ID NO: 48 as markers for the differentiation of DCIS from benign breast disorders. The term “benign breast disorders” as used herein shall be taken to include healthy breast tissue, fibroadenoma, fibrocystic disease and atypical ductal hyperplasia. Said use of the genes and/or sequences may be enabled by means of any analysis of the expression of the gene, by means of mRNA expression analysis or protein expression analysis. However, in the most preferred embodiment of the invention, the detection of breast cell proliferative disorders is enabled by means of analysis of the methylation status of said genes or genomic sequences and their promoter or regulatory elements. Methods for the methylation analysis of genes are described herein.

It is also preferred that the expression level of only one gene or genomic sequence from the group consisting HS3ST2, SLIT2, RASSF1A, GSTP1, GJB2, IGFBP7, CDH13, ARH1/NOEY2, SCGB3A1, FHIT, SEQ ID NO: 27, LIMK-1, SEQ ID NO: 46, SEQ ID NO: 3, SEQ ID NO: 117, SEQ ID NO: 48, SEQ ID NO: 41, SEQ ID NO: 4, SEQ ID NO: 6, and SEQ ID NO: 24 is analyzed. It is particularly preferred that this is carried out by means of methylation analysis.

In one embodiment the method discloses the use of one or more genes or genomic sequences selected from the group consisting of ARH1/NOEY2, CCND2, CDKN1A, CDKN2A, SEQ ID NO: 9, DAPK1, SEQ ID NO: 2, EYA4, FHIT, GSTP1, HIC1, IGFBP7, SERPINB5, TERT, TGFBR2, THRB, TIMP3, TP73, NME1, CDH13, THBS1, TMS1/ASC, IL6, APAF1, SYK, HOXA5, FABP3, RASSF1A, SEQ ID NO: 3, TWIST, ESR2, PLAU, STAT1, SEQ ID NO: 4, LOT1, GPC3, CLDN7, GJB2, SLIT2, IGSF4, MCT1, PRDM2, ALX4, SEQ ID NO: 5, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 8, SCGB3A1, SEQ ID NO: 1, PROSTAGLANDIN E2 RECEPTOR, EP4 SUBTYPE (PROSTANOID EP4 RECEPTOR) (PGE RECEPTOR, EP4 SUBTYPE), ORPHAN NUCLEAR RECEPTOR NR5A2 (ALPHA-1-FETOPROTEIN TRANSCRIPTION FACTOR) (HEPATOCYTIC TRANSCRIPTION FACTOR) (B1-BINDING FACTOR) (HB1F) (CYP7A PROMOTER BINDING FACTOR), LIM DOMAIN KINASE 1, BCL11B, SEQ ID NO: 51, MGC34831, SEQ ID NO: 54, PDLIM1, MSF, SEQ ID NO: 14, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 18, SEQ ID NO: 19, PRDM6, NR2E1, PCDH7, DKK3, RTTN, SNAP25, SEQ ID NO: 26, GIRK2, SEQ ID NO: 28, SEQ ID NO: 29, ARL7, SEQ ID NO: 31, THH, HOXB13, SEQ ID NO: 35, SEQ ID NO: 36, MGC10561, LMX1A, SENP3, GS1, TITF1, SEQ ID NO: 42, DDX51, SEQ ID NO: 117, SEQ ID NO: 45, SEQ ID NO: 46, O60279, and SEQ ID NO: 48 as markers for the differentiation of breast cancer from benign breast disorders. The term benign breast disorders as used herein shall be taken to include healthy breast tissue, fibroadenoma, fibrocystic disease and atypical ductal hyperplasia. Said use of the genes and/or sequences may be enabled by means of any analysis of the expression of the gene, by means of mRNA expression analysis or protein expression analysis. However, in the most preferred embodiment of the invention, the detection of breast cell proliferative disorders is enabled by means of analysis of the methylation status of said genes or genomic sequences and their promoter or regulatory elements. Methods for the methylation analysis of genes are described herein.

It is also preferred that the expression level of only one gene or genomic sequence from the group consisting SLIT2, HS3ST2, HOXA5, ARH1/NOEY2, IGFBP7, PLAU, CDH13, TIMP3, CCND2, GSTP1, SEQ ID NO: 117, LIMK-1, SEQ ID NO: 46, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 3, SEQ ID NO: 41, SEQ ID NO: 27, SEQ ID NO: 31, and SEQ ID NO: 4 is analyzed. It is particularly preferred that this is carried out by means of methylation analysis.

Aberrant levels of mRNA expression of the genes, genomic sequences or genes regulated by genomic sequences according to Table 3 are associated with breast cell proliferative disorders. Accordingly, decreased levels of expression of said all of said genes or sequences with the exception of PRDM2 and S100A7 are associable with the development of breast cancers and other breast cell proliferative disorders. Increased levels of expression of PRDM2 and S100A7 are associable with the development of breast cancers and other breast cell proliferative disorders.

To detect the presence of mRNA encoding a gene or genomic sequence in a detection system for breast cancer, a sample is obtained from a patient. The sample can be a tissue biopsy sample or a sample of blood, plasma, serum or the like. The sample may be treated to extract the nucleic acids contained therein. The resulting nucleic acid from the sample is subjected to gel electrophoresis or other separation techniques. Detection involves contacting the nucleic acids and in particular the mRNA of the sample with a DNA sequence serving as a probe to form hybrid duplexes. The stringency of hybridization is determined by a number of factors during hybridization and during the washing procedure, including temperature, ionic strength, length of time and concentration of form amide. These factors are outlined in, for example, Sambrook et al. (Molecular Cloning: A Laboratory Manual, 2d ed., 1989). Detection of the resulting duplex is usually accomplished by the use of labeled probes. Alternatively, the probe may be unlabeled, but may be detectable by specific binding with a ligand which is labeled, either directly or indirectly. Suitable labels and methods for labeling probes and ligands are known in the art, and include, for example, radioactive labels which may be incorporated by known methods (e.g., nick translation or kinasing), biotin, fluorescent groups, chemiluminescent groups (e.g., dioxetanes, particularly triggered dioxetanes), enzymes, antibodies, and the like.

In order to increase the sensitivity of the detection in a sample of mRNA transcribed from the gene or genomic sequence, the technique of reverse transcription/polymerization chain reaction can be used to amplify cDNA transcribed from the mRNA. The method of reverse transcription/PCR is well known in the art (for example, see Watson and Fleming, supra).

The reverse transcription/PCR method can be performed as follows. Total cellular RNA is isolated by, for example, the standard guanidium isothiocyanate method and the total RNA is reverse transcribed. The reverse transcription method involves synthesis of DNA on a template of RNA using a reverse transcriptase enzyme and a 3′ end primer. Typically, the primer contains an oligo(dT) sequence. The cDNA thus produced is then amplified using the PCR method and specific primers. (Belyavsky et al, Nucl Acid. Res 17:2919-2932, 1989; Krug and Berger, Methods in Enzymology, Academic Press, N.Y., Vol. 152, pp. 316-325, 1987 which are incorporated by reference)

The present invention may also be described in certain embodiments as a kit for use in detecting a breast cell proliferative disorder state through testing of a biological sample. A representative kit may comprise one or more nucleic acid segments that selectively hybridize to the mRNA and a container for each of the one or more nucleic acid segments. In certain embodiments the nucleic acid segments may be combined in a single tube. In further embodiments, the nucleic acid segments may also include a pair of primers for amplifying the target mRNA. Such kits may also include any buffers, solutions, solvents, enzymes, nucleotides, or other components for hybridization, amplification or detection reactions. Preferred kit components include reagents for reverse transcription-PCR, hybridization, Northern analysis and/or RPA

The present invention further provides for methods to detect the presence of the polypeptide encoded by said genes or gene sequences in a sample obtained from a patient.

Aberrant levels of polypeptide expression of the polypeptides encoded by the genes, genomic sequences or genes regulated by genomic sequences of the group consisting all genes and genomic sequences of genomic regions listed in Table 3 are associated with breast carcinoma. Accordingly over expression of said polypeptides with the exception of polypeptides encoded by the PRDM2 and S100A7 genes are associable with the development of breast carcinoma and other breast cell proliferative disorders. Under expression of PRDM2 and S100A7 are associable with the development of breast cancers and other breast cell proliferative disorders.

Any method known in the art for detecting proteins can be used. Such methods include, but are not limited to immunodiffusion, immunoelectrophoresis, immunochemical methods, binder-ligand assays, immunohistochemical techniques, agglutination and complement assays. (for example see Basic and Clinical Immunology, Sites and Terr, eds., Appleton and Lange, Norwalk, Conn. pp 217-262, 1991 which is incorporated by reference). Preferred are binder-ligand immunoassay methods including reacting antibodies with an epitope or epitopes and competitively displacing a labeled protein or derivative thereof.

Certain embodiments of the present invention comprise the use of antibodies specific to the polypeptide encoded by the genes or genomic sequences of the group consisting all genes and genomic sequences of genomic regions as listed in Table 3, below.

Such antibodies may be useful for diagnostic and prognostic applications in detecting the disease state, by comparing a patient's levels of breast disease marker expression to expression of the same markers in normal individuals. In certain embodiments production of monoclonal or polyclonal antibodies can be induced by the use of the coded polypeptide as antigene. Such antibodies may in turn be used to detect expressed proteins as markers for human disease states. The levels of such proteins present in the peripheral blood or tissue sample of a patient may be quantified by conventional methods. Antibody-protein binding may be detected and quantified by a variety of means known in the art, such as labeling with fluorescent or radioactive ligands. The invention further comprises kits for performing the above-mentioned procedures, wherein such kits contain antibodies specific for the investigated polypeptides.

Numerous competitive and non-competitive protein binding immunoassays are well known in the art. Antibodies employed in such assays may be unlabeled, for example as used in agglutination tests, or labeled for use a wide variety of assay methods. Labels that can be used include radionuclides, enzymes, fluorescers, chemiluminescers, enzyme substrates or co-factors, enzyme inhibitors, particles, dyes and the like for use in radioimmunoassay (RIA), enzyme immunoassays, e.g., enzyme-linked immunosorbent assay (ELISA), fluorescent immunoassays and the like. Polyclonal or monoclonal antibodies or epitopes thereof can be made for use in immunoassays by any of a number of methods known in the art. One approach for preparing antibodies to a protein is the selection and preparation of an amino acid sequence of all or part of the protein, chemically synthesizing the sequence and injecting it into an appropriate animal, usually a rabbit or a mouse (Milstein and Kohler Nature 256:495-497, 1975; Gulfre and Milstein, Methods in Enzymology: Immunochemical Techniques 73:1-46, Langone and Banatis eds., Academic Press, 1981 which are incorporated by reference). Methods for preparation of the polypeptides or epitopes thereof include, but are not limited to chemical synthesis, recombinant DNA techniques or isolation from biological samples.

In a further embodiment the present invention is based upon the analysis of methylation levels within two or more genes or genomic sequences taken from the group consisting all genes and genomic sequences of genomic regions listed in Table 3 and/or their regulatory sequences. It is further preferred that the sequences of said genes or genomic sequences are as according to SEQ ID NO: 1 to SEQ ID NO: 118.

Particular embodiments of the present invention provide a novel application of the analysis of methylation status, levels and/or patterns within said sequences that enables a precise detection and/or characterization of breast cell proliferative disorders. Early detection of breast cell proliferative disorders is directly linked with disease prognosis, and the disclosed method thereby enables the physician and patient to make early and more informed treatment decisions.

Further Improvements

The present invention provides novel uses for genomic sequences selected from the group consisting of SEQ ID NO: 1 to SEQ ID NO: 118. Additional embodiments provide modified variants, in particular chemically modified variants, of SEQ ID NO: 1 to SEQ ID NO: 118, as well as oligonucleotides and/or PNA-oligomers for analysis of cytosine methylation patterns within the group consisting SEQ ID NO: 1 to SEQ ID NO: 118.

An objective of the invention comprises analysis of the methylation state of one or more CpG dinucleotides within at least one of the genomic sequences selected from the group consisting of SEQ ID NO: 1 to SEQ ID NO: 118 and sequences complementary thereto.

The disclosed invention provides treated nucleic acids, derived from genomic SEQ ID NO: 1 to SEQ ID NO: 118, wherein the treatment is suitable to convert at least one unmethylated cytosine base of the genomic DNA sequence to uracil or another base that is detectably dissimilar to cytosine in terms of hybridization. The genomic sequences in question may comprise one, or more, consecutive or random methylated CpG positions. Said treatment preferably comprises use of a reagent selected from the group consisting of bisulfate, hydrogen sulfite, disulfite, and combinations thereof. In a preferred embodiment the invention provides a non-naturally occurring modified nucleic acid comprising a sequence of at least 16 contiguous nucleotide bases in length of a sequence selected from the group consisting of SEQ ID NO: 493 TO SEQ ID NO: 964, wherein said sequence comprises at least one CpG, TpA or CpA dinucleotide and sequences complementary thereto, The sequences of SEQ ID NO: 493 TO SEQ ID NO: 964 provide non-naturally occurring modified versions of the nucleic acid according to SEQ ID NO: 1 to SEQ ID NO: 118, wherein the modification of each genomic sequence results in the synthesis of a nucleic acid having a sequence that is unique and distinct from said genomic sequence as follows. Particularly preferred is a nucleic acid comprising a sequence that is not identical to a part of human genomic DNA, including human genomic DNA comprising one or more methylated CpG positions.

For each sense strand genomic DNA, e.g., SEQ ID NO: 1, four converted versions are disclosed. A first version wherein “C” is converted to “T,” but “CpG” remains “CpG” (i.e., corresponds to case where, for the genomic sequence, all “C” residues of CpG dinucleotide sequences are methylated and are thus not converted); a second version discloses the complement of the disclosed genomic DNA sequence (i.e. antisense strand), wherein “C” is converted to “T,” but “CpG” remains “CpG” (i.e., corresponds to case where, for all “C” residues of CpG dinucleotide sequences are methylated and are thus not converted). The ‘upmethylated’ converted sequences of SEQ ID NO: 1 to SEQ ID NO: 118 correspond to SEQ ID NO: 493 to SEQ ID NO: 728. A third chemically converted version of each genomic sequences is provided, wherein “C” is converted to “T” for all “C” residues, including those of “CpG” dinucleotide sequences (i.e., corresponds to case where, for the genomic sequences, all “C” residues of CpG dinucleotide sequences are unmethylated); a final chemically converted version of each sequence, discloses the complement of the disclosed genomic DNA sequence (i.e. antisense strand), wherein “C” is converted to “T” for all “C” residues, including those of “CpG” dinucleotide sequences (i.e., corresponds to case where, for the complement (antisense strand) of each genomic sequence, all “C” residues of CpG dinucleotide sequences are unmethylated), The ‘downmethylated’ converted sequences of SEQ ID NO: 1 to SEQ ID NO: 118 correspond to SEQ ID NO: 729 to SEQ ID NO: 964.

In an alternative preferred embodiment, the method according to the invention comprises the use of an oligonucleotide or oligomer for detecting the cytosine methylation state within genomic or treated (chemically modified) DNA, according to SEQ ID NO: 1 to SEQ ID NO: 964. Said oligonucleotide or oligomer comprising a nucleic acid sequence having a length of at least nine (9) nucleotides which hybridizes, under moderately stringent or stringent conditions (as defined herein above), to a treated nucleic acid sequence according to SEQ ID NO: 493 to SEQ ID NO: 964 and/or sequences complementary thereto, or to a genomic sequence according to SEQ ID NO: 1 to SEQ ID NO: 118 and/or sequences complementary thereto.

Thus, the present invention provides nucleic acid molecules (e.g., oligonucleotides and peptide nucleic acid (PNA) molecules (PNA-oligomers) having a length of at least nine (9) nucleotides that hybridize under moderately stringent and/or stringent hybridization conditions to all or a portion of the sequences SEQ ID NO: 1 to SEQ ID NO: 964, or to the complements thereof.

Particularly preferred are oligonucleotides and peptide nucleic acid (PNA) molecules that hybridize under moderately stringent and/or stringent hybridization conditions to all or a portion of the sequences SEQ ID NO: 493 to SEQ ID NO: 964, or to the complements thereof wherein said sequence comprises at least one CpG, TpA or CpA dinucleotide and furthermore wherein said sequence is not identical to a part of human genomic DNA, including human genomic DNA comprising one or more methylated CpG positions.

The hybridizing portion of the hybridizing nucleic acids is typically at least 9, 15, 20, 25, 30 or 35 nucleotides in length. However, longer molecules have inventive utility, and are thus within the scope of the present invention.

Preferably, the hybridizing portion of the inventive hybridizing nucleic acids is at least 95%, or at least 98%, or 100% identical to the sequence, or to a portion thereof of SEQ ID NO: 1 to SEQ ID NO: 964, or to the complements thereof.

Hybridizing nucleic acids of the type described herein can be used, for example, as a primer (e.g., a PCR primer), or a diagnostic and/or prognostic probe or primer. Preferably, hybridization of the oligonucleotide probe to a nucleic acid sample is performed under stringent conditions and the probe is 100% identical to the target sequence. Nucleic acid duplex or hybrid stability is expressed as the melting temperature or Tm, which is the temperature at which a probe dissociates from a target DNA. This melting temperature is used to define the required stringency conditions.

For target sequences that are related and substantially identical to the corresponding sequence of SEQ ID NO: 1 to SEQ ID NO: 964 (such as allelic variants and SNPs), rather than identical, it is useful to first establish the lowest temperature at which only homologous hybridization occurs with a particular concentration of salt (e.g., SSC or SSPE). Then, assuming that 1% mismatching results in a 1° C. decrease in the Tm, the temperature of the final wash in the hybridization reaction is reduced accordingly (for example, if sequences having >95% identity with the probe are sought, the final wash temperature is decreased by 5° C.). In practice, the change in Tm can be between 0.5° C. and 1.5° C. per 1% mismatch.

Examples of inventive oligonucleotides of length X (in nucleotides), as indicated by polynucleotide positions with reference to, e.g., SEQ ID NO: 1, include those corresponding to sets (sense and antisense sets) of consecutively overlapping oligonucleotides of length X, where the oligonucleotides within each consecutively overlapping set (corresponding to a given X value) are defined as the finite set of Z oligonucleotides from nucleotide positions:

n to (n+(X−1));where n=1, 2, 3, . . . (Y−(X−1));where Y equals the length (nucleotides or base pairs) of SEQ ID NO: 1 (6435);where X equals the common length (in nucleotides) of each oligonucleotide in the set (e.g., X=20 for a set of consecutively overlapping 20-mers); andwhere the number (Z) of consecutively overlapping oligomers of length X for a given SEQ ID NO of length Y is equal to Y−(X−1).

For example Z=6435−19=6416 for either sense or antisense sets of SEQ ID NO: 1, where X=20.

Examples of inventive 20-mer oligonucleotides include the following set of 6416 oligomers (and the antisense set complementary thereto), indicated by polynucleotide positions with reference to SEQ ID NO: 1:1-20, 2-21, 3-22, 4-23, 5-24, etc. . . . 6416-6435.

Likewise, examples of inventive 25-mer oligonucleotides include the following set of 6410 oligomers (and the antisense set complementary thereto), indicated by polynucleotide positions with reference to SEQ ID NO: 1:1-25, 2-26, 3-27, 4-28, 5-29, etc. . . . 6408-6433, 6409-6434 and 6410-6435.

Preferably, the set is limited to those oligomers that comprise at least one CpG, TpG or CpA dinucleotide.

The present invention encompasses, for each of SEQ ID NO: 1 to SEQ ID NO: 964 (sense and antisense), multiple consecutively overlapping sets of oligonucleotides or modified oligonucleotides of length X, where, e.g., X=9, 10, 17, 20, 22, 23, 25, 27, 30 or 35 nucleotides.

The oligonucleotides or oligomers according to the present invention constitute effective tools useful to ascertain genetic and epigenetic parameters of the genomic sequence corresponding to SEQ ID NO: 1 to SEQ ID NO: 118. Preferred sets of such oligonucleotides or modified oligonucleotides of length X are those consecutively overlapping sets of oligomers corresponding to SEQ ID NO: 1 to SEQ ID NO: 964 (and to the complements thereof). Preferably, said oligomers comprise at least one CpG, TpG or CpA dinucleotide.

Particularly preferred oligonucleotides or oligomers according to the present invention are those in which the cytosine of the CpG dinucleotide (or of the corresponding converted TpG or CpA dinculeotide) sequences is within the middle third of the oligonucleotide; that is, where the oligonucleotide is, for example, 13 bases in length, the CpG, TpG or CpA dinucleotide is positioned within the fifth to ninth nucleotide from the 5′-end.

The oligonucleotides of the invention can also be modified by chemically linking the oligonucleotide to one or more moieties or conjugates to enhance the activity, stability or detection of the oligonucleotide. Such moieties or conjugates include chromophores, fluorophors, lipids such as cholesterol, cholic acid, thioether, aliphatic chains, phospholipids, polyamines, polyethylene glycol (PEG), palmityl moieties, and others as disclosed in, for example, U.S. Pat. Nos. 5,514,758, 5,565,552, 5,567,810, 5,574,142, 5,585,481, 5,587,371, 5,597,696 and 5,958,773. The probes may also exist in the form of a PNA (peptide nucleic acid) which has particularly preferred pairing properties. Thus, the oligonucleotide may include other appended groups such as peptides, and may include hybridization-triggered cleavage agents (Krol et al., Biotechniques 6:958-976, 1988) or intercalating agents (Zon, Pharm. Res. 5:539-549, 1988). To this end, the oligonucleotide may be conjugated to another molecule, e.g., a chromophore, fluorophore, peptide, hybridization-triggered cross-linking agent, transport agent, hybridization-triggered cleavage agent, etc.

The oligonucleotide may also comprise at least one art-recognized modified sugar and/or base moiety, or may comprise a modified backbone or non-natural internucleoside linkage.

The oligonucleotides or oligomers according to particular embodiments of the present invention are typically used in ‘sets,’ which contain at least one oligomer for analysis of each of the CpG dinucleotides of genomic sequences SEQ ID NO: 1 to SEQ ID NO: 118 and sequences complementary thereto, or to the corresponding CpG, TpG or CpA dinucleotide within a sequence of the treated nucleic acids according to SEQ ID NO: 493 to SEQ ID NO: 964 and sequences complementary thereto. However, it is anticipated that for economic or other factors it may be preferable to analyze a limited selection of the CpG dinucleotides within said sequences, and the content of the set of oligonucleotides is altered accordingly.

Therefore, in particular embodiments, the present invention provides a set of at least two (2) (oligonucleotides and/or PNA-oligomers) useful for detecting the cytosine methylation state in treated genomic DNA (SEQ ID NO: 493 to SEQ ID NO: 964), or in genomic DNA (SEQ ID NO: 1 to SEQ ID NO: 118 and sequences complementary thereto). These probes enable diagnosis and/or classification of genetic and epigenetic parameters of breast cell proliferative disorders. The set of oligomers may also be used for detecting single nucleotide polymorphisms (SNPs) in treated genomic DNA (SEQ ID NO: 493 to SEQ ID NO: 964), or in genomic DNA (SEQ ID NO: 1 to SEQ ID NO: 118 and sequences complementary thereto).

In preferred embodiments, at least one, and more preferably all members of a set of oligonucleotides is/are bound to a solid phase.

In further embodiments, the present invention provides a set of at least two (2) oligonucleotides that are used as ‘primer’ oligonucleotides for amplifying DNA sequences of one of SEQ ID NO: 1-118 and SEQ ID NO: 493 to SEQ ID NO: 964 and sequences complementary thereto, or segments thereof.

It is anticipated that the oligonucleotides may constitute all or part of an “array” or “DNA chip” (i.e., an arrangement of different oligonucleotides and/or PNA-oligomers bound to a solid phase). Such an array of different oligonucleotide- and/or PNA-oligomer sequences can be characterized, for example, in that it is arranged on the solid phase in the form of a rectangular or hexagonal lattice. The solid-phase surface may be composed of silicon, glass, polystyrene, aluminum, steel, iron, copper, nickel, silver, or gold. Nitrocellulose as well as plastics such as nylon, which can exist in the form of pellets or also as resin matrices, may also be used. An overview of the Prior Art in oligomer array manufacturing can be gathered from a special edition of Nature Genetics (Nature Genetics Supplement, Volume 21, January 1999, and from the literature cited therein). Fluorescently labeled probes are often used for the scanning of immobilized DNA arrays. The simple attachment of Cy3 and Cy5 dyes to the 5′-OH of the specific probe are particularly suitable for fluorescence labels. The detection of the fluorescence of the hybridized probes may be carried out, for example, via a confocal microscope. Cy3 and Cy5 dyes, besides many others, are commercially available.

It is also anticipated that the oligonucleotides, or particular sequences thereof, may constitute all or part of an “virtual array” wherein the oligonucleotides, or particular sequences thereof; are used, for example, as ‘specifiers’ as part of; or in combination with a diverse population of unique labeled probes to analyze a complex mixture of analytes. Such a Method, for example is described in US 2003/0013091 (U.S. Ser. No. 09/898,743, published 16 Jan. 2003). In such methods, enough labels are generated so that each nucleic acid in the complex mixture (i.e., each analyte) can be uniquely bound by a unique label and thus detected (each label is directly counted, resulting in a digital read-out of each molecular species in the mixture).

It is particularly preferred that the oligomers according to the invention are utilized for at least one of: detection of; detection and differentiation between or among subclasses of; diagnosis of; prognosis of; treatment of; monitoring of; and treatment and monitoring of breast cell proliferative disorders. This is enabled by use of said sets for the differentiation and/or detection of the tissue types according to Table 14. Particularly preferred are those sets of oligomer that comprise at least two oligonucleotides selected from one of the following sets of oligonucleotides.

In one embodiment of the method, breast cancer tissue is detected. This is achieved by analysis of the CpG methylation status of at least one target sequence comprising, or hybridizing under stringent conditions to at least 16 contiguous nucleotides of a gene or sequence selected from the group consisting of APC, ARH1/NOEY2, BRCA2, CCND2, CDKN1A, CDKN2A, SEQ ID NO: 9, DAPK1, SEQ ID NO: 2, EYA4, FHIT, GSTP1, HIC1, IGFBP7, MLH1, PGR, SERPINB5, RARB, SFN, SOD2, TGFBR2, THRB, TIMP3, TP73, NME1, CDH13, THBS1, TMS1/ASC, ESR1, IL6, APAF1, CASP8, SYK, HOXA5, FABP3, RASSF1A, SEQ ID NO: 3, RARA, TWIST, ESR2, PLAU, STAT1, SEQ ID NO: 4, BRCA1, LOT1, PRSS8, SNCG, TPM1, GPC3, CLDN7, SLC19A1, GJB2, SLIT2, IGSF4, MCT1, HS3ST2, PRDM2, ALX4, SEQ ID NO: 5, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 8, SCGB3A1, SEQ ID NO: 1, PROSTAGLANDIN E2 RECEPTOR, EP4 SUBTYPE (PROSTANOID EP4 RECEPTOR) (PGE RECEPTOR, EP4 SUBTYPE), ORPHAN NUCLEAR RECEPTOR NR5A2 (ALPHA-1-FETOPROTEIN TRANSCRIPTION FACTOR) (HEPATOCYTIC TRANSCRIPTION FACTOR) (B1-BINDING FACTOR) (HB1F) (CYP7A PROMOTER BINDING FACTOR), LIM DOMAIN KINASE 1, SASH1, S100A7, BCL11B, SEQ ID NO: 51, MGC34831, SEQ ID NO: 54, PDLIM1, MSF, SEQ ID NO: 14, SEQ ID NO: 15, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 18, SEQ ID NO: 19, PRDM6, RAP2B, NR2E1, PCDH7, DKK3, RTTN, SNAP25, SEQ ID NO: 26, GIRK2, SEQ ID NO: 28, SEQ ID NO: 29, ARL7, SEQ ID NO: 31, THH, HOXB13, SEQ ID NO: 35, MGC10561, LMX1A, SENP3, GS1, TITF1, SEQ ID NO: 42, DDX51, SEQ ID NO: 117, SEQ ID NO: 45, SEQ ID NO: 46, O60279, and SEQ ID NO: 48 and complements thereof.

In a further embodiment the CpG methylation status of at least one target sequence comprising, or hybridizing under stringent conditions to at least 16 contiguous nucleotides of a gene or sequence selected from the group consisting of PRDM2, PLAU, GSTP1, SLIT2, CCND2, HOXA5, RASSF1A, HS3ST2, ARH1/NOEY2, SCGB3A1, LIMK-1, SEQ ID NO: 6, SEQ ID NO: 3, SEQ ID NO: 18, SEQ ID NO: 7, SEQ ID NO: 41, SEQ ID NO: 22, SEQ ID NO: 46, SEQ ID NO: 13, and SEQ ID NO: 31 and complements thereof.

In both cases this is preferably achieved by use of a set consisting of at least one oligonucleotide, and more preferably at least two selected from one of the groups consisting of 1475-1477, 1477, 1478, 1478, 1479, 1479, 1480, 1480-1497, 1497, 1498, 1498, 1499, 1499, 1500, 1500, 1501, 1501, 1502, 1502-1511, 1511, 1512, 1512-1527, 1527, 1528, 1528-1557, 1557, 1558, 1558-1567, 1567, 1568, 1568, 1569, 1569, 1570, 1570-1573, 1573, 1574, 1574-1607, 1607, 1608, 1608-1619, 1619, 1620, 1620-1623, 1623, 1624, 1624-1639, 1639, 1640, 1640-1655, 1655, 1656, 1656-1693, 1693, 1694, 1694, 1695, 1695, 1696, 1696, 1697, 1697-1702, 1702, 1703, 1703-1706, 1706, 1706, 1706, 1707-1720, 1720, 1721, 1721-1724, 1724, 1725, 1725-1728, 1728, 1729, 1729-1734, 1734, 1735, 1735-1738, 1738, 1739, 1739-1752, 1752, 1753, 1753-1758, 1758, 1759, 1759′-1762, 1762, 1763, 1763-1770, 1770, 1771, 1771-1778, 1778, 1779, 1779, 1780, 1780, 1781, 1781-1790, 1790, 1791, 1791-1798, 1798, 1799, 1799-1838, 1838, 1839, 1839, 1840, 1840, 1841, 1841-1852, 1852, 1853, 1853, 1854, 1854, 1855, 1855-1870, 1870, 1871, 1871-1874, 1874, 1875, 1875-1878, 1878, 1879, 1879, 1880, 1880, 1881, 1881, 1882, 1882, 1883, 1883-1886, 1886, 1887, 1887-1890, 1890, 1891, 1891-1906, 1906, 1907, 1907-1940, 1940, 1941, 1941, 1942, 1942, 1943, 1943-1946, 1946, 1947, 1947-1952, 1952, 1953, 1953-1966, 1966, 1967, 1967, 1968, 1968, 1969, 1969, 1970, 1970, 1971, 1971-1978, 1978, 1979, 1979-1982, 1982, 1983, 1983-1992, 1992, 1993, 1993-1998, 1998, 1999, 1999-2006, 2006, 2007, 2007-2016, 2016, 2017, 2017-2022, 2022, 2023, 2023-2030, 2030, 2031, 2031-2036, 2036, 2037, 2037-2050, 2050, 2051, 2051-2060, 2060, 2061, 2061-2070, 2070, 2071, 2071-2076, 2076, 2077, 2077-2104, 2104, 2105, 2105, 2106, 2106, 2107, 2107-2114, 2114, 2115, 2115-2128, 2128, 2129, 2129, 2130, 2130, 2131, 2131-2134, 2134, 2135, 2135, 2136, 2136, 2137, 2137, 2138, 2138, 2139, and 2139.

In one embodiment of the method, breast cancer tissue is differentiated from other cancers. This is achieved by analysis of the CpG methylation status of at least one target sequence comprising, or hybridizing under stringent conditions to at least 16 contiguous nucleotides of a gene or sequence selected from the group consisting of APC, ARH1/NOEY2, BRCA2, CCND2, CDKN1A, CDKN2A, SEQ ID NO: 9, DAPK1, SEQ ID NO: 2, EYA4, FHIT, GSTP1, HIC1, IGFBP7, MLH1, PGR, SERPINB5, RARB, SFN, S002, TGFBR2, THRB, TIMP3, TP73, NME1, CDH13, THBS1, TMS1/ASC, ESR1, IL6, APAF1, CASP8, SYK, HOXA5, FABP3, RASSF1A, SEQ ID NO: 3, RARA, TWIST, ESR2, PLAU, STAT1, SEQ ID NO: 4, BRCA1, LOT1, PRSS8, SNCG, TPM1, GPC3, CLDN7, SLC19A1, GJB2, SLIT2, IGSF4, MCT1, HS3ST2, PRDM2, ALX4, SEQ ID NO: 5, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 8, SCGB3A1, SEQ ID NO: 1, PROSTAGLANDIN E2 RECEPTOR, EP4 SUBTYPE (PROSTANOID EP4 RECEPTOR) (PGE RECEPTOR, EP4 SUBTYPE), ORPHAN NUCLEAR RECEPTOR NR5A2 (ALPHA-1-FETOPROTEIN TRANSCRIPTION FACTOR) (HEPATOCYTIC TRANSCRIPTION FACTOR) (B1-BINDING FACTOR) (HB1F) (CYP7A PROMOTER BINDING FACTOR), LIM DOMAIN KINASE 1, SASH1, S100A7, BCL11B, SEQ ID NO: 51, MGC34831, SEQ ID NO: 54, PDLIM1, MSF, SEQ ID NO: 14, SEQ ID NO: 15, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 18, SEQ ID NO: 19, PRDM6, RAP2B, NR2E1, PCDH7, DKK3, RTTN, SNAP25, SEQ ID NO: 26, GIRK2, SEQ ID NO: 28, SEQ ID NO: 29, ARL7, SEQ ID NO: 31, THH, HOXB13, SEQ ID NO: 35, MGC10561, LMX1A, SENP3, GS1, TITF1, SEQ ID NO: 42, DDX51, SEQ ID NO: 117, SEQ ID NO: 45, SEQ ID NO: 46, O60279, and SEQ ID NO: 48 and complements thereof. In a further embodiment the CpG methylation status of at least one target sequence comprising, or hybridizing under stringent conditions to at least 16 contiguous nucleotides of a gene or sequence selected from the group consisting PRDM2, GSTP1, ALX4, HOXA5, PLAU, RASSF1A, IGSF4, SLIT2, DAPK1, CDKN1A, SEQ ID NO: 38, SEQ ID NO: 35, LIMK-1, SEQ ID NO: 39, SEQ ID NO: 10, SEQ ID NO: 26, SEQ ID NO: 8, SEQ ID NO: 22, SEQ ID NO: 18, and SEQ ID NO: 47 and complements thereof.

In both cases this is preferably achieved by use of a set consisting of at least one oligonucleotide, and more preferably at least two selected from one of the groups consisting of 1475, 1476, 1485-1497, 1497, 1498, 1498, 1499, 1499, 1500, 1500, 1501, 1501, 1502, 1502-1504, 1509-1511, 1511, 1512, 1512-1522, 1525-1527, 1527, 1528, 1528-1540, 1551-1554, 1569, 1569, 1570, 1570-1573, 1573, 1574, 1574-1580, 1585, 1586, 1591-1600, 1603, 1604, 1609-1619, 1619, 1620, 1620-1623, 1623, 1624, 1624-1626, 1629, 1630, 1633-1639, 1639, 1640, 1640-1642, 1649, 1650, 1667, 1668, 1675-1680, 1683-1688, 1710-1717, 1724, 1724, 1725, 1725-1728, 1728, 1729, 1729-1731, 1736-1738, 1738, 1739, 1739, 1748, 1749, 1752, 1752, 1753, 1753, 1760, 1761, 1764, 1765, 1774-1778, 1778, 1779, 1779, 1780, 1780, 1781, 1781-1783, 1788, 1789, 1792-1798, 1798, 1799, 1799-1801, 1804-1819, 1830, 1831, 1858-1865, 1870, 1870, 1871, 1871, 1874, 1874, 1875, 1875-1878, 1878, 1879, 1879, 1880, 1880, 1881, 1881, 1882, 1882, 1883, 1883, 1900; 1901, 1904-1906, 1906, 1907, 1907-1909, 1916, 1917, 1924-1931, 1942, 1942, 1943, 1943, 1948, 1949, 1952, 1952, 1953, 1953-1957, 1966, 1966, 1967, 1967, 1968, 1968, 1969, 1969, 1970, 1970, 1971, 1971, 1980-1982, 1982, 1983, 1983-1985, 1994-1998, 1998, 1999, 1999, 2004, 2005, 2010-2015, 2020, 2021, 2028-2030, 2030, 2031, 2031-2033, 2036, 2036, 2037, 2037-2049, 2054-2059, 2066-2070, 2070, 2071, 2071-2073, 2076, 2076, 2077, 2077, 2080-2089, 2092-2099, 2104, 2104, 2105, 2105, 2108, 2109, 2116-2119, 2130, 2130, 2131, 2131-2134, 2134, 2135, 2135, 2136, 2136, 2137, 2137, 2138, 2138, 2139, 2139, 2140, 2140, 2141, 2141-2144, 2144, 2145, 2145, 2146, 2146-2149, 2149, 2150, 2150-2154, 2163, 2164, 2169, 2170, and 2177-2180.

In one further embodiment of the method, breast cancer cells are detected against a background of blood or blood derived fluids by the differentiation of breast cancer cells from peripheral blood lymphocytes. This is achieved by analysis of the CpG methylation status of at least one target sequence comprising, or hybridizing under stringent conditions to at least 16 contiguous nucleotides of a gene or sequence selected from the group consisting APC, ARH1/NOEY2, CCND2, CDH1, CDKN1A, CDKN2A, SEQ ID NO: 9, DAPK1, SEQ ID NO: 2, EYA4, FHIT, GSTP1, HIC1, IGFBP7, FOR, SERPINB5, RARB, SFN, SOD2, TERT, TGFBR2, THRB, TIMP3, NME1, CDH13, THBS1, TMS1/ASC, ESR1, IL6, APAF1, CASP8, SYK, HOXA5, FABP3, RASSF1A, SEQ ID NO: 3, TWIST, ESR2, PLAU, STAT1, SEQ ID NO: 4, BRCA1, LOT1, PRSS8, SNCG, GPC3, CLDN7, SLC19A1, GJB2, SLIT2, IGSF4, MCT1, HS3ST2, PRDM2, ALX4, SEQ ID NO: 5, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 8, SCGB3A1, SEQ ID NO: 1, PROSTAGLANDIN E2 RECEPTOR, EP4 SUBTYPE (PROSTANOID EP4 RECEPTOR) (PGE RECEPTOR, EP4 SUBTYPE), ORPHAN NUCLEAR RECEPTOR NR5A2 (ALPHA-1-FETOPROTEIN TRANSCRIPTION FACTOR) (HEPATOCYTIC TRANSCRIPTION FACTOR) (B1-BINDING FACTOR) (HB1F) (CYP7A PROMOTER BINDING FACTOR), LIM DOMAIN KINASE 1, SASH/, S100A7, BCL1113, SEQ ID NO: 51, MGC34831, SEQ ID NO: 54, PDLIM1, MSF, SEQ ID NO: 14, SEQ ID NO: 15, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 18, SEQ ID NO: 19, PRDM6, RAP2B, NR2E1, PCDH7, DKK3, RTTN, SNAP25, SEQ ID NO: 26, GIRK2, SEQ ID NO: 28, SEQ ID NO: 29, ARL7, SEQ ID NO: 31, THE, HOXB13, SEQ ID NO: 35, SEQ ID NO: 36, MGC10561, LMX1A, SENP3, GS1, TITF1, SEQ ID NO: 42, DDX51, SEQ ID NO: 117, SEQ ID NO: 46, O60279, and SEQ ID NO: 48 and complements thereof.

In a further embodiment the CpG methylation status of at least one target sequence comprising, or hybridizing under stringent conditions to at least 16 contiguous nucleotides of a gene or sequence selected from the group consisting FABP3, RASSF1A, MSF, PRDM6, LMX1A, SEQ ID NO: 4, SCGB3A1, SLIT2, NR2E1, EYA4, PRDM2, SERPINB5, TWIST, STAT1, ALX4, IGFBP7, DAPK1, THBS1, PLAU, SEQ ID NO: 20, SEQ ID NO: 38, SEQ ID NO: 8, SEQ ID NO: 37, SEQ ID NO: 10, SEQ ID NO: 35, SEQ ID NO: 47, SEQ ID NO: 6, LIMK-1 and SEQ ID NO: 46 and complements thereof.

In both cases, this is preferably achieved by use of a set consisting of at least one oligonucleotide, and more preferably at least two selected from one of the groups consisting of 1475-1477, 1477, 1478, 1478, 1479, 1479, 1480, 1480, 1485-1497, 1497, 1498, 1498, 1501, 1501, 1502, 1502-1511, 1511, 1512, 1512-1522, 1525-1527, 1527, 1528, 1528-1540, 1543-1546, 1549-1557, 1557, 1558, 1558-1567, 1567, 1568, 1568, 1569, 1569, 1570, 1570-1572, 1583-1596, 1599, 1600, 1603, 1604, 1607, 1607, 1608, 1608-1619, 1619, 1620, 1620-1623, 1623, 1624, 1624-1626, 1631-1639, 1639, 1640, 1640, 1645, 1646, 1649-1655, 1655, 1656, 1656-1660, 1663-1668, 1671-1693, 1693, 1694, 1694, 1695, 1695, 1696, 1696, 1697, 1697-1699, 1704-1706, 1706, 1707, 1707-1720, 1720, 1721, 1721, 1724, 1724, 1725, 1725-1728, 1728, 1729, 1729-1733, 1738, 1738, 1739, 1739, 1742, 1743, 1746, 1747, 1750, 1751, 1758, 1758, 1759, 1759-1762, 1762, 1763, 1763-1770, 1770, 1771, 1771-1778, 1778, 1779, 1779, 1782-1789, 1792-1798, 1798, 1799, 1799-1838, 1838, 1839, 1839, 1840, 1840, 1841, 1841-1845, 1848-1852, 1852, 1853, 1853, 1854, 1854, 1855, 1855-1869, 1872, 1873, 1878, 1878, 1879, 1879, 1880, 1880, 1881, 1881, 1882, 1882, 1883, 1883-1885, 1888-1890, 1890, 1891, 1891-1906, 1906, 1907, 1907-1935, 1938-1940, 1940, 1941, 1941, 1942, 1942, 1943, 1943-1946, 1946, 1947, 1947-1952, 1952, 1953, 1953-1966, 1966, 1967, 1967, 1968, 1968, 1969, 1969, 1970, 1970, 1971, 1971-1973, 1976-1978, 1978, 1979, 1979-1982, 1982, 1983, 1983-1987, 1990-1992, 1992, 1993, 1993-1998, 1998, 1999, 1999-2006, 2006, 2007, 2007-2016, 2016, 2017, 2017-2022, 2022, 2023, 2023-2025, 2028-2030, 2030, 2031, 2031-2036, 2036, 2037, 2037-2049, 2052-2060, 2060, 2061, 2061-2070, 2070, 2071, 2071-2076, 2076, 2077, 2077-2104, 2104, 2105, 2105, 2106, 2106, 2107, 2107-2114, 2114, 2115, 2115-2117, 2120-2128, 2128, 2129, 2129, 2130, 2130, 2131, 2131-2134, 2134, 2135, 2135, 2136, 2136, 2137, 2137, 2138, 2138, 2139, 2139, 2140, 2140, 2141, 2141-2143, 2147-2149, 2149, 2150, 2150-2156, 2161, 2162, 2171, 2172, 2181, 2181, 2182, 2182-2187, 2187, 2188, 2188-2199, 2199, 2200, and 2200-2218.

In one embodiment of the method, DCIS is differentiated from benign breast cell proliferative disorders. This is achieved by analysis of the CpG methylation status of at least one target sequence comprising, or hybridizing under stringent conditions to at least 16 contiguous nucleotides of a gene or sequence selected from the group consisting of APC, ARH1/NOEY2, CCND2, CDKN1A, CDKN2A, SEQ ID NO: 9, SEQ ID NO: 2, EYA4, FHIT, GSTP1, HIC1, IGFBP7, MLH1, PGR, SERPINB5, RARB; SOD2, TERT, TGFBR2, THRB, TIMP3, TP73, CDH13, THBS1, TMS1/ASC, ESR1, APAF1, CASP8, SYK, HOXA5, FABP3, RASSF1A, SEQ ID NO: 3, RARA, TWIST, ESR2, PLAU, SEQ ID NO: 4, SNCG, SLC19A1, GJB2, SLIT2, IGSF4, MCT1, HS3ST2, PRDM2, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 8, SCGB3A1, PROSTAGLANDIN E2 RECEPTOR, EP4 SUBTYPE (PROSTANOID EP4 RECEPTOR) (PGE RECEPTOR, EP4 SUBTYPE), ORPHAN NUCLEAR RECEPTOR NR5A2 (ALPHA-1-FETOPROTEIN TRANSCRIPTION FACTOR) (HEPATOCYTIC TRANSCRIPTION FACTOR) (B1-BINDING FACTOR) (HB1F) (CYP7A PROMOTER BINDING FACTOR), LIM DOMAIN KINASE 1, SASH1, S100A7, BCL11B, SEQ ID NO: 51, MGC34831, SEQ ID NO: 54, PDLIM1, MSF, SEQ ID NO: 14, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 18, SEQ ID NO: 19, NR2E1, PCDH7, DKK3, RTTN, SNAP25, GIRK2, SEQ ID NO: 28, SEQ ID NO: 29, ARL7, SEQ ID NO: 31, THH, HOXB13, SEQ ID NO: 36, LMX1A, SENP3, TITF1, SEQ ID NO: 42, DDX51, SEQ ID NO: 117, SEQ ID NO: 46, O60279, and SEQ ID NO: 48 and complements thereof.

In a further embodiment the CpG methylation status of at least one target sequence comprising, or hybridizing under stringent conditions to at least 16 contiguous nucleotides of a gene or sequence selected from the group consisting of HS3ST2, SLIT2, RASSF1A, GSTP1, GJB2, IGFBP7, CDH13, ARH1/NOEY2, SCGB3A1, FHIT, SEQ ID NO: 27, LIMK-1, SEQ ID NO: 46, SEQ ID NO: 3, SEQ ID NO: 117, SEQ ID NO: 48, SEQ ID NO: 41, SEQ ID NO: 4, SEQ ID NO: 6, and SEQ ID NO: 24 and complements thereof.

In both eases this is preferably achieved by use of a set consisting of at least one oligonucleotide, and more preferably at least two selected from one of the groups consisting of 1475-1477, 1477, 1478, 1478, 1479, 1479, 1480, 1480-1482, 1485-1497, 1497, 1498, 1498, 1501, 1501, 1502, 1502-1508, 1513, 1514, 1517, 1518, 1521-1527, 1527, 1528, 1528-1534, 1541-1544, 1547-1550, 1555-1557, 1557, 1558, 1558-1560, 1567, 1567, 1568, 1568, 1569, 1569, 1570, 1570-1573, 1573, 1574, 1574-1578, 1581-1592, 1595-1600, 1605-1607, 1607, 1608, 1608-1618, 1623, 1623, 1624, 1624-1626, 1631-1636, 1639, 1639, 1640, 1640, 1663-1668, 1671-1676, 1689, 1690, 1695, 1695, 1696, 1696, 1697, 1697-1701, 1706, 1706, 1707, 1707-1713, 1720, 1720, 1721, 1721, 1726-1728, 1728, 1729, 1729, 1732-1734, 1734, 1735, 1735, 1740, 1741, 1746-1752, 1752, 1753, 1753, 1756-1758, 1758, 1759, 1759, 1772-1778, 1778, 1779, 1779, 1780, 1780, 1781, 1781, 1784-1790, 1790, 1791, 1791-1798, 1798, 1799, 1799-1805, 1812-1835, 1842-1845, 1848, 1849, 1852, 1852, 1853, 1853, 1854, 1854, 1855, 1855-1869, 1872, 1873, 1876-1878, 1878, 1879, 1879, 1882, 1882, 1883, 1883-1886, 18860887, 1887-1890, 1890, 1891, 1891-1895, 1902-1906, 1906, 1907, 1907, 1910, 1911, 1914-1923, 1932-1935, 1938-1940, 1940, 1941, 1941, 1952, 1952, 1953, 1953, 1958-1963, 1966, 1966, 1967, 1967, 1968, 1968, 1969, 1969, 1970, 1970, 1971, 1971, 1974-1977, 1980-1982, 1982, 1983, 1983-1987, 1992, 1992, 1993, 1993, 1996-1998, 1998, 1999, 1999-2005, 2010-2013, 2028-2030, 2030, 2031, 2031-2036, 2036, 2037, 2037-2039, 2042-2050, 2050, 2051, 2051, 2060, 2060, 2061, 2061-2070, 2070, 2071, 2071-2076, 2076, 2077, 2077, 2092, 2093, 2104, 2104, 2105, 2105, 2106, 2106, 2107, 2107, 2110, 2111, 2116, 2117, 2120-2127, 2130, 2130, 2131, 2131-2134, 2134, 2135, 2135, 2136, 2136, 2137, 2137, 2138, 2138, 2139, 2139, 2155, 2156, 2161, 2162, 2183, 2184, 2187, 2187, 2188, 2188, 2199, 2199, 2200, 2200-2202, and 2219-2222.

In one embodiment of the method, breast cancer is differentiated from benign breast cell proliferative disorders. This is achieved by analysis of the CpG methylation status of at least one target sequence comprising, or hybridizing under stringent conditions to at least 16 contiguous nucleotides of a gene or sequence selected from the group consisting of ARH1/NOEY2, CCND2, CDKN1A, CDKN2A, SEQ ID NO: 9, DAPK1, SEQ ID NO: 2, EYA4, FHIT, GSTP1, HIC1, IGFBP7, SERPINB5, TERT, TGFBR2, THRB, TIMP3, TP73, NME1, CDH13, THBS1, TMS1/ASC, IL6, APAF1, SYK, HOXA5, FABP3, RASSF1A, SEQ ID NO: 3, TWIST, ESR2, PLAU, STAT1, SEQ ID NO: 4, LOT1, GPC3, CLDN7, GJB2, SLIT2, IGSF4, MCT1, PRDM2, ALX4, SEQ ID NO: 5, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 8, SCGB3A1, SEQ ID NO: 1, PROSTAGLANDIN E2 RECEPTOR, EP4 SUBTYPE (PROSTANOID EP4 RECEPTOR) (PGE RECEPTOR, EP4 SUBTYPE), ORPHAN NUCLEAR RECEPTOR NR5A2 (ALPHA-1-FETOPROTEIN TRANSCRIPTION FACTOR) (HEPATOCYTIC TRANSCRIPTION FACTOR) (E1-BINDING FACTOR) (HB1F) (CYP7A PROMOTER BINDING FACTOR), LIM DOMAIN KINASE 1, BCL11B, SEQ ID NO: 51, MGC34831, SEQ ID NO: 54, PDLIM1, MSF, SEQ ID NO: 14, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 18, SEQ ID NO: 19, PRDM6, NR2E1, PCDH7, DKK3, RTTN, SNAP25, SEQ ID NO: 26, GIRK2, SEQ ID NO: 28, SEQ ID NO: 29, ARL7, SEQ ID NO: 31, THH, HOXB13, SEQ ID NO: 35, SEQ ID NO: 36, MGC10561, LMX1A, SENP3, GS1, TITF1, SEQ ID NO: 42, DDX51, SEQ ID NO: 117, SEQ ID NO: 45, SEQ ID NO: 46, O60279, and SEQ ID NO: 48 and complements thereof.

In a further embodiment the CpG methylation status of at least one target sequence comprising, or hybridizing under stringent conditions to at least 16 contiguous nucleotides of a gene or sequence selected from the group consisting SLIT2, HS3ST2, HOXA5, ARH1/NOEY2, IGFBP7, PLAU, CDH13, TIMP3, CCND2, GSTP1, SEQ ID NO: 117, SEQ ID NO: 46, SEQ ID NO: 6, SEQ ID NO: 7, SEQ ID NO: 3, SEQ ID NO: 41, SEQ ID NO: 27, SEQ ID NO: 31, and SEQ ID NO: 4 and complements thereof.

In both cases this is preferably achieved by use of a set consisting of at least one oligonucleotide, and more preferably at least two selected from one of the groups consisting of 1475, 1476, 1485-1497, 1497, 1498, 1498, 1499, 1499, 1500, 1500, 1501, 1501, 1502, 1502-1504, 1509-1511, 1511, 1512, 1512-1522, 1525-1527, 1527, 1528, 1528-1540, 1551-1554, 1569, 1569, 1570, 1570-1573, 1573, 1574, 1574-1580, 1585, 1586, 1591-1600, 1603, 1604, 1609-1619, 1619, 1620, 1620-1623, 1623, 1624, 1624-1626, 1629, 1630, 1633-1639, 1639, 1640, 1640-1642, 1649, 1650, 1667, 1668, 1675-1680, 1683-1688, 1710-1717, 1724, 1724, 1725, 1725-1728, 1728, 1729, 1729-1731, 1736-1738, 1738, 1739, 1739, 1748, 1749, 1752, 1752, 1753, 1753, 1760, 1761, 1764, 1765, 1774-1778, 1778, 1779, 1779, 1780, 1780, 1781, 1781-1783, 1788, 1789, 1792-1798, 1798, 1799, 1799-1835, 1842-1852, 1852, 1853, 1853, 1854, 1854, 1855, 1855-1870, 1870, 1871, 1871-1873, 1876-1878, 1878, 1879, 1879, 1880, 1880, 1881, 1881, 1882, 1882, 1883, 1883-1886, 1886, 1887, 1887-1890, 1890, 1891, 1891-1895, 1898, 1899, 1902-1906, 1906, 1907, 1907-1925, 1932-1940, 1940, 1941, 1941, 1942, 1942, 1943, 1943, 1958-1966, 1966, 1967, 1967, 1968, 1968, 1969, 1969, 1970, 1970, 1971, 1971-1977, 1980-1982, 1982, 1983, 1983-1987, 1992, 1992, 1993, 1993, 1998, 1998, 1999, 1999-2006, 2006, 2007, 2007, 2010-2015, 2020-2022, 2022, 2023, 2023, 2028-2030, 2030, 2031, 2031-2036, 2036, 2037, 2037-2045, 2048-2050, 2050, 2051, 2051-2057, 2060, 2060, 2061, 2061-2070, 2070, 2071, 2071-2076, 2076, 2077, 2077-2079, 2082, 2083, 2086, 2087, 2092-2101, 2104, 2104, 2105, 2105, 2106, 2106, 2107, 2107-2111, 2116, 2117, 2120-2128, 2128, 2129, 2129, 2130, 2130, 2131, 2131-2134, 2134, 2135, 2135, 2136, 2136, 2137, 2137, 2138, 2138, 2139, 2139, 2140, 2140, 2141, 2141-2144, 2144, 2145, 2145, 2146, 2146-2149, 2149, 2150, 2150-2167, 2167, 2168, 2168-2175, 2175, 2176, and 2176.

The present invention further provides a method for ascertaining genetic and/or epigenetic parameters of the genomic sequences according to SEQ ID NO: 1 to SEQ ID NO: 118 within a subject by analyzing cytosine methylation and single nucleotide polymorphisms. Said method comprising contacting a nucleic acid comprising one or more of SEQ ID NO: It to SEQ ID NO: 118 in a biological sample obtained from said subject with at least one reagent or a series of reagents, wherein said reagent or series of reagents, distinguishes between methylated and non-methylated CpG dinucleotides within the target nucleic acid.

Preferably, said method comprises the following steps: In the first step, a sample of the tissue to be analyzed is obtained. The source may be any suitable source, such as cell lines, histological slides, biopsies, paraffin-embedded tissue, body fluids, blood plasma, blood serum, whole blood, isolated blood cells, cells isolated from the blood and all possible combinations thereof. It is preferred that said sources of DNA are body fluids selected from the group consisting nipple aspirate fluid, lymphatic fluid, ductal lavage fluid, fine needle aspirate, blood plasma, blood serum, whole blood, isolated blood cells, cells isolated from the blood.

The genomic DNA is then isolated from the sample. Genomic DNA may be isolated by any means standard in the art, including the use of commercially available kits. Briefly, wherein the DNA of interest is encapsulated in by a cellular membrane the biological sample must be disrupted and lysed by enzymatic, chemical or mechanical means. The DNA solution may then be cleared of proteins and other contaminants e.g. by digestion with proteinase K. The genomic DNA is then recovered from the solution. This may be carried out by means of a variety of methods including salting out, organic extraction or binding of the DNA to a solid phase support. The choice of method will be affected by several factors including time, expense and required quantity of DNA. Once the nucleic acids have been extracted, the genomic double stranded DNA is used in the analysis.

In the second step of the method, the genomic DNA sample is treated in such a manner that cytosine bases which are unmethylated at the 5′-position are converted to uracil, thymine, or another base which is dissimilar to cytosine in terms of hybridization behavior. This will be understood as ‘pretreatment’ or ‘treatment’ herein.

This is preferably achieved by means of treatment with a bisulfite reagent. The term “bisulfite reagent” refers to a reagent comprising bisulfite, disulfite, hydrogen sulfite or combinations thereof, useful as disclosed herein to distinguish between methylated and unmethylated CpG dinucleotide sequences. Methods of said treatment are known in the art (e.g. PCT/EP2004/1011715, which is incorporated by reference in its entirety). It is preferred that the bisulfite treatment is conducted in the presence of denaturing solvents such as but not limited to n-alkylenglycol, particulary diethylene glycol dimethyl ether (DME), or in the presence of dioxane or dioxane derivatives. In a preferred embodiment the denaturing solvents are used in concentrations between 1% and 35% (v/v). It is also preferred that the bisulfite reaction is carried out in the presence of scavengers such as but not limited to chromane derivatives, e.g., 6-hydroxy-2,5,7,8,-tetramethylchromane 2-carboxylic acid (see: PCT/EP2004/011715 which is incorporated by reference in its entirety). The bisulfite conversion is preferably carried out at a reaction temperature between 30° C. and 70° C., whereby the temperature is increased to over 85° C. for short periods of times during the reaction (see: PCT/EP2004/011715 which is incorporated by reference in its entirety). The bisulfite treated DNA is preferably purified prior to further analysis. This may be conducted by any means known in the art, such as but not limited to ultrafiltration, preferably carried out by means of Microcon̂™ columns (manufactured by Milliporê™). The purification is carried out according to a modified manufacturer's protocol (see: PCT/EP2004/011715 which is incorporated by reference in its entirety).

In the third step of the method, at least one target sequence of the treated DNA is amplified, using at least one pair of primer oligonucleotides according to the present invention, and an amplification enzyme. The amplification of several DNA segments can be carried out simultaneously in one and the same reaction vessel. Typically, the amplification is carried out using a polymerase chain reaction (PCR). The set of primer oligonucleotides includes at least two oligonucleotides whose sequences are reverse complementary, identical, or hybridize under stringent or highly stringent conditions to an at least 16-base-pair long segment of a base sequence selected from the group consisting of SEQ ID NO: 493 to SEQ ID NO: 964 and sequences complementary thereto. In alternative embodiments of the method the amplification may be carried out by means of methylation specific primers and/or in the presence of blocker oligonucleotides as will be discussed herein.

In a first alternate embodiment of the method, the methylation status of pre-selected CpG positions within the nucleic acid sequences comprising one or more of SEQ ID NO: 1 to SEQ ID NO: 118 may be determined by use of methylation-specific primer oligonucleotides. This technique (MSP) has been described in U.S. Pat. No. 6,265,171 to Herman. The use of methylation status specific primers for the amplification of bisulfite treated DNA allows the differentiation between methylated and unmethylated nucleic acids. MSP primers pairs contain at least one primer which hybridizes to a bisulfite treated CpG dinucleotide. Therefore, the sequence of said primers comprises at least one CpG dinucleotide. MSP primers specific for non-methylated DNA contain a “T” at the position of the C position in the CpG. Preferably, therefore, the base sequence of said primers is required to comprise a sequence having a length of at least 9 nucleotides which hybridizes to a treated nucleic acid sequence according to one of SEQ ID NO: 493 to SEQ ID NO: 964 and sequences complementary thereto, wherein the base sequence of said oligomers comprises at least one CpG dinucleotide.

A further preferred embodiment of the method comprises the use of blocker oligonucleotides. The use of such blocker oligonucleotides has been described by Yu et al., BioTechniques 23:714-720, 1997. Blocking probe oligonucleotides are hybridized to the bisulfite treated nucleic acid concurrently with the PCR primers. PCR amplification of the nucleic acid is terminated at the 5′ position of the blocking probe, such that amplification of a nucleic acid is suppressed where the complementary sequence to the blocking probe is present. The probes may be designed to hybridize to the bisulfite treated nucleic acid in a methylation status specific manner. For example, for detection of methylated nucleic acids within a population of unmethylated nucleic acids, suppression of the amplification of nucleic acids which are unmethylated at the position in question would be carried out by the use of blocking probes comprising a ‘CpA’ or ‘TpA’ at the position in question, as opposed to a ‘CpG’ if the suppression of amplification of methylated nucleic acids is desired.

For PCR methods using blocker oligonucleotides, efficient disruption of polymerase-mediated amplification requires that blocker oligonucleotides not be elongated by the polymerase. Preferably, this is achieved through the use of blockers that are 3′-deoxyoligonucleotides, or oligonucleotides derivitized at the 3′ position with other than a “free” hydroxyl group. For example, 3′-O-acetyl oligonucleotides are representative of a preferred class of blocker molecule.

Additionally, polymerase-mediated decomposition of the blocker oligonucleotides should be precluded. Preferably, such preclusion comprises either use of a polymerase lacking 5′-3′ exonuclease activity, or use of modified blocker oligonucleotides having, for example, thioate bridges at the 5′-terminii thereof that render the blocker molecule nuclease-resistant. Particular applications may not require such 5′ modifications of the blocker. For example, if the blocker- and primer-binding sites overlap, thereby precluding binding of the primer (e.g., with excess blocker), degradation of the blocker oligonucleotide will be substantially precluded. This is because the polymerase will not extend the primer toward, and through (in the 5′-3′ direction) the blocker—a process that normally results in degradation of the hybridized blocker oligonucleotide.

A particularly preferred blocker/PCR embodiment, for purposes of the present invention and as implemented herein, comprises the use of peptide nucleic acid (PNA) oligomers as blocking oligonucleotides. Such PNA blocker oligomers are ideally suited, because they are neither decomposed nor extended by the polymerase.

Preferably, therefore, the base sequence of said blocking oligonucleotides is required to comprise a sequence having a length of at least 9 nucleotides which hybridizes to a treated nucleic acid sequence according to one of SEQ ID NO: 493 to SEQ ID NO: 964 and sequences complementary thereto, wherein the base sequence of said oligonucleotides comprises at least one CpG, TpG or CpA dinucleotide.

The fragments obtained by means of the amplification can carry a directly or indirectly detectable label. Preferred are labels in the form of fluorescence labels, radionuclides, or detachable molecule fragments having a typical mass which can be detected in a mass spectrometer. Where said labels are mass labels, it is preferred that the labeled amplificates have a single positive or negative net charge, allowing for better detectability in the mass spectrometer. The detection may be carried out and visualized by means of e.g., matrix assisted laser desorption/ionization mass spectrometry (MALDI) or using electron spray mass spectrometry (ESI).

Matrix Assisted Laser Desorption/Ionization Mass Spectrometry (MALDI-TOF) is a very efficient development for the analysis of biomolecules (Karas and Hillenkamp, Anal Chem., 60:2299-301, 1988). An analyte is embedded in a light-absorbing matrix. The matrix is evaporated by a short laser pulse thus transporting the analyte molecule into the vapor phase in an unfragmented manner. The analyte is ionized by collisions with matrix molecules. An applied voltage accelerates the ions into a field-free flight tube. Due to their different masses, the ions are accelerated at different rates. Smaller ions reach the detector sooner than bigger ones. MALDI-TOP spectrometry is well suited to the analysis of peptides and proteins. The analysis of nucleic acids is somewhat more difficult (Gut and Beck, Current Innovations and Future Trends, 1:147-57, 1995). The sensitivity with respect to nucleic acid analysis is approximately 100-times less than for peptides, and decreases disproportionally with increasing fragment size. Moreover, for nucleic acids having a multiply negatively charged backbone, the ionization process via the matrix is considerably less efficient. In MALDI-TOF spectrometry, the selection of the matrix plays an eminently important role. For desorption of peptides, several very efficient matrixes have been found which produce a very fine crystallization. There are now several responsive matrixes for DNA, however, the difference in sensitivity between peptides and nucleic acids has not been reduced. This difference in sensitivity can be reduced, however, by chemically modifying the DNA in such a manner that it becomes more similar to a peptide. For example, phosphorothioate nucleic acids, in which the usual phosphates of the backbone are substituted with thiophosphates, can be converted into a charge-neutral DNA using simple alkylation chemistry (Gut and Beck, Nucleic Acids Res. 23: 1367-73, 1995). The coupling of a charge tag to this modified DNA results in an increase in MALDI-TOF sensitivity to the same level as that found for peptides. A further advantage of charge tagging is the increased stability of the analysis against impurities, which makes the detection of unmodified substrates considerably more difficult.

In the fourth step of the method, the amplificates obtained during the third step of the method are analyzed in order to determine the methylation status of the CpG dinucleotides prior to the treatment.

In embodiments where the amplificates were obtained by means of MSP amplification, the presence or absence of an amplificate is in itself indicative of the methylation state of the CpG positions covered by the primer, according to the base sequences of said primer.

Similarly in embodiments where the amplificates were obtained by means of amplification in the presence of blocker oligonucleotides the presence or absence of an amplificate is in itself indicative of the methylation state of the CpG positions covered by the blocker, according to the base sequences of said blocker.

In embodiments where the amplificates were obtained by means of MSP amplification in the presence of blocker oligonucleotides the presence or absence of an amplificate is in itself indicative of the methylation state of the CpG positions covered by the primer and blocker oligonucleotides, according to the base sequences of said primer and blocker oligonucleotides.

Amplificates obtained by means of both standard and methylation specific PCR may be further analyzed by means of hybridization based methods such as, but not limited to, array technology and probe based technologies as well as by means of techniques such as sequencing and template directed extension.

In one embodiment of the method, the amplificates synthesized in step three are subsequently hybridized to an array or a set of oligonucleotides and/or PNA probes. In this context, the hybridization takes place in the following manner: the set of probes used during the hybridization is preferably composed of at least 2 oligonucleotides or PNA-oligomers; in the process, the amplificates serve as probes which hybridize to oligonucleotides previously bonded to a solid phase; the non-hybridized fragments are subsequently removed; said oligonucleotides contain at least one base sequence having a length of at least 9 nucleotides which is reverse complementary or identical to a segment of the base sequences specified in the present Sequence Listing; and the segment comprises at least one CpG, TpG or CpA dinucleotide.

In a preferred embodiment, said dinucleotide is present in the central third of the oligomer. For example, wherein the oligomer comprises one CpG dinucleotide, said dinucleotide is preferably the fifth to ninth nucleotide from the 5′-end of a 13-mer. One oligonucleotide exists for the analysis of each CpG dinucleotide within a sequence selected from the group according to SEQ ID NO: 1 to SEQ ID NO: 118, and the equivalent positions within SEQ ID NO: 493 to SEQ ID NO: 964. Said oligonucleotides may also be present in the form of peptide nucleic acids. The non-hybridized amplificates are then removed. The hybridized amplificates are then detected. In this context, it is preferred that labels attached to the amplificates are identifiable at each position of the solid phase at which an oligonucleotide sequence is located.

In yet a further embodiment of the method, the genomic methylation status of the CpG positions may be ascertained by means of oligonucleotide probes that are hybridized to the bisulfite treated DNA concurrently with the PCR amplification primers (wherein said primers may either be methylation specific or standard).

A particularly preferred embodiment of this method is the use of fluorescence-based Real Time Quantitative PCR (Held et al., Genome Res. 6:986-994, 1996; also see U.S. Pat. No. 6,331,393) employing a dual-labeled fluorescent oligonucleotide probe (TaqMan™ PCR, using an ABI Prism 7700 Sequence Detection System, Perkin Elmer Applied Biosystems, Foster City, Calif.). The TaqMan™ PCR reaction employs the use of a non-extendible interrogating oligonucleotide, called a TaqMan™ probe, which, in preferred embodiments, is designed to hybridize to a GpC-rich sequence located between the forward and reverse amplification primers. The TaqMan™ probe further comprises a fluorescent “reporter moiety” and a “quencher moiety” covalently bound to linker moieties (e.g., phosphoramidites) attached to the nucleotides of the TaqMan™ oligonucleotide. For analysis of methylation within nucleic acids subsequent to bisulfite treatment, it is required that the probe be methylation specific, as described in U.S. Pat. No. 6,331,393, (hereby incorporated by reference in its entirety) also known as the MethylLight™ assay. Variations on the TaqMan™ detection methodology that are also suitable for use with the described invention include the use of dual-probe technology (Lightcycler™) or fluorescent amplification primers (Sunrise™ technology). Both these techniques may be adapted in a manner suitable for use with bisulfite treated DNA, and moreover for methylation analysis within CpG dinucleotides.

A further suitable method for the use of probe oligonucleotides for the assessment of methylation by analysis of bisulfite treated nucleic acids. In a further preferred embodiment of the method, the fifth step of the method comprises the use of template-directed oligonucleotide extension, such as MS-SNuPE as described by Gonzalgo and Jones, Nucleic Acids Res. 25:2529-2531, 1997.

In yet a further embodiment of the method, the fifth step of the method comprises sequencing and subsequent sequence analysis of the amplificate generated in the third step of the method (Sanger F., et al., Proc. Natl Acad Set USA 74:5463-5467, 1977).

In the most preferred embodiment of the method the genomic nucleic acids are isolated and treated according to the first three steps of the method outlined above, namely:

a) obtaining, from a subject, a biological sample having subject genomic DNA;b) extracting or otherwise isolating the genomic DNA;c) treating the genomic DNA of b), or a fragment thereof, with one or more reagents to convert cytosine bases that are unmethylated in the 5-position thereof to uracil or to another base that is detectably dissimilar to cytosine in terms of hybridization properties; and whereind) amplifying subsequent to treatment in c) is carried out in a methylation specific manner, namely by use of methylation specific primers and/or blocking oligonucleotides, and further, whereine) detecting of the amplificates is carried out by means of a real-time detection probe, as described above.

Preferably, where the subsequent amplification of d) is carried out by means of methylation specific primers, as described above, said methylation specific primers comprise a sequence having a length of at least 9 nucleotides which hybridizes to a treated nucleic acid sequence according to one of SEQ ID NO: 493 to SEQ ID NO: 964 and sequences complementary thereto, wherein the base sequence of said oligomers comprises at least one CpG dinucleotide.

In an alternative, and most preferred embodiment of the method, the subsequent amplification of d) is carried out in the presence of blocking oligonucleotides, as described above. Said blocking oligonucleotides comprising a sequence having a length of at least 9 nucleotides which hybridizes to a treated nucleic acid sequence according to one of SEQ ID NO: 493 to SEQ ID NO: 964 and sequences complementary thereto, wherein the base sequence of said oligomers comprises at least one CpG, TpG or CpA dinucleotide. Step e) of the method, namely the detection of the specific amplificates indicative of the methylation status alone or more CpG positions according to SEQ ID NO: 1 to SEQ ID NO: 118 is carried out by means of real-time detection methods as described above.

Additional embodiments of the invention provide a method for the analysis of the methylation status of genomic DNA according to the invention (SEQ ID NO: 1 to SEQ ID NO: 118, and complements thereof) without the need for pretreatment.

In the first step of such additional embodiments, the genomic DNA sample is isolated from tissue or cellular sources. Preferably, such sources include cell lines, histological slides, body fluids, or tissue embedded in paraffin. In the second step, the genomic DNA is extracted. Extraction may be by means that are standard to one skilled in the art, including but not limited to the use of detergent lysates, sonification and vortexing with glass beads. Once the nucleic acids have been extracted, the genomic double-stranded DNA is used in the analysis.

In a preferred embodiment, the DNA may be cleaved prior to the treatment, and this may be by any means standard in the state of the art, in particular with methylation-sensitive restriction endonucleases.

In the second step, the DNA is then digested with one or more methylation sensitive restriction enzymes. The digestion is carried out such that hydrolysis of the DNA at the restriction site is informative of the methylation status of a specific CpG dinucleotide.

In the third step, which is optional but a preferred embodiment, the restriction fragments are amplified. This is preferably carried out using a polymerase chain reaction, and said amplificates may carry suitable detectable labels as discussed above, namely fluorophore labels, radionuclides and mass labels.

In the fourth step the amplificates are detected. The detection may be by any means standard in the art, for example, but not limited to, gel electrophoresis analysis, hybridization analysis, incorporation of detectable tags within the PCR products, DNA array analysis, MALDI or ESI analysis.

Subsequent to the determination of the methylation state of the genomic nucleic acids the presence, absence or subclass of breast cell proliferative disorder is deduced based upon the methylation state of at least one CpG dinucleotide sequence of SEQ ID NO: 1 to SEQ ID NO: 118, or an average, or a value reflecting an average methylation state of a plurality of CpG dinucleotide sequences of SEQ ID NO: 1 to SEQ ID NO: 118. Methylation of CpG positions within any of the genes of Table 3, with the exception of PRDM2 and S100A7, is indicative of the presence of breast cell proliferative disorders. No methylation of CpG positions within the genes PRDM2 and S100A7 is indicative of the presence of breast cell proliferative disorders.

In alternative embodiments (e.g. Real-time analysis) of the method it is possible to quantify the level of methylation at the analyzed CpG positions (or an average thereof or a value reflecting an average thereof), in such embodiments it is preferred that a pre-determined cut-off point is determined above which measured methylation levels are determined as “methylated” and below which measured methylation levels are determined as “unmethylated”. Particularly preferred is a cut-off between 0% and 10% methylation or equivalent values, also preferred is a cut-off point between 3% and 7% methylation or equivalent values and further preferred is a cut-off point between 4% and 6% methylation or equivalent values.

Moreover, an additional aspect of the present invention is a kit comprising, for example: a bisulfite-containing reagent; a set of primer oligonucleotides containing at least two oligonucleotides whose sequences in each case correspond, are complementary, or hybridize under stringent or highly stringent conditions to a 16-base long segment of the sequences SEQ ID NO: 1 to SEQ ID NO: 964 (most preferably SEQ ID NO: 493 to SEQ ID NO: 964); oligonucleotides and/or PNA-oligomers; as well as instructions for carrying out and evaluating the described method. In a further preferred embodiment, said kit may further comprise standard reagents for performing a CpG position-specific methylation analysis, wherein said analysis comprises one or more of the following techniques: MS-SNuPE, MSP, MethyLight™, HeavyMethyl™, COBRA, and nucleic acid sequencing. However, a kit along the lines of the present invention can also contain only part of the aforementioned components.

In a further embodiment the present invention provides for molecular genetic markers selected from the group consisting APC, BCL113, CASP8, CDKN2A, DAPK1, DDX51, DKK3, ESR1, ESR2, FABP3, SEQ ID NO: 4, SEQ ID NO: 7, SEQ ID NO: 9, SEQ ID NO: 14, SEQ ID NO: 16, SEQ ID NO: 17, SEQ ID NO: 19, SEQ ID NO: 28, SEQ ID NO: 29, SEQ ID NO: 36, SEQ ID NO: 46, SEQ ID NO: 48, SEQ ID NO: 51, SEQ ID NO: 117, GIRK2, GJB2, GS1, HS3ST2, MCT1, MGC34831, MLH1, NME1, ORPHAN NUCLEAR RECEPTOR NR5A2 PGR, PRDM6, RARA, RARB, S100A7, SASH1, SEQ ID NO:42, SERPINB5, SLC19A1, SNCG, SOD2, TERT, TGFBR2 and TP73 according to Table 26 that have novel utility for the analysis of methylation patterns associated with the development of cancer, in particular lung, breast and colon cancer. Said markers may be used for detecting cancer, in particular lung, breast and colon cancer and thereby providing improved means for the detection and early treatment of said disorders. As used herein the term cancer shall be understood as a generic term for all classes of malignant neoplasms characterized by uncontrolled cell proliferation and capable of invading other tissues by direct growth into adjacent tissue (invasion) and/or by migration of cells to distant sites (metastasis).

The use of said genes and/or sequences may be enabled by means of any analysis of the expression of the gene, by means of mRNA expression analysis or protein expression analysis. However, in the most preferred embodiment of the invention, the detection of breast cell proliferative disorders is enabled by means of analysis of the methylation status of said genes or genomic sequences and their promoter or regulatory elements. Methods for the methylation analysis of genes are described herein.

It is further preferred that the sequences of said genes in Table 26 according to SEQ ID NO: 65, 50, 71, 57, 98, 43, 24, 75, 91, 77, 4, 7, 9, 14, 16, 17, 19, 28, 29, 36, 46, 48, 51, 117, 27, 111, 40, 113, 101, 52, 89, 107, 11, 83, 20, 108, 88, 96, 102, 42, 68, 116, 73, 105, 92, 93 and 86 as described in the accompanying sequence listing are analyzed.

In a preferred embodiment the invention provides a method for detecting cancer in a subject. Said method comprises the following steps

i) contacting genomic DNA obtained from the subject with at least one reagent, or series of reagents that distinguishes between methylated and non-methylated CpG dinucleotides within at least one target region of the genomic DNA, wherein said contiguous nucleotides comprise at least one CpG dinucleotide sequence, andii) detecting, or detecting and distinguishing between or among breast cell proliferative disorders.

It is particularly preferred that said genomic DNA is obtained from isolated from body fluids of the subject.

Genomic DNA may be isolated by any means standard in the art, including the use of commercially available kits. Briefly, wherein the DNA of interest is encapsulated in by a cellular membrane the biological sample must be disrupted and lysed by enzymatic, chemical or mechanical means. The DNA solution may then be cleared of proteins and other contaminants e.g. by digestion with proteinase K. The genomic DNA is then recovered from the solution. This may be carried out by means of a variety of methods including salting out, organic extraction or binding of the DNA to a solid phase support. The choice of method will be affected by several factors including time, expense and required quantity of DNA. Body fluids are the preferred source of the DNA; particularly preferred are blood plasma, blood serum, whole blood, isolated blood cells and cells isolated from the blood.

The genomic DNA sample is then treated in such a manner that cytosine bases which are unmethylated at the 5′-position are converted to uracil, thymine, or another base which is dissimilar to cytosine in terms of hybridization behavior. This will be understood as ‘treatment’ herein.

This is preferably achieved by means of treatment with a bisulfite reagent. The term “bisulfite reagent” refers to a reagent comprising bisulfite, disulfite, hydrogen sulfite or combinations thereof, useful as disclosed herein to distinguish between methylated and unmethylated CpG dinucleotide sequences. Methods of said treatment are known in the art (e.g. PCT/EP2004/011715, which is incorporated by reference in its entirety). It is preferred that the bisulfite treatment is conducted in the presence of denaturing solvents such as but not limited to n-alkylenglycol, particularly diethylene glycol dimethyl ether (DME), or in the presence of dioxane or dioxane derivatives. In a preferred embodiment the denaturing solvents are used in concentrations between 1% and 35% (v/v). It is also preferred that the bisulfite reaction is carried out in the presence of scavengers such as but not limited to chromane derivatives, e.g., 6-hydroxy-2,5,7,8,-tetramethylchromane 2-carboxylic acid (see: PCT/EP2004/011715 which is incorporated by reference in its entirety). The bisulfite conversion is preferably carried out at a reaction temperature between 30° C. and 70° C., whereby the temperature is increased to over 85° C. for short periods of times during the reaction (see: PCT/EP2004/011715 which is incorporated by reference in its entirety). The bisulfite treated DNA is preferably purified prior to further analysis. This may be conducted by any means known in the art, such as but not limited to ultrafiltration, preferably carried out by means of Microcon™ columns (manufactured by Millipore™). The purification is carried out according to a modified manufacturer's protocol (see: PCT/EP2004/011715 which is incorporated by reference in its entirety).

The treated DNA is then analyzed in order to determine the methylation state of one or more target gene sequences (prior to the treatment) associated with the development of cancer. It is particularly preferred that the target region comprises, or hybridizes under stringent conditions to at least 16 contiguous nucleotides of at least one gene or genomic sequence selected from the group consisting the genes and genomic sequences as listed in Table 26. It is further preferred that the sequences of said genes in Table 26 according to SEQ ID NO: 65, 621, 622; 857, 858, 50, 591, 592, 827, 828, 71, 633, 634, 869, 870, 57, 605, 606, 841, 842, 98, 687, 688, 923, 924, 43, 577, 578, 813, 814, 24, 539, 540, 775, 776, 75, 641, 642, 877, 878, 91, 673, 674, 909, 910, 77, 645, 646, 881, 882, 4, 499, 500, 735, 736, 7, 505, 506, 741, 742, 9, 509, 510, 745, 746, 14, 519, 520, 755, 756, 16, 523, 524, 759, 760, 17, 525, 526, 761, 762, 19, 529, 530, 765, 766, 28, 547, 548, 783, 784, 29, 549, 550, 785, 786, 36, 563, 564, 799, 800, 46, 583, 584, 819, 820, 48; 587, 588, 823, 824, 51, 593, 594, 829, 830, 117, 725, 726, 961, 962, 27, 545, 546, 781, 782, 111, 713, 714, 949, 950, 40, 571, 572, 807, 808, 113, 717, 718, 953, 954, 101, 693, 694, 929, 930, 52, 595, 596, 831, 832, 89, 669, 670, 905, 906, 107, 705, 706, 941, 942, 11, 513, 514, 749, 750, 83, 657, 658, 893, 894, 20, 531, 532, 767, 768, 108, 707, 708, 943, 944, 88, 667, 668, 903, 904, 96, 683, 684, 919, 920, 102, 695, 696, 931, 932, 42, 575, 576, 811, 812, 68, 627, 628, 863, 864, 116, 723, 724, 959, 960, 73, 637, 638, 873, 874, 105, 701, 702, 937, 938, 92, 675, 676, 911, 912, 93, 677, 678, 913, 914, 86, 663, 664, 899 and 900 as described in the accompanying sequence listing are analyzed. The method of analysis may be selected from those known in the art, including those listed herein. Particularly preferred are MethyLight™, MSP and the use of blocking oligonucleotides as previously described herein. It is further preferred that any oligonucleotides used in such analysis (including primers, blocking oligonucleotides and detection probes) should be reverse complementary, identical, or hybridize under stringent or highly stringent conditions to an at least 16-base-pair long segment of the base sequences of one or more of the converted sequences selected from the group consisting 65, 621, 622, 857, 858, 50, 591, 592, 827, 828, 71, 633, 634, 869, 870, 57, 605, 606, 841, 842, 98, 687, 688, 923, 924, 43, 577, 578, 813, 814, 24, 539, 540, 775, 776, 75, 641, 642, 877, 878, 91, 673, 674, 909, 910, 77, 645, 646, 881, 882, 4, 499, 500, 735, 736, 7, 505, 506, 741, 742, 9, 509, 510, 745, 746, 14, 519, 520, 755, 756, 16, 523, 524, 759, 760, 17, 525, 526, 761, 762, 19, 529, 530, 765, 766, 28, 547, 548, 783, 784, 29, 549, 550, 785, 786, 36, 563, 564, 799, 800, 46, 583, 584, 819, 820, 48, 587, 588, 823, 824, 51, 593, 594, 829, 830, 117, 725, 726, 961, 962, 27, 545, 546, 781, 782, 111, 713, 714, 949, 950, 40, 571, 572, 807, 808, 113, 717, 718, 953, 954, 101, 693, 694, 929, 930, 52, 595, 596, 831, 832, 89, 669, 670, 905, 906, 107, 705, 706, 941, 942, 11, 513, 514, 749, 750, 83, 657, 658, 893, 894, 20, 531, 532, 767, 768, 108, 707, 708, 943, 944, 88, 667, 668, 903, 904, 96, 683, 684, 919, 920, 102, 695, 696, 931, 932, 42, 575, 576, 811, 812, 68, 627, 628, 863, 864, 116, 723, 724, 959, 960, 73, 637, 638, 873, 874, 105, 701, 702, 937, 938, 92, 675, 676, 911, 912, 93, 677, 678, 913, 914, 86, 663, 664, 899 and 900 according to Table 26 and sequences complementary thereto.

It is particularly preferred, that the CpG methylation analysis of the genes according to Table 26 are carried out in the form of a gene panel wherein said gene panel consists of one or more markers selected from Table 26 and one or more tissue specific methylation markers. The term tissue specific methylation marker shall be taken to mean a DNA sequence comprising at least one CpG position, the methylation status thereof being a unique characteristic of a specific tissue type thereby enabling the identification of biological matter of said tissue origin. It is further preferred that said gene panel consists of one or more markers selected from Table 26 and one or more tissue specific methylation markers selected from the group consisting of tissue specific markers for each of breast, colon and lung. In an alternative embodiment said gene panel consists of one or more markers selected from Table 26 and one or more tissue specific methylation markers selected from the group consisting of tissue specific markers for each of bladder, breast, colon, lung, rectal, pancreatic, endometrium, prostate, kidney and skin tissues.

It will be appreciated by one skilled in the art that the nucleic acid, oligonucleotides and kits as described herein for the detection and/or characterization will have an additional utility for the detection of all cancers, more preferably breast, lung and colon.

More specifically a preferred embodiment of the invention comprises the use of an oligonucleotide or oligomer for detecting the cytosine methylation state within genomic or treated (chemically modified) DNA, according to Table 26. Said oligonucleotide or oligomer comprising a nucleic acid sequence having a length of at least nine (9) nucleotides which hybridizes, under moderately stringent or stringent conditions (as defined herein above), to a treated nucleic acid sequence according to Table 26 and/or sequences complementary thereto, or to a genomic sequence according to Table 26 and/or sequences complementary thereto.

Furthermore, the present invention also provides kits for the detection of cancer comprising, for example: a bisulfite-containing reagent; a set of primer oligonucleotides containing at least two oligonucleotides whose sequences in each case correspond, are complementary, or hybridize under stringent or highly stringent conditions to a 16-base long segment of the sequences according to Table 26 (most preferably the converted sequences as shown in Table 26); oligonucleotides and/or PNA-oligomers; as well as instructions for carrying out and evaluating the described method. In a further preferred embodiment, said kit may further comprise standard reagents for performing a CpG position-specific methylation analysis, wherein said analysis comprises one or more of the following techniques: MS-SNuPE, MSP, MethyLight, HeavyMethyl, COBRA, and nucleic acid sequencing. However, a kit along the lines of the present invention can also contain only part of the aforementioned components.

While the present invention has been described with specificity in accordance with certain of its preferred embodiments, the following examples serve only to illustrate the invention and are not intended to limit the invention within the principles and scope of the broadest interpretations and equivalent configurations thereof.

Example 1

Microarray Analysis

Microarray Analysis

To evaluate marker candidates a significant number of patient and control samples was analyzed using the applicant's proprietary methylation sensitive Microarray technology. For the Microarray study two gene panels were analyzed on a collection of 475 samples.

Patient Samples

An overview of patient samples collected for the microarray study is provided in Table 25.

Patient Samples: Breast Cancer

Early stage breast cancer samples were obtained from Erasmus Medical Centre, Rotterdam, The Netherlands. The tumor cell proportion was estimated to be on average 60%, ranging from 30% to 90%. Infiltrating ductal carcinomas (IDC) represented the largest histological subtype. Among the IDC patient samples, estrogen receptor (ER) positive and negative, pre- and post menopausal as well as aggressive (node positive) and less aggressive (node negative) tumors were included. In addition, infiltrating lobular carcinomas (ILC) and ductal carcinomas in-situ (DCIS) were analyzed. For all DCIS samples, the diagnosis was confirmed by pathology review and estimates of tumor cell content were provided. Finally, tumors with confirmed BRCA1 mutations were analyzed to assess whether genetic breast cancer samples, which represent about 5-10% of all breast cancer incidences, would show different DNA methylation patterns.

Samples: Benign Breast Conditions

Normal breast samples were obtained primarily from breast reductions or from patient samples that were originally diagnosed with DCIS but were classified to be normal during a pathology review. To analyze DNA methylation patterns in breast epithelial cells, from which breast cancer is almost exclusively derived, epithelial cells were sorted using epithelial cell surface markers. In addition, samples with the diagnosis fibroadenoma, fibrocystic disease and atypical ductal hyperplasia were included into the group benign breast conditions.

Samples: Other Cancers

To evaluate the marker performance on other cancer samples, tumor DNA from several other cancer types was analyzed. Emphasis was put on the most frequently occurring cancer classes in women (lung, colon) and tumors of the female reproductive system (endometrium, ovary).

Lymphocytes

Age matched female lymphocyte samples were used to assess the methylation level of candidate markers in blood cells.

Control Samples

For control purposes additional samples were included in both Microarray studies. In order to control the quality and the functionality of detection oligos, artificially up- and downmethylated. DNA (Promega) was used. 8 male lymphocyte samples were included to allow for a positive control of the overall Microarray process by comparing differential methylation between male and female lymphocytes samples.

Gene Selection

An initial selection of 63 candidate genes or sequences were identified. In addition, one gene fragment, ELK1, which was known to differentiate DNA of male from female origin, was included as a positive control. The gene panel for the second microarray study consisted of 59 sequences initially identified using AP-PCR, MCA or DMH and confirmed by sequencing and the ELK1 gene as a positive control. It has to be noted that not all sequences of the second panel currently map to known genes. Candidate markers from both chips are fully listed in Table 3.

DNA Extraction

Samples were received from external collaborators or commercial providers either as frozen tissues, cell nuclei pellets, or extracted genomic DNA. DNA from tissue samples and cell nuclei pellets was isolated at using the QiaAmp Mini Kit (Qiagen, Hilden, Germany; No: 51306).

The DNA quality of all delivered and extracted samples was first assessed by photometrical measurements. Extinction at 260 nut and 280 mm was measured, A260/280 ratios were determined and the resulting DNA concentration were calculated.

After photometrical measurements each genomic DNA sample was analyzed by gel electrophoresis to assess the integrity of the DNA. Only minor signs of degradation were observed, indicating good overall quality of the extracted DNA.

PCR Establishment and Multiplex PCP optimization

To amplify all gene fragments, PCR assays were designed to match bisulfite treated DNA and to allow amplification independent of the methylation status of the respective fragment. A standardized primer design workflow optimized by the applicant for bisulfite treated DNA was employed. Individual PCR assays were considered established when successful amplification on bisulfite treated lymphocyte DNA was reproduced in triplicate and no background amplification of genomic DNA was detectable, ensuring bisulfite DNA specific amplification. Primers are listed in Table 1.

To allow efficient amplification, individual PCR assays were combined into multiplex PCR (mPCR) assays usually combining up to 8 primer pairs into one mPCR assay. Several multiplex PCR sets were calculated based on the primer sequences of the individual PCR amplificates and tested on lymphocyte DNA. Based on ALF express analyses the best performing combination of multiplex PCR sets were chosen.

Bisulfite Treatment and Multiplex PCR

Total genomic DNA of all samples and controls was bisulfite treated converting unmethylated cytosines to uracil. Methylated cytosines are conserved. Bisulfite treatment was performed according to the applicant's optimized proprietary bisulfite treatment procedure. In order to avoid a potential process bias, the samples were randomized into processing batches. The patient samples were first grouped according to the major diagnosis classes:

• • ILC
  • IDC, N0, ER=neg
  • IDC, N0, ER=pos
  • IDC, N1 or N2, ER=neg
  • IDC, N1 or N2, ER=pos
  • Other Tumors:
  • benign disease/DCIS
  • lymphocytes:
  • normal breast and epithelial cells
  • BRCA1

Batches of 50 samples were created. Each batch contained the same proportion of samples from the major diagnosis classes. Two independent bisulfite reactions were performed for each DNA sample. 10 ng of bisulfite treated DNA was used for each multiplex PCR (mPCR) reaction. In order to monitor the mPCR results, two methods were used: ALF analysis and gel electrophoresis.

Hybridization

All PCR products from each individual sample were then hybridized to glass slides carrying a pair of immobilized oligonucleotides for each CpG position under analysis. For hybridizations, the samples were grouped into processing batches in order to avoid a potential process-bias. The samples were processed in batches of 80 samples randomized for bisulfite batches. Each detection oligonucleotide was designed to hybridize to the bisulphite converted sequence around one CpG site which was either originally unmethylated (TG) or methylated (CG). See Table 2 for further details of all hybridization oligonucleotides used (both informative and non-informative.) Hybridization conditions were selected to allow the detection of the single nucleotide differences between the TG and CG variants.

Fluorescent signals from each hybridized oligonucleotide were detected using genepix scanner and software. Ratios for the two signals (from the CG oligonucleotide and the TG oligonucleotide used to analyze each CpG position) were calculated based on comparison of intensity of the fluorescent signals.

The samples were processed in batches of 80 samples randomized for sex, diagnosis, tissue, and bisulphite batch For each bisulfite treated DNA sample 2 hybridizations were performed. This means that for each sample a total number of 4 chips were processed.

Data Analysis

For the analysis of chip data, Epigenomics' proprietary software ('Episcape') was used. EpiScape contains a data warehouse that supports queries to sample, genome and laboratory management databases, respectively. It encompasses a variety of statistical tools for analyzing and visualizing methylation array data. In the following sections we summarize the most important data analysis techniques that were applied for analyzing the data.

From Raw Hybridization Intensities to Methylation Ratios

The log methylation ratio (log(CG/TG)) at each CpG position was determined according to a standardized preprocessing pipeline that includes the following steps:

• • For each spot the median background pixel intensity is subtracted from the median foreground pixel intensity. This gives a good estimate of background corrected hybridization intensities.
  • For both CG and TG detection oligonucleotides of each CpG position the background corrected median of the 4 redundant spot intensities is taken.
  • For each chip and each CG/TG oligo pair, the log(CG/TG) ratio is calculated.
  • For each sample the median of log(CG/TG) intensities over the redundant chip repetitions is taken.

This log ratio has the property that the hybridization noise has approximately constant variance over the full range of possible methylation rates (see e.g. Huber W, Von Heydebreck A, Sultmann Poustka A, Vingron M. 2002. Variance stabilization applied to Microarray data calibration and to the quantification of differential expression. Bioinformatics. 18 Suppl 1: S96-S104.)

Principle Component Analysis

Principle component analysis (PCA) projects measurement vectors (e.g. chip data, methylation profiles on several CpG sites etc.) onto a new coordinate system. The new coordinate axes are referred to as principal components. The first principal component spans the direction of largest variance of the data. Subsequent components are ordered by decreasing variance and are orthogonal to each other. Different CpG positions contribute with different weights to the extension of the data cloud along different components. PCA is an unsupervised technique, i.e. it does not take into account any group or label information of the data points (for further details see e.g. Ripley, B. D. 1996. Pattern Recognition and Neural Networks, Cambridge, UK, Cambridge University Press.).

PCA is typically used to project high dimensional data (in our case methylation-array data) onto lower dimensional subspaces in order to visualize or extract features with high variance from the data. In the present report we used 2 dimensional projections for statistical quality control of the data, We investigated the effect of different process parameters on the chip data in order to rule out that changing process parameters caused large alterations in the measurement values.

A robust version of PCA was used to detect single outlier chips and exclude them from further analysis (Model F, Koenig T, Piepenbrock C, Adorjan P. 2002. Statistical process control for large scale Microarray experiments. Bioinformatics. 18 Suppl 1:S155-163.).

T² Control Charts

To control the general stability of the chip production process we use methods from the field of multivariate statistical process control (MVSPC). Our major tool is the T² control chart, which is used to detect significant deviations of the chip process from normal working conditions (Model F, Koenig T, Piepenbrock C, Adorjan P. 2002. Statistical process control for large scale Microarray experiments. Bioinformatics, 18 Suppl 1:S155463.).

• • Order the chip data with respect to a process parameter (e.g. hybridization data or spotting robot).
  • Define a historic data set, which describes the chip process under normal working conditions (e.g. the first 75 hybridized chips). In the chart, data from the historical data set are indicated by a special plot symbol.
  • Compute the distance of every new chip to the historic data set. If the distance of several consecutive chips exceeds a given control limit the process has to be regarded as out of control.

Use of T² charts to monitor the chip production process allows us to efficiently detect and eliminate most systematic error sources,

Comparison of Groups: Univariate Methods

Wilcoxon rank sum tests are used to compare groups (e.g. male vs. female lymphocytes) in terms of measurement values of single CpG sites. A significant test result (p<0.05) indicates a shift between the distributions of the respective methylation log-ratios, i.e. log(CG/TG).

For the comparison of up- vs. down methylated chips hybridized with Promega DNA, Fisher scores are used to rank single CpG sites according to their discriminatory power. For each methylation ratio y=CG/TG, the Fisher score is calculated as

$\frac{{\left({\stackrel{\_}{y}}_1-{\stackrel{\_}{y}}_2\right)}^2}{S_1^2+S_2^2},$

where y₁ and S₁² denote mean and variance of group i, respectively.

Comparison of Groups: Multivariate Methods

As referred to herein a marker (sometimes also simply referred to as gene or amplicon) is a genomic region of interest (also referred to herein using the abbreviation ROI). The ROI usually comprises several CpG positions. For testing the null hypothesis that a marker has no predictive power we use the likelihood ratio test for logistic regression models (see Venables, W. N. and Ripley, B. D. Modern Applied Statistics with S-PLUS, 3rd Ed. edition. New York: Springer, 2002.). The logistic regression model for a single marker is a linear combination of methylation measurements from all CpG positions in the respective ROI. The fitted logistic regression model is compared to a constant probability model that is independent of methylation and represents the null hypothesis. The p-value of the marker is computed via the likelihood ratio test.

A significant p-value for a marker means that the methylation of this ROI has some systematic correlation to the question of interest as given by the sample classes. In general a significant p-value does not necessarily imply a good classification performance. However, because with logistic regression we use a linear predictor as the basis of our test statistic small p-values will be indicative of a good clinical performance.

Multiple Test Corrections

Performing a large number of tests at the 5% level will lead to a large number of false positive test results. If there are no differences between groups, the probability of rejecting at least one hypothesis of equality is nearly 1, if about 200 tests are performed. Correction for multiplicity is therefore necessary to reliably conclude that a test result is really significant. A conservative, but simple method is the Bonferroni correction which multiplies all p-values by the number of tests performed, where corrected values>1 are censored to 1.0.

Bonferroni corrections are used for all analyses. The correction helps to avoid spurious findings, however, it is a very conservative method and false negative results (“missed markers”) are a frequent consequence. Therefore, results corrected by the less conservative False Discovery Rate (FDR) methods are also given.

Class Prediction by Supervised Learning

In order to give a reliable estimate of how well the CpG ensemble of a selected marker can differentiate between different tissue classes we can determine its prediction accuracy by classification. For that purpose we calculate a methylation profile-based prediction function using a certain set of tissue samples with a specific class label. This step is called training and it exploits the prior knowledge represented by the data labels. The prediction accuracy of that function is then tested on a set of independent samples. As a method of choice, we use the support vector machine (SVM) algorithm (see e.g. Cristiannini, N. and Shawe-Taylor, J. An introduction to support vector machines. Cambridge, UK: Cambridge University Press, 2000.; Duda, R. O., Hart, P. E., and Stork, D. G. Pattern Classification. New York: John Wiley & Sons, 2001.) to learn the prediction function. For this report, sensitivity and specificity are weighted equally. This is achieved by setting the risk associated with false positive and false negative classifications to be inversely proportional to the respective class sizes. Therefore sensitivity and specificity of the resulting classifier can be expected to be approximately equal. Note that this weighting can be adapted according to the clinical requirements.

Estimating the Performance of the Tissue Class Prediction: Cross Validation

With limited sample size the cross-validation method provides an effective and reliable estimate for the prediction accuracy of a discriminator function, and therefore in addition to the significance of the markers we provide cross-validation accuracy, sensitivity and specificity estimates. For each classification task, the samples were partitioned into 5 groups of approximately equal size. Then the learning algorithm was trained on 4 of these 5 sample groups. The predictor obtained by this method was then tested on the remaining group of independent test samples. The number of correct positive and negative classifications was counted over 10 runs for the learning algorithm for all possible choices of the independent test group without using any knowledge obtained from the previous runs. This procedure was repeated on 10 random permutations of the sample set giving a better estimate of the prediction performance than if performed by simply splitting the samples into one training sample set and one independent test set.

Results

The first step in the analysis of the array data was to identify discriminatory markers when comparing breast cancer samples with benign breast conditions Since the preferred aim of the test is to detect early lesions differentiating between DCIS and benign breast conditions was the primary focus. In order to meet the requirements of a blood based screening test the performance of the marker candidate genes in differentiating breast cancer from lymphocytes and cancer from other origins, respectively was analyzed.

Finally, all breast cancer samples were compared against all other control samples and it was determined that a large number of markers met the specified statistical criteria.

For every comparison, two data analysis methods were used. Multivariate logistic regression analyses were performed and resulting p-values corrected for multiple testing according to the Bonferroni method. Separate models were fitted for each amplificate, comprising methylation ratios measured by 2-6 detection oligo pairs. A marker was preferred, if a p-value below 0.05 after Bonferroni correction for multiple testing was observed. In addition, linear support vector machine (SVM) algorithms were trained and accuracy, sensitivity and specificity to distinguish the respective classes were estimated based on cross validation.

In addition, co-methylation of CpU sites was assessed by analyzing individual detection oligos by means of univariate analyses. Co-methylation was assumed if at least two detection oligos of the same gene fragment differentiated the respective classes with statistical significance (p<0.05 after Bonferroni correction for multiple testing).

Breast Cancer Vs. Benign Breast Conditions

Microarray 1: See Table 12 for Results.

In this comparison the positive was 263 breast cancer samples consisting of 197 IDC, 24 ILC, 22 DCIS and 20 BRCA1 samples, respectively. The negative class consisted 28 normal breast samples and 46 breast samples with a benign breast condition, including fibroadenoma, fibrocystic disease and atypical ductal hyperplasia. Based on multivariate logistic regression analysis 49 markers differentiate between breast cancer and benign breast conditions with statistical significance. Of these, 28 markers fulfilled the co-methylation criterion with at least two detection oligos based on univariate analysis.

Microarray 2: See Table 13 for Results.

In this comparison the positive class was 256 breast cancer samples which are consisting of 191 IDC, 22 ILC, 21 DCIS and 22 BRCA1 samples, respectively. The negative consisted 26 normal breast samples and 42 breast samples with a benign breast condition, including fibroadenoma, fibrocystic disease and atypical ductal hyperplasia. Based on multivariate logistic regression 48 markers differentiate between breast cancer and benign breast conditions with statistical significance. Of these, 32 markers fulfilled the co-methylation criterion with at least two detection oligos based on univariate analysis.

Results are also presented in graphical form in FIGS. 19-30. Each of said figures presents a matrix of the level of methylation of each significant oligomer, oligomers belonging to each gene or genomic sequence are grouped in one discrete block. The SEQ ID NO: of each oligomer is shown on the left hand side of the matrix, on the right hand side of the matrix the FDR corrected multivariate P-value of the oligomers belonging to each individual gene or genomic sequence is shown. The level of methylation is shown by the color of each square of the matrix, from black representing total methylation (+2) to white representing total unmethylation (−2) as shown on the scale to the right hand side of the matrix. Each vertical line of the matrix represents one sample, the type of sample is shown above the matrix.

DCIS Vs. Benign Breast Conditions

Microarray 1: See Table 10 for Results.

In this comparison the positive class was 263 breast cancer samples consisting of 197 IDC, 24 ILC, 22 DCIS and 20 BRCA1 samples, respectively. The negative class is composed of 28 normal breast samples and 46 breast samples with a benign breast condition, including fibroadenoma, fibrocystic disease and atypical ductal hyperplasia. Based on multivariate logistic regression analysis 31 markers differentiate between breast cancer and benign breast conditions with statistical significance. Of these, 13 markers fulfilled the co-methylation criterion with at least two detection oligos statistically significant based on univariate analysis.

Microarray 2: See Table 11 for Results.

In this comparison the positive class was 256 breast cancer samples consisting 191 IDC, 22 ILC, 21 DCIS and 22 BRCA1 samples, respectively, The negative class i consisted of 26 normal breast samples and 42 breast samples with a benign breast condition, including fibroadenoma, fibrocystic disease and atypical ductal hyperplasia. Based on multivariate logistic regression 35 markers differentiate between breast cancer and benign breast conditions with statistical significance. Of these, 17 markers fulfilled the co-methylation criterion with at least two detection oligos statistically significant based on univariate analysis.

Results are also presented in graphical form in FIGS. 31-42. Each of said figures presents a matrix of the level of methylation of each significant oligomer, oligomers belonging to each gene or genomic sequence are grouped in one discrete block. The SEQ ID NO: of each oligomer is shown on the left hand side of the matrix, on the right hand side of the matrix the FDR corrected multivariate P-value of the oligomers belonging to each individual gene or genomic sequence is shown. The level of methylation is shown by the colour of each square of the matrix, from black representing total methylation (+2) to white representing total unmethylation (−2) as shown on the scale to the right hand side of the matrix. Each vertical line of the matrix represents one sample, the type of sample is shown above the matrix.

Breast Cancer Vs. Lymphocytes

Microarray 1: See Table 8 for Results.

In this comparison the positive class was 263 breast cancer samples which consisted 197 IDC, 24 ILC, 22 DCIS and 20 BRCA1 samples, respectively. The negative class consisted of 28 lymphocyte samples. Based on multivariate logistic regression analysis 49 markers differentiate between breast cancer and benign breast conditions with statistical significance. Of these, 30 markers fulfilled the co-methylation criterion with at least two detection oligos statistically significant based on univariate analysis.

Microarray 2: See Table 9 for Results.

In this comparison the positive class was 256 breast cancer samples which consisted of 191 IDC, 22 ILC, 21 DCIS and 22 BRCA1 samples, respectively. The negative class consisted of 34 lymphocyte samples. Based on multivariate logistic regression, 47 markers differentiate between breast cancer and benign breast conditions with statistical significance. Of these, 37 markers fulfilled the co-methylation criterion with at least two detection oligos statistically significant based on univariate analysis.

Results are also presented in graphical form in FIGS. 43-54. Each of said figures presents a matrix of the level of methylation of each significant oligomer, oligomers belonging to each gene or genomic sequence are grouped in one discrete block. The SEQ ID NO: of each oligomer is shown on the left hand side of the matrix, on the right hand side of the matrix the FDR corrected multivariate P-value of the oligomers belonging to each individual gene or genomic sequence is shown. The level of methylation is shown by the colour of each square of the matrix, from black representing total methylation (+2) to white representing total unmethylation (−2) as shown on the scale to the right hand side of the matrix. Each vertical line of the matrix represents one sample, the type of sample is shown above the matrix.

Breast Cancer Vs. Other Cancers

Microarray 1: See Table 6 for Results.

In this comparison the positive class was 263 breast cancer samples which consisted of 197 IDC, 24 ILC, 22 DCIS and 20 BRCA1 samples, respectively. The negative class consisted of 71 other cancer samples which is composed of 12 colon samples, 19 lung samples, 16 ovary samples and 28 further samples of smaller tissue groups. Based on multivariate logistic regression analysis 28 markers differentiate between breast cancer and benign breast conditions with statistical significance. Of these, 16 markers fulfilled the co-methylation criterion with at least two detection oligos statistically significant based on univariate analysis.

Microarray 2: See Table 7 for Results.

In this comparison the positive class was 256 breast cancer samples which consisted of 191 IDC, 22 ILC, 21 DCIS and 22 BRCA1 samples, respectively. The negative class consisted of 73 other cancer samples which consisted of 18 colon samples, 18 lung samples, 16 ovary samples and 21 further samples of smaller tissue groups. Based on multivariate logistic regression 25 markers differentiate between breast cancer and benign breast conditions with statistical significance. Of these, 15 markers fulfilled the co-methylation criterion with at least two detection oligos statistically significant based on univariate analysis.

Results are also presented in graphical form in FIGS. 55-66. Each of said figures presents a matrix of the level of methylation of each significant oligomer, oligomers belonging to each gene or genomic sequence are grouped in one discrete block. The SEQ ID NO: of each oligomer is shown on the left hand side of the matrix, on the right hand side of the matrix the FDR corrected multivariate P-value of the oligomers belonging to each individual gene or genomic sequence is shown. The level of methylation is shown by the colour of each square of the matrix, from black representing total methylation (+2) to white representing total unmethylation (−2) as shown on the scale to the right hand side of the matrix. Each vertical line of the matrix represents one sample, the type of sample is shown above the matrix,

Breast Cancer Vs. all Other Controls

Microarray 1: See Table 4 for Results.

In this comparison the positive class was 263 breast cancer samples which consisted of 197 IDC, 24 ILC, 22 DCIS and 20 BRCA1 samples, respectively. The negative class consisted of 74 breast samples (normal and benign disease), 71 other cancer samples and 28 lymphocyte samples. Based on multivariate logistic regression analysis 50 markers differentiate between breast cancer and benign breast conditions with statistical significance. Of these, 29 markers fulfilled the co-methylation criterion with at least two detection oligos statistically significant based on univariate analysis.

Microarray 2: See Table 5 for Results.

In this comparison the positive class was 256 breast cancer samples which consisted of 191 IDC, 22 ILC, 21 DCIS and 22 BRCA1 samples, respectively. The negative class consisted of 68 breast samples (normal and benign disease), 73 other cancer samples and 34 lymphocyte samples. Based on multivariate logistic regression 48 markers differentiate between breast cancer and benign breast conditions with statistical significance. Of these, 32 markers fulfilled the co-methylation criterion with at least two detection oligos statistically significant based on univariate analysis.

Results are also presented in graphical form in FIGS. 67-78. Each of said figures presents a matrix of the level of methylation of each significant oligomer, oligomers belonging to each gene or genomic sequence are grouped in one discrete block. The SEQ ID NO: of each oligomer is shown on the left hand side of the matrix, on the right hand side of the matrix the FDR corrected multivariate P-value of the oligomers belonging to each individual gene or genomic sequence is shown. The level of methylation is shown by the color of each square of the matrix, from black representing total methylation (+2) to white representing total unmethylation (−2) as shown on the scale to the right hand side of the matrix. Each vertical line of the matrix represents one sample, the type of sample is shown above the matrix.

Selection of General Cancer Markers

Markers from both microarrays which were significant in differentiating Breast cancer vs. benign breast conditions but were not significant in differentiating Breast cancer vs. other cancers as listed in Table 27 were determined to have utility as general cancer markers.

Example 2

Real-Time Assay Analysis of Breast Cancer Markers

In the following example a variety of Real-Time assays were developed for the methylation analysis of:

SEQ ID NO: 104 (CCND2)

SEQ ID NO: 77 (FABP3)

SEQ ID NO: 90 (RASSF1A)

SEQ ID NO: 13 (MSF)

SEQ ID NO: 15

SEQ ID NO: 20 (PRDM6)

SEQ ID NO: 38 (LMX1A)

SEQ ID NO: 3

SEQ ID NO: 4

SEQ ID NO: 29

SEQ ID NO: 22 (NR2E1)

SEQ ID NO: 115 (SCGB3A1)

SEQ ID NO: 112 (SLIT2)

SEQ ID NO: 6

SEQ ID NO: 98 (DAPK1)

The assays were designed to be run on the LightCycler platform (Roche Diagnostics), but other such instruments commonly used in the art are also suitable. The assays were MSP and HeavyMethyl assays for the analysis of bisulfite treated DNA.

The MSP assay comprises one pair of methylation specific primers suitable for the amplification of a bisulfite converted target sequence, each primer comprising at least one CpG position. Accordingly, only target DNA which was methylated at the relevant CpG positions (prior to bisulfite treatment) is amplified. The amplificate is then detected by means of a Taqman style fluorescent labelled detection probes.

In the HeavyMethyl assay the target DNA is amplified by means of a pair of primers that are specific for amplification of a bisulfite converted target sequence, wherein said primers do not hybridise to positions that comprised CpG dinucleotides prior to bisulfite treatment. Amplification is carried out in the presence of a blocker oligonucleotide that comprises at least one ApC dinucleotide and that hybridises to bisulfite converted non-methylated CpG positions situated between the two primers. The blocker oligonucleotides are suitably modified to suppress amplification of target sequences by the primers. Accordingly, only target DNA which was methylated at the relevant CpG positions (prior to bisulfite treatment) is amplified. Amplificates are detected by means of Lightcycler style fluorescent labelled dual detection probes.

Primer, probe and where relevant blocker oligonucleotides according to Table 22 were used. The following reagents and reaction temperatures were used:

SEQ ID NO: 104 (CCND2) (Assay 4),

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Denaturation at 95° C. for 15 sec
Annealing at 62° C. for    45 sec
Reagents:
Reagent                    Concentration
1a + 1b reagent mix        1.00x
Taqman probe               0.30 μM
Primer mix                 0.60 pmol/μl (each)
MgCl2                      3.50 mM

SEQ ID NO: 77 (FABP3) (Assay 1-5)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Denaturation at 95° C. for 15 sec
Annealing at 62° C. for    45 sec
Reagents:
Reagent                    Concentration
1a + 1b reagent mix        1.00x
Taqman probe               0.30 μM
Primer mix                 0.60 pmol/μl (each)
MgCl2                      3.50 mM

SEQ ID NO: 90 (RASSF1A) (Assay 1)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Initial denaturation at 95° C. for 15 sec
Annealing at 62° C. for          45 sec
Reagents:
Reagent                          Concentration
1a + 1b reagent mix              1.00x
Taqman probe                     0.30 μM
Primer mix                       0.60 pmol/μl (each)
MgCl2                            3.50 mM

SEQ ID NO: 13 (MSF) (Assay 2)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Initial denaturation at 95° C. for 15 sec
Annealing at 62° C. for          45 sec
Reagents:
Reagent                          Concentration
1a + 1b reagent mix              1.00x
Taqman probe                     0.30 μM
Primer mix                       0.60 pmol/μl (each)
MgCl2                            3.50 mM

SEQ ID NO: 15 (Assay 5)

Lightcycler thermal cycling program:
Activation:                   95° C. 10 min
55 cycles:                    95° C. 10 sec
                              56° C. 30 sec
                              72° C. 10 sec
melting curve:                95° C. 10 sec
                              40° C. 10 sec
                              70° C. 0 sec
cooling:                      40° C. 5 sec
Reagents:
Reagent                       Concentration
MgCl2                         3.50 mM
Primer mix                    0.30 μM (each)
Blocker                       4.00 μM
Detection probes              0.15 μM (each)
1a + 1b reagent FastStart mix 1.00

SEQ ID NO: 20 (PRDM6) (Assay 100)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Initial denaturation at 95° C. for 15 sec
Annealing at 62° C. for          45 sec
Reagents:
Reagent                          Concentration
1a + 1b reagent mix              1.00x
Taqman probe                     0.30 μM
Primer mix                       0.60 pmol/μl (each)
MgCl2                            3.50 mM

SEQ ID NO: 38 (LMX1A) (Assay 3)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Initial denaturation at 95° C. for 15 sec
Annealing at 62° C. for          45 sec
Reagents:
Reagent                          Concentration
1a + 1b reagent mix              1.00x
Taqman probe                     0.30 μM
Primer mix                       0.60 pmol/μl (each)
MgCl2                            3.50 mM

SEQ ID NO: 3 (Assay 8)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Denaturation at 95° C. for 15 sec
Annealing at 62° C. for    45 sec
Reagents:
Reagent                    Concentration
1a + 1b reagent mix        1.00x
Taqman probe               0.30 μM
Primer mix                 0.60 pmol/μl (each)
MgCl2                      3.50 mM

SEQ ID NO: 29 (Assay 2)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Denaturation at 95° C. for 15 sec
Annealing at 62° C. for    45 sec
Reagents:
Reagent                    Concentration
1a + 1b reagent mix        1.00x
Taqman probe               0.30 μM
Primer mix                 0.60 pmol/μl (each)
MgCl2                      3.50 mM

SEQ ID NO: 22 (NR2E1) (Assay o)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Denaturation at 95° C. for 15 sec
Annealing at 62° C. for    45 sec
Reagents:
Reagent                    Concentration
1a + 1b reagent mix        1.00x
Taqman probe               0.30 μM
Primer mix                 0.60 pmol/μl (each)
MgCl2                      3.50 mM

SEQ ID NO 115 (SCGB3A1) (Assay 1)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Denaturation at 95° C. for 15 sec
Annealing at 62° C. for    45 sec
Reagents:
Reagent                    Concentration
1a + 1b reagent mix        1.00x
Taqman probe               0.30 μM
Primer mix                 0.60 pmol/μl (each)
MgCl2                      3.50 mM

SEQ ID NO: 112 (SLIT2) (Assay 2-2)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Denaturation at 95° C. for 15 sec
Annealing at 62° C. for    45 sec
Reagents:
Reagent                    Concentration
1a + 1b reagent mix        1.00x
Taqman probe               0.30 μM
Primer mix                 0.60 pmol/μl (each)
MgCl2                      3.50 mM

SEQ ID NO: 6 (Assay 5)

Lightcycler thermal cycling program:
Activation:                   95° C. for 10 min
55 cycles:                    95° C. 10 sec
                              56° C. 30 sec
                              72° C. 10 sec
melting curve:                95° C. 10 sec
                              40° C. 10 sec
                              70° C. 0 sec
cooling:                      40° C. 5 sec
Reagents:
Reagent                       Concentration
MgCl2                         3.50 mM
Primer mix                    0.30 μM (each)
Blocker                       4.00 μM
Detection probes              0.15 μM (each)
1a + 1b reagent FastStart mix 1.00

SEQ ID NO: 98 (DAPK1) (Assay 2)

Lightcycler thermal cycling program:
Initial denaturation at 95° C. for 10 min
55 cycles:
Denaturation at 95° C. for 15 sec
Annealing at 62° C. for    45 sec
Reagents:
Reagent                    Concentration
1a + 1b reagent mix        1.00x
Taqman probe               0.30 μM
Primer mix                 0.60 pmol/μl (each)
MgCl2                      3.50 mM

SEQ ID NO: 22 (NR2E1) (Assay 2)

Lightcycler thermal cycling program:
Activation:                   95° C. 10 min
55 cycles:                    95° C. 10 sec
                              56° C. 30 sec
                              72° C. 10 sec
melting curve:                95° C. 10 sec
                              40° C. 10 sec
                              70° C. 0 sec
cooling:                      40° C. 5 sec
Reagents:
Reagent                       Concentration
MgCl2                         3.50 mM
Primer mix                    0.30 μM (each)
Blocker                       4.00 μM
Detection probes              0.15 μM (each)
1a + 1b reagent FastStart mix 1.00

Samples

The assays were tested in two different settings. In a first setting the following breast cancer markers as confirmed according to the above microarray experiment were analysed in both blood and breast cancer samples in order to determine their utility as diagnostic markers suitable for use in a blood based screening test.

SEQ ID NO: 104 (CCND2)

SEQ ID NO: 77 (FABP3)

SEQ ID NO: 90 (RASSF1A)

SEQ ID NO: 13 (MSF)

SEQ ID NO: 15

SEQ ID NO: 20 (PRDM6)

SEQ ID NO: 38 (LMX1A)

SEQ ID NO: 3

SEQ ID NO: 4

SEQ ID NO: 29

SEQ ID NO: 22 (NR2E1)

SEQ ID NO: 115 (SCGB3A1)

SEQ ID NO: 112 (SLIT2)

SEQ ID NO: 6

SEQ ID NO: 98 (DAPK1)

Ten whole blood samples and 14 breast cancer samples were analysed.

In a second setting the following breast cancer markers as confirmed according to the above microarray experiment were analysed in order to determine whether they were general cancer markers (i.e. would need to be combined with more cancer type specific markers in a blood based screening test) or if they were specifically methylated in breast cancer only (as opposed to other cancers):

SEQ ID NO: 104 (CCND2)

SEQ ID NO: 77 (FABP3)

SEQ ID NO: 90 (RASSF1A)

SEQ ID NO: 13 (MSF)

SEQ ID NO: 20 (PRDM6)

SEQ ID NO: 38 (LMX1A)

All sample were analysed in twenty four breast cancer samples and a “other cancers” sample group consisting of 12 lung cancer and 12 colon cancer samples, with the exception of 17378 wherein data is only presented with respect to a “other cancers” group consisting of the 12 lung cancer samples.

Results

Quantification of the amount of methylated DNA measured by each assay was calculated by comparison of the amplification curve of a test sample to a standard curve. The standard curve was generated according to a dilution series used as a reference.

FIGS. 1 to 12 show the binary distribution plot (left hand side of the figure) of the proportion (Y-axis) of blood and breast cancer samples with a measured methylation level above a specified cut-off point (X-axis). On the right hand side of each figure is a ROC plot of sensitivity against specificity. The ROC curve is a plot of the true positive rate against the false positive rate for the different possible cutpoints of a diagnostic test. It shows the trade-off between sensitivity and specificity depending on the selected cutpoint (any increase in sensitivity will be accompanied by a decrease in specificity). The area under an ROC curve (AUC) is a measure for the accuracy of a diagnostic test (the larger the area the better, optimum is 1, a random test would have a ROC curve lying on the diagonal with an area of 0.5; for reference: J. P. Egan. Signal Detection Theory and ROC Analysis, Academic Press, New York, 1975). Each detected blood sample was considered a false positive and each undetected breast cancer was considered a false negative.

FIGS. 13 to 18 show the binary distribution plots (top left hand side of the figure) of the proportion of blood vs. other cancer samples (Y-axis) with a measured methylation level above a specified cut-off point (X-axis). The bottom left hand side plot show the binary distribution plots (top left hand side of the figure) of the proportion (Y-axis) of each type of cancer sample with a measured methylation level above a specified cut-off point (X-axis).

On the right hand side of each figure is a ROC plot of sensitivity against specificity. The ROC curve is a plot of the true positive rate against the false positive rate for the different possible cutpoints of a diagnostic test. It shows the trade-off between sensitivity and specificity depending on the selected cutpoint (any increase in sensitivity will be accompanied by a decrease in specificity). The area under an ROC curve (AUC) is a measure for the accuracy of a diagnostic test (the larger the area the better, optimum is 1, a random test would have a ROC curve lying on the diagonal with an area of 0.5; for reference: J. P. Egan. Signal Detection Theory and ROC Analysis, Academic Press, New York, 1975).

Each detected other cancer sample was considered a false positive and each undetected breast cancer was considered a false negative.

Refer to Tables 23 and 24 to determine which figure correspond to which assay.

Table 23 shows the AUG and particularly preferred sensitivity and specificities of each assayed gene according to the blood vs. breast cancer comparison.

Table 24 shows the AUG and particularly preferred sensitivity and specificities of each assayed gene according to the other cancer vs. breast cancer comparison.

TABLE 1
Primer according to Example I.
		Amplificate
No:	Primer:	Length:
1. MSF	AATAAACAACCCTCCCCTC	423
(SEQ ID NO: 13)	(SEQ ID NO: 973)
	TGGAGATTATTGTGTGAGTTTT
	(SEQ ID NO: 972)
2. SEQ ID NO: 14	CCAAAAACCTCTACATTCAAAC	358
(SEQ ID NO: 14)	(SEQ ID NO: 975)
	AAAAAGGGGATTAGTGGGT
	(SEQ ID NO: 974)
3. SEQ ID NO: 15	ATTTTAGGTGTAAGTTTAAGGTTGT	473
(SEQ ID NO: 15)	(SEQ ID NO: 976)
	ATCTACCTTTCCCCACCC
	(SEQ ID NO: 977)
4. SEQ ID NO: 16	ACACAACTAAAACCCTCAAATC	262
(SEQ ID NO: 16)	(SEQ ID NO: 979)
	AGGGAAAGGAGGTAGAGGT
	(SEQ ID NO: 978)
5. SEQ ID NO: 17)	ATCACACCCTCCCAAAAC	385
(SEQ ID NO: 17)	(SEQ ID NO: 981)
	AGTAGGAATTGTTTATAGATATGTTGA
	(SEQ ID NO: 980)
6. SEQ ID NO: 18	ACTCCCCAAAATCCCACT	488
(SEQ ID NO: 18)	(SEQ ID NO: 983)
	TGTTTTAGGTTTGATGGATTAGA
	(SEQ ID NO: 982)
7. SEQ ID NO: 19	AAAACCCCATCTCTACAACC	498
(SEQ ID NO: 19)	(SEQ ID NO: 985)
	AATGAGAGGGAAAATGAAAGT
	(SEQ ID NO: 984)
8. PRDMG	ACTTCCAATCTTAAAAACCAAA	272
(SEQ ID NO: 20)	(SEQ ID NO: 987)
	GGAGGAGAGGATGAAGTTTTA
	(SEQ ID NO: 986)
9. RAP2B	CTCAACCTACAAACAAATCTTAAC	176
(SEQ ID NO: 21)	(SEQ ID NO: 989)
	AGGGGTAGGGGAGTGTTT
	(SEQ ID NO: 988)
10. NR2E1	CACCCCTACAACCCAAAC	495
(SEQ ID NO: 22)	(SEQ ID NO: 991)
	GGTGGAGGGAAGATTAGTGTA
	(SEQ ID NO: 990)
11. NR2E1	CCTTAAAAACCTCCAACCC	343
(SEQ ID NO: 22)	(SEQ ID NO: 993)
	GGTTGTTGAAAGAAGTTAGTTTG
	(SEQ ID NO: 992)
12. PCDH7	TCAATTCAAAAACACAACCAA	448
(SEQ ID NO: 23)	(SEQ ID NO: 995)
	AATTTTAGAGAGTTGGAGAAAGAT
	(SEQ ID NO: 994)
13. DKK3	TAGGTATAGTAGGGTGGTTTTTAGT	338
(SEQ ID NO: 24)	(SEQ ID NO: 996)
	AAAACTCCAACATCACAAATAA
	(SEQ ID NO: 997)
14. RTTN	TTCAAAAACAAACCACTAATACC	438
(SEQ ID NO: 25)	(SEQ ID NO: 999)
	GTGATTTTAGAGAGGTTGGAAG
	(SEQ ID NO: 998)
15. BCL11B	CCCCAAACTATAACCAACTTTA	381
(SEQ ID NO: 50)	(SEQ ID NO: 1001)
	TATGGGATTGGAAGGGAT
	(SEQ ID NO: 1000)
16. COL5A1	GATTAGTAGGAGGGGTTGTTTA	500
(SEQ ID NO: 53)	(SEQ ID NO: 1002)
	AAATCCCACATCTACATATCATC
	(SEQ ID NO: 1003)
17. SEQ ID NO: 51	GTAGGGGTGGAGTGAAGG	404
(SEQ ID NO: 51)	(SEQ ID NO: 1004)
	CACTCAAAACTCCCAAATAAAA
	(SEQ ID NO: 1005)
18. MGC34831	AATGAGAGTAGGGTTTGAAATTAG	273
(SEQ ID NO: 52)	(SEQ ID NO: 1006)
	TATCCAAAAACTTCACCTCAAC
	(SEQ ID NO: 1007)
19. SEQ ID NO: 54	TGGGATGAAGAAGTAGTGTGTT	398
(SEQ ID NO: 54)	(SEQ ID NO: 1008)
	CTCCAACTAAACATTAAATAAATCTCA
	(SEQ ID NO: 1009)
20. PDLIM1	GGTTTATTTGTTGGGTGGTTA	440
(SEQ ID NO: 55)	(SEQ ID NO: 1010)
	CTATCAAAACCTACTTCCCTCTC
	(SEQ ID NO: 1011)
21. KOX7	ACCACCACAAATATCCCAA	423
(SEQ ID NO: 49)	(SEQ ID NO: 1013)
	GAGGTTAAGGGATGGTTTTATT
	(SEQ ID NO: 1012)
22. SEQ ID NO: 3	TCCTCAACTCTACAAACCTAAAA	408
(SEQ ID NO: 3)	(SEQ ID NO: 1015)
	GTAGGGGAGGGAAGTAGATGT
	(SEQ ID NO: 1014)
23. SEQ ID NO: 4	TGTTTGGGTTAGATGGGG	378
(SEQ ID NO: 4)	(SEQ ID NO: 1016)
	ATTCTCAACCACCAAAATCTAC
	(SEQ ID NO: 1017)
24. SEQ ID NO: 1	CCTCTAATTCCTATCAATCACC	435
(SEQ ID NO: 1)	(SEQ ID NO: 1019)
	TTAGAAGTGAAAGTAGAAGGGTTT
	(SEQ ID NO: 1018)
25. SEQ ID NO: 9	GAAAGGAGAGGTTAAAGGTTG	696
(SEQ ID NO: 9)	(SEQ ID NO: 1020)
	AACTCACTTAACTCCAATCCC
	(SEQ ID NO: 1021)
26. SEQ ID NO: 5	TTCTATTAAAACCCAACTCCTC	395
(SEQ ID NO: 5)	(SEQ ID NO: 1023)
	ATAAGGGGAATTGTTGTAGGTT
	(SEQ ID NO: 1022)
27. SEQ ID NO: 6	AGGGAGTTAAGTAAGGGGTTAG	442
(SEQ ID NO: 6)	(SEQ ID NO: 1024)
	AACACCAACAAAATATCCATCT
	(SEQ ID NO: 1025)
28. SEQ ID NO: 8	TAGTAGTTTGAAGAAGGGGAAG	373
(SEQ ID NO: 8)	(SEQ ID NO: 1026)
	AAACATTCCTAAAATCACAAAAA
	(SEQ ID NO: 1027)
29. SEQ ID NO: 6	AGATGGATATTTTGTTGGTGTT	250
(SEQ ID NO: 6)	(SEQ ID NO: 1028)
	TACACAATTATACCTTTCAAACAAT
	(SEQ ID NO: 1029)
30. SEQ ID NO: 7	CAAACCCAATTCTCAATATCC	434
(SEQ ID NO: 7)	(SEQ ID NO: 1031)
	GAAGTTGTTGTATATGAGGTTGTTA
	(SEQ ID NO: 1030)
31. PROSTAGLANDIN	GAAGAGGAATGGGAAAATTAG	500
E2 RECEPTOR, EP4	(SEQ ID NO: 1032)
SUBTYPE	TCACCAACAAAATACCCAA
(PROSTANOID EP4	(SEQ ID NO: 1033)
RECEPTOR) (PGE
RECEPTOR, EP4
SUBTYPE)
(SEQ ID NO: 10)
32. PROSTAGLANDIN	AACCATCAACCATACCTATTTC	467
E2 RECEPTOR, EP4	(SEQ ID NO: 1035)
SUBTYPE	TGAGTAAGATGATTATTTGGATTT
(PROSTANOID EP4	(SEQ ID NO: 1034)
RECEPTOR) (PGE
RECEPTOR, EP4
SUBTYPE)
(SEQ ID NO: 10)
33. ORPHAN	CCACTCACTCAACCCATAA	398
NUCLEAR	(SEQ ID NO: 1037)
RECEPTOR NR5A2	GTGTGAGGTTTGGGTATTTTT
(ALPHA-1-	(SEQ ID NO: 1036)
FETOPROTEIN
TRANSCRIPTION
FACTOR)
(HEPATOCYTIC
TRANSCRIPTION
FACTOR) (B1-
BINDING FACTOR)
(HB1F) (CYP7A
PROMOTER
BINDING FACTOR)
(SEQ ID NO: 11)
34. LIM DOMAIN	AAACCCTACTTCCTACAAACAA	420
KINASE 1 (EC	(SEQ ID NO: 1039)
2.7.1.37) (LIMK-1)	AGGGAGGTTTGGTGTATTTT
(SEQ ID NO: 12)	(SEQ ID NO: 1038)
36. HOXB13	CTCACACTCTTTAACCTTTTCC	496
(SEQ ID NO: 34)	(SEQ ID NO: 1041)
	GAGAGGGATATGAGGGTTTTT
	(SEQ ID NO: 1040)
37. SEQ ID NO: 35	TAAATCCCCCAACACATACTAC	473
	(SEQ ID NO: 1043)
	GTTTATTGGTTTTTATAGATTAAGG
	(SEQ ID NO: 1042)
38. SEQ ID NO: 36	AGGGGTGAGTTTTATTAGAGGT	479
	(SEQ ID NO: 1044)
	CTAAACCCCAATCTCTCCA
	(SEQ ID NO: 1045)
39. MGC10561	AAAACCATAAAATCCCACATAA	486
(SEQID NO: 37)	(SEQ ID NO: 1047)
	TTTTTGGGAGGGAAGAGT
	(SEQ ID NO: 1046)
40. LMX1A	AACAACACTCTTACCCTTATCC	490
(SEQ ID NO: 38)	(SEQ ID NO: 1049)
	TGAATGTGGAGGATGAGATAGT
	(SEQ ID NO: 1048)
41. SENP3	GGTTAAGGAAGGTAGGAGATTT	466
(SEQ ID NO: 39)	(SEQ ID NO: 1050)
	CTTCCAAACTAAAAACCACTTT
	(SEQ ID NO: 1051)
42. GSI	ATCACCATTCAAAATACAAATATC	470
(SEQ ID NO: 40)	(SEQ ID NO: 1053)
	GTTTTGGAGATTAGTTGGGG
	(SEQ ID NO: 1052)
43. TTTF1	CTTACTCCCTCAATACAAAACC	467
(SEQ ID NO: 41)	(SEQ ID NO: 1055)
	GAGAGAAAGAAGTTGGGTGAT
	(SEQ ID NO: 1054)
44. SEQ ID NO: 42	GAGAAAAAGAGGGAGATTATTG	336
(SEQ ID NO: 42)	(SEQ ID NO: 1056)
	CCACATTCAAAAACACAAATAC
	(SEQ ID NO: 1057)
45. DDX51	CAAACTCACTCTATAACCTCCC	482
(SEQ ID NO: 43)	(SEQ ID NO: 1059)
	TTTAGGGGTTTGGATTTTG
	(SEQ ID NO: 1058)
46. SEQ ID NO: 117	GGTTAGGGTGGGTAAAGGTAG	288
	(SEQ ID NO: 1060)
	CCTTTCCTTCAAATAACAAAAC
	(SEQ ID NO: 1061)
47. Q8NAN2	TTGTATAGGAAAGTAGGAGGGTT	307
(SEQ ID NO: 44)	(SEQ ID NO: 1062)
	AAACAAAATAATCTTTCACATCC
	(SEQ ID NO: 1063)
48. SEQ ID NO: 45	CAAAACAAATTAACTCCCCC	461
(SEQ ID NO: 45)	(SEQ ID NO: 1065)
	AGGGTGATAGTATAAAGGAAATTG
	(SEQ ID NO: 1064)
49. SEQ ID NO: 46	TCCTCTACCCTTCACCTACC	383
(SEQ ID NO: 46)	(SEQ ID NO: 1067)
	TGGAAGATAATGTGTTATTTAGTATTT
	(SEQ ID NO: 1066)
50. O60279	TTAAAAGGGAATGGATATAGAGTT	485
(SEQ ID NO: 47)	(SEQ ID NO: 1068)
	ACTTTCCTAAAATCTCCAAAAA
	(SEQ ID NO: 1069)
51. SEQ ID NO: 48	TATTTTTGGGGATGAAGAAAAT	484
(SEQ ID NO: 48)	(SEQ ID NO: 1070)
	ACAAAATCTCCTTTCATTTAACA
	(SEQ ID NO: 1071)
52. SEQ ID NO: 2	TCCAATAAACACAAACCTAAATC	471
(SEQ ID NO: 2)	(SEQ ID NO: 1212)
	ATATGGGATTGATGGAAGATAG
	(SEQ ID NO: 1213)
53. SNAP25	ACTCCACCACAATTACAACCTA	352
(SEQ ID NO: 33)	(SEQ ID NO: 1075)
	AGAAAGAGGGGGTTTTATTATT
	(SEQ ID NO: 1074)
54. SEQ ID NO: 26	CTTTACCCATCAACAACCCTA	257
(SEQ ID NO: 26)	(SEQ ID NO: 1077)
	GGAGGTGTGATTTTATTGTTTG
	(SEQ ID NO: 1076)
55. GIRK2	ACCTTCCACAAAAACAATAAAC	457
(SEQ ID NO: 27)	(SEQ ID NO: 1079)
	TTTTAAGAGAGGAGATTATGATTGA
	(SEQ ID NO: 1078)
56. SEQ ID NO: 28	GTTGAGAGGTAAGGTATGAAGG	477
(SEQ ID NO: 28)	(SEQ ID NO: 1080)
	TTAATTCCCCTCTTTAACCTAATAA
	(SEQ ID NO: 1081)
57. SEQ ID NO: 28	TACAAAAATAAACTCAAAATCCCTA	477
(SEQ ID NO: 28)	(SEQ ID NO: 1083)
	TTTTTAAGGGAAAGTGGAGG
	(SEQ ID NO: 1082)
58. SEQ ID NO: 29	GAGAGAAATGGGTGATGAAGT	493
(SEQ ID NO: 29)	(SEQ ID NO: 1084)
	CCCAACAAATAAAACCCC
	(SEQ ID NO: 1085)
59. ARL7	TTGAATGTAAGGAGAGGTGG	385
(SEQ ID NO: 30)	(SEQ ID NO: 1086)
	AAATCTCTACACCCAAATACAAA
	(SEQ ID NO: 1087)
60. SEQ ID NO: 31	CTCAACAAATAAACTTCACAAAA	435
(SEQ ID NO: 31)	(SEQ ID NO: 1089)
	TTTTTGGAGATAGTAGGAAGGG
	(SEQ ID NO: 1088)
61. THH	GTTTTAGGAAAGGGAGAGGG	475
(SEQ ID NO: 32)	(SEQ ID NO: 1090)
	TTAATTCACTCCCACCAATAAA
	(SEQ ID NO: 1091)
62. APC	TCAACTACCATCAACTTCCTTA	491
(SEQ ID NO: 65)	(SEQ ID NO: 1092)
	AATTTATTTTTAGTGTTGTAGTGGG
	(SEQ ID NO: 1093)
63. ESR1	AACTATACTCTTTTTCCAAATAACC	197
(SEQ ID NO: 75)	(SEQ ID NO: 1095)
	TTTTAGGGGGATTTTGAGTT
	(SEQ ID NO: 1094)
64. MLH1	TTTTAGGAGTGAAGGAGGTTA	442
(SEQ ID NO: 89)	(SEQ ID NO: 1096)
	ATATCCAACCAATAAAAACAAA
	(SEQ ID NO: 1097)
65. TIMP3	TTTGTTTTAGGAGAGGGGTAG	487
(SEQ ID NO: 103)	(SEQ ID NO: 1098)
	CTTAAATCCACCCAAACTTAAC
	(SEQ ID NO: 1099)
66. CDKN1A	AGTTAGAAAGGGGGTTTATTTT	452
(SEQ ID NO: 67)	(SEQ ID NO: 1100)
	TCTCTCACCTCCTCTAAATACC
	(SEQ ID NO: 1101)
67. TP53	AATAATTTCCACCAATTCTACC	251
(SEQ ID NO: 80)	(SEQ ID NO: 1103)
	TTAGTTTTGAGTATATGGGAGGG
	(SEQ ID NO: 1102)
68. GSTP1	ATTTGGGAAAGAGGGAAAG	301
(SEQ ID NO: 59)	(SEQ ID NO: 1104)
	TAAAAACTCTAAACCCCATCC
	(SEQ ID NO: 1105)
69. PGR	ATGATTGAGTTGAAGGTAAAGG	347
(SEQ ID NO: 83)	(SEQ ID NO: 1106)
	TCCAAAACACTATCCAACAAT
	(SEQ ID NO: 1107)
70. RARB	GGGAGTTTTTAAGTTTTGTGAG	415
(SEQ ID NO: 88)	(SEQ ID NO: 1108)
	AATCATTTACCATTTTCCAAAC
	(SEQ ID NO: 1109)
71. CASP8	ACCCCCTTCCCTACTAAAC	436
(SEQ ID NO: 71)	(SEQ ID NO: 1110)
	TTAGGGTTAAATGAAAAAGAAAA
	(SEQ ID NO: 1111)
72. SNCG	ACCCTTTAACCACCACACTAT	444
(SEQ ID NO: 73)	(SEQ ID NO: 1112)
	TTGGGTTGAGTTAGTAGGAGTT
	(SEQ ID NO: 1113)
73. TGFBR2	GGATGGTTAGAGAGTTGAAATG	374
(SEQ ID NO: 93)	(SEQ ID NO: 1114)
	AAAATCCTACACTTCCTACAACA
	(SEQ ID NO: 1115)
74. THBS1	CCCCCTTCACTTTCTAACTAA	497
(SEQ ID NO: 81)	(SEQ ID NO: 1117)
	AGAGGATGGTTTTGGAGTTT
	(SEQ ID NO: 1116)
75. CDH1	CCCTTTCTAATCCCAAATCT	421
(SEQ ID NO: 79)	(SEQ ID NO: 1119)
	GTTTTAAGGGTTTATGGTTGG
	(SEQ ID NO: 1118)
76. DAPK1	GGTGGGTATGTGTGTAGAGAA	407
(SEQ ID NO: 98)	(SEQ ID NO: 1120)
	AAACCCAAAACACTTCAACTC
	(SEQ ID NO: 1121)
77. TP73	AGAGGGGATAGTAGGAGGA	322
(SEQ ID NO: 86)	(SEQ ID NO: 1122)
	ACTACAAATAAAAAACCCAAAAC
	(SEQ ID NO: 1123)
78. SFN	TTTTTGATGAGGTGGTTGTT	489
(SEQ ID NO: 69)	(SEQ ID NO: 1124)
	AAACAAATCTTAAACCCTAATCC
	(SEQ ID NO: 1125)
79. HIC1	TTTTTAAAAGGGGGTTTTAGGT	589
(SEQ ID NO: 85)	(SEQ ID NO: 1126)
	TACCCTTCCAAAAACTAAAAAAAAC
	(SEQ ID NO: 1127)
80. RASSF1A	AGTGGGTAGGTTAAGTGTGTTG	319
(SEQ ID NO: 90)	(SEQ ID NO: 1128)
	CCCCAAAATCCAAACTAAA
	(SEQ ID NO: 1129)
81. BRCA1	TTGGAAGAGTAGAGGTTAGAGG	425
(SEQ ID NO: 66)	(SEQ ID NO: 1130)
	TACCCCAAAACATCACTTAAAC
	(SEQ ID NO: 1131)
82. APAF1	TTGGGGTGTGTTTATTTGTAT	451
(SEQ ID NO: 82)	(SEQ ID NO: 1132)
	CTCCCCTAAATCTCTACAACC
	(SEQ ID NO: 1133)
83. TMS1/ASC	GGATTAAGGGTGTAGTAAGGAA	364
(SEQ ID NO: 84)	(SEQ ID NO: 1134)
	TCTCCAAATAAAAACTAACCAAC
	(SEQ ID NO: 1135)
84. HOXA5	AATCCTACCTAATAACCTCTAAAAAT	361
(SEQ ID NO: 78)	(SEQ ID NO: 1137)
	GGGGAAATAAAGTTGTTGTAAA
	(SEQ ID NO: 1136)
85. SASH1	TTTTGTAGTGGGTTTAATTGTTTT	500
(SEQ ID NO: 102)	(SEQ ID NO: 1138)
	ATAACTTACCAAAATACCCATCA
	(SEQ ID NO: 1139)
86. BRCA2	ACCCACCCAAACCTAACT	388
(SEQ ID NO: 56)	(SEQ ID NO: 1141)
	GGTTGGTAGAGATAAAAGGGTA
	(SEQ ID NO: 1140)
87. NME1	CACCCAAACTAAAATACCCTAA	306
(SEQ ID NO: 107)	(SEQ ID NO: 1143)
	GGAAAAAGTTGATAAATTGGAA
	(SEQ ID NO: 1142)
88. TPM1	GGGAAAGGGTAGGTAGAAAATA	386
(SEQ ID NO: 110)	(SEQ ID NO: 1144)
	ACACCCAACCATTAAAATCC
	(SEQ ID NO: 1145)
89. SOD2	CCTATCCTAAAATAAATCCCAA	441
(SEQ ID NO: 105)	(SEQ ID NO: 1147)
	GGAGAAAGGAGGTTGTAGGTT
	(SEQ ID NO: 1146)
90. THRB	GGGTATTGGTAATTTGGTTAGA	452
(SEQ ID NO: 106)	(SEQ ID NO: 1148)
	CACACAACTTCCTCATCATAAA
	(SEQ ID NO: 1149)
91. TWIST	GTGGGGATGAAATGGTTATAG	354
(SEQ ID NO: 100)	(SEQ ID NO: 1150)
	AACCCCTTAAAATTCCAAAA
	(SEQ ID NO: 1151)
92. IL6	CAAAAACAAACTCCCAACTATAC	485
(SEQ ID NO: 99)	(SEQ ID NO: 1153)
	AAGGTGGGTATGGATTTTAGA
	(SEQ ID NO: 1152)
93. RARA	CATATACATTTCCATCCTTCCT	305
(SEQ ID NO: 108)	(SEQ ID NO: 1155)
	ATAAATATAGGTAGAGGGGGTTTT
	(SEQ ID NO: 1154)
94. CDH13	GGAAAAGTGGAATTAGTTGGTA	407
(SEQ ID NO: 70)	(SEQ ID NO: 1156)
	TCTTCCCTACCTAAAACAAAAA
	(SEQ ID NO: 1157)
95. CLDN7	TCCTTTCTTCCCAACAAATA	345
(SEQ ID NO: 87)	(SEQ ID NO: 1159)
	TTGAGTGTAAAGGGTTTAGGTT
	(SEQ ID NO: 1158)
96. ESR2	AGTTGGAGAAATTGAAAAGATTA	441
(SEQ ID NO: 91)	(SEQ ID NO: 1160)
	TAACAAACCCAAAACCTCTCTA
	(SEQ ID NO: 1161)
97. IGFBP7	CCTCTCTCTACATCCCCAAA	414
(SEQ ID NO: 94)	(SEQ ID NO: 1163)
	GGGAGAAGGTTATTATTTAGGTT
	(SEQ ID NO: 1162)
98. FHIT	GGGAGGTAAGTTTAAGTGGAAT	302
(SEQ ID NO: 76)	(SEQ ID NO: 1164)
	ACTACACCCCCAAAACCA
	(SEQ ID NO: 1165)
99. SERPINB5	TTTTTGTTTAATGGGTAGTTATTTT	353
(SEQ ID NO: 68)	(SEQ ID NO: 1166)
	CTCCTCTCCTACTCAAACCTC
	(SEQ ID NO: 1167)
100. LOT1	AGAGGAAAGAGAGTAGTTGGTG	479
(SEQ ID NO: 95)	(SEQ ID NO: 1168)
	TATAAAATTCTCCCAACCAAAA
	(SEQ ID NO: 1169)
101. PLAU	GTGATATTTGGGGATTGTTATT	479
(SEQ ID NO: 62)	(SEQ ID NO: 1170)
	ACTCCCTCCCCTATCTTACA
	(SEQ ID NO: 1171)
102. PRSS8	GGTTTGTAGTTTTGAAAGGATT	481
(SEQ ID NO: 72)	(SEQ ID NO: 1172)
	AATACATTATCCCCACCCTAC
	(SEQ ID NO: 1173)
103. S100A7	TATCCTACCCCCATAACTATCA	243
(SEQ ID NO: 96)	(SEQ ID NO: 1175)
	AGTTTGAGATTTGGTTTATTTTG
	(SEQ ID NO: 1174)
104. SLC19A1	TAGGGGAAAGTGATTTTGA	459
(SEQ ID NO: 116)	(SEQ ID NO: 1176)
	TTTTCCTTTTAACACCCTAAAAC
	(SEQ ID NO: 1177)
105. SYK	GTGGGTTTTGGGTAGTTATAGA	485
(SEQ ID NO: 60)	(SEQ ID NO: 1178)
	TAACCTCCTCTCCTTACCAA
	(SEQ ID NO: 1179)
106. TERT	TAGGTTTTGGATGTTAGGGATT	483
(SEQ ID NO: 92)	(SEQ ID NO: 1180)
	ACCACCTCCTCACCTAAACT
	(SEQ ID NO: 1181)
107. GJB2	ATTTTGAGGGGAGAAAGAAG	450
(SEQ ID NO: 111)	(SEQ ID NO: 1182)
	CCCATAAATTCCCCAAATAC
	(SEQ ID NO: 1183)
108. FABP3	TAGGAAAGGGAGAAGGTTTTAT	488
(SEQ ID NO: 77)	(SEQ ID NO: 1184)
	CTATTCCCCAATCTTAACCAA
	(SEQ ID NO: 1185)
109. GPC3	TCAAATCTAACAAACCACAAAA	489
(SEQ ID NO: 118)	(SEQ ID NO: 1187)
	AATTATTGTAGAGGGGTTGTAGG
	(SEQ ID NO: 1186)
110. ARH1/NOEY2	TGGTAGAAGAGTAGTATTAGTGGTTT	279
(SEQ ID NO: 97)	(SEQ ID NO: 1188)
	CCAATCCCTTTTCCAAATA
	(SEQ ID NO: 1189)
111. SLIT2	AAATTACCCAAACATCCTTCA	309
(SEQ ID NO: 112)	(SEQ ID NO: 1191)
	AGGTATAAGATAGAAGAGGGGATTT
	(SEQ ID NO: 1190)
112. HS3ST2	CAAAAACTTCTCCAAAAATCC	171
(SEQ ID NO: 113)	(SEQ ID NO: 1193)
	TATAATGAGGGTTTGGGGTAAT
	(SEQ ID NO: 1192)
113. STAT1	TGTTTTGGTAGTGAAGAGGATT	372
(SEQ ID NO: 109)	(SEQ ID NO: 1194)
	AACATTAAACCCTTCCATCTTT
	(SEQ ID NO: 1195)
114. PRDM2	CCAACTCATCTCCAACCTATAC	438
(SEQ ID NO: 114)	(SEQ ID NO: 1197)
	AGAATTAAAAAGATTGAAGGAGG
	(SEQ ID NO: 1196)
115. MCT1	CTCTATCACTTCTTCCCTCTCA	430
(SEQ ID NO: 101)	(SEQ ID NO: 1199)
	AATTTTAGGGAGTTAGGATGGTA
	(SEQ ID NO: 1198)
116. IGSF4	TAATCCCCAACTTCCTTAAAAA	489
(SEQ ID NO: 74)	(SEQ ID NO: 1201)
	GGAGTGGAGAGTAAGAAGGTAG
	(SEQ ID NO: 1200)
117. SCGB3A1	TTTAGTGTTTAATGTTTGGGGT	395
(SEQ ID NO: 115)	(SEQ ID NO: 1202)
	CAATTCCTAACTCCCTAATCC
	(SEQ ID NO: 1203)
118. AR	AATATAGGGAGGTTTAGGGTTT	424
(SEQ ID NO: 61)	(SEQ ID NO: 1204)
	TAACCATACATTTCTCATCCAA
	(SEQ ID NO: 1205)
119. EYA4	GGAAGAGGTGATTAAATGGAT	226
(SEQ ID NO: 58)	(SEQ ID NO: 1206)
	CCCAAAAATCAAACAACAA
	(SEQ ID NO: 1207)
120. LEF1	ATAGAATGGTTAGGGGGTATTT	484
(SEQ ID NO: 63)	(SEQ ID NO: 1209)
	TACAAATATCAACCTCTCTCCC
	(SEQ ID NO: 1208)
121. ALX4	CTCCTCCTTCCAACAAAAA	487
(SEQ ID NO: 64)	(SEQ ID NO: 1210)
	GTTTAGAGGTTTTGGGATGATT
	(SEQ ID NO: 1211)
122. SEQ ID NO: 2	TCCAATAAACACAAACCTAAATC	471
(SEQ ID NO: 2)	(SEQ ID NO: 1212)
	ATATGGGATTGATGGAAGATAG
	(SEQ ID NO: 1213)
123. CCND2	GGAGGAAGGAGGTGAAGA	378
(SEQ ID NO: 104)	(SEQ ID NO: 1214)
	CCCCTACATCTACTAACAAACC
	(SEQ ID NO: 1215)
124. CDKN2A	GGGGTTGGTTGGTTATTAGA	256
(SEQ ID NO: 57)	(SEQ ID NO: 1216)
	AACCCTCTACCCACCTAAAT
	(SEQ ID NO: 1217)

TABLE 2
Detection oligonucleotides according to Example 2.
No:	Gene	Oligo:
1	SEQ ID NO: 5	AATGAGCGAGAAAGTA
	(SEQ ID NO: 5)	(SEQ ID NO: 1970)
2	SEQ ID NO: 5	AGAATGAGTGAGAAAGT
	(SEQ ID NO: 5)	(SEQ ID NO: 1971)
3	SEQ ID NO: 5	ATTAAACGGGATGGTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1972)
4	SEQ ID NO: 5	AATATTAAATGGGATGGT
	(SEQ ID NO: 5)	(SEQ ID NO: 1973)
5	SEQ ID NO: 5	GAGTTGCGAGGATTTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1974)
6	SEQ ID NO: 5	GGAGTTGTGAGGATTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1975)
7	SEQ ID NO: 5	TATGAGGTCGTATTGG
	(SEQ ID NO: 5)	(SEQ ID NO: 2196)
8	SEQ ID NO: 5	TATGAGGTTGTATTGGT
	(SEQ ID NO: 5)	(SEQ ID NO: 2197)
9	SEQ ID NO: 5	GGGAATCGTTGATTTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1976)
10	SEQ ID NO: 5	AGGGGAATTGTTGATT
	(SEQ ID NO: 5)	(SEQ ID NO: 1977)
11	SEQ ID NO: 6	AAGTTTATCGGCGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1838)
12	SEQ ID NO: 6	AGAAGTTTATTGGTGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1839)
13	SEQ ID NO: 6	ATTTCGGAATTTAAGCGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1840)
14	SEQ ID NO: 6	TTTTGGAATTTAAGTGTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1841)
15	SEQ ID NO: 6	TAATTTCGGACGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1842)
16	SEQ ID NO: 6	TTTTGGATGTGGAGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1843)
17	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1844)
18	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1845)
19	SEQ ID NO: 6	TTTCGGTTTTCGTTAAT
	(SEO ID NO: 6)	(SEQ ID NO: 1846)
20	SEQ ID NO: 6	TTTGGTTTTTGTTAATTTAG
	(SEO ID NO: 6)	(SEQ ID NO: 1847)
21	SEQ ID NO: 6	TGTGCGAAGTTAACGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1848)
22	SEQ ID NO: 6	TTGTGTGAAGTTAATGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1849)
23	SEQ ID NO: 7	TAGTCGTCGTGTAGGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1978)
24	SEQ ID NO: 7	TAGGTAGTTGTTGTGTA
	(SEQ ID NO: 7)	(SEQ ID NO: 1979)
25	SEQ ID NO: 7	TATAGGTACGCGATGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1980)
26	SEQ ID NO: 7	AGGTATGTGATGAGGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1981)
27	SEQ ID NO: 7	TATGGTTACGTACGAG
	(SEQ ID NO: 7)	(SEQ ID NO: 1982)
28	SEQ ID NO: 7	ATGGTTATGTATGAGTTT
	(SEQ ID NO: 7)	(SEQ ID NO: 1983)
29	SEQ ID NO: 7	ATGATTTGCGTTACGT
	(SEQ ID NO: 7)	(SEQ ID NO: 1984)
30	SEQ ID NO: 7	ATGATTTGTGTTATGTTT
	(SEQ ID NO: 7)	(SEQ ID NO: 1985)
31	SEQ ID NO: 7	TAACGTTGTGGTTCGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1986)
32	SEQ ID NO: 7	TAATGTTGTGGTTTGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1987)
33	SEQ ID NO: 8	ATAGGGCGGGATTTTA
	(SEQ ID NO: 8)	(SEQ ID NO: 2186)
34	SEQ ID NO: 8	GATAGGGTGGGATTTT
	(SEQ ID NO: 8)	(SEQ ID NO: 2187)
35	SEQ ID NO: 8	ATAAAGCGGGGTTTTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1850)
36	SEQ ID NO: 8	GGATAAAGTGGGGTTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1851)
37	SEQ ID NO: 8	AGGAGGCGAGAAATTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1852)
38	SEQ ID NO: 8	GAGGAGGTGAGAAATT
	(SEQ ID NO: 8)	(SEQ ID NO: 1853)
39	SEQ ID NO: 8	AGAAATTTCGGGGTAG
	(SEQ ID NO: 8)	(SEQ ID NO: 1354)
40	SEQ ID NO: 8	GAAATTTTGGGGTAGTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1855)
41	SEQ ID NO: 8	GGTAGTATCGTTTATAGA
	(SEQ ID NO: 8)	(SEQ ID NO: 1856)
42	SEQ ID NO: 8	GGGGTAGTATTGTTTATA
	(SEQ ID NO: 8)	(SEQ ID NO: 1857)
43	SEQ ID NO: 1	GGTCGGCGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1988)
44	SEQ ID NO 1	GGTTGGTGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1989)
45	SEQ ID NO: 1	GATTCGAACGGATTTT
	(SEQ ID NO: 1)	(SEQ ID NO: 1990)
46	(SEQ ID NO: 1	GGGATTTGAATGGATTT
	(SEQ ID NO: 1)	(SEQ ID NO: 1991)
47	SEQ ID NO: 1	TGGGTCGGGATTCGAA
	(SEQ ID NO: 1)	(SEQ ID NO: 1992)
48	SEQ ID NO: 1	TGGGTTGGGATTTGAA
	(SEQ ID NO: 1)	(SEQ ID NO: 1993)
49	SEQ ID NO: 1	GTCGGAAGTTTCGGGA
	(SEQ ID NO: 1)	(SEQ ID NO: 1994)
50	SEQ ID NO: 1	GTTGGAAGTTTTGGGAT
	(SEQ ID NO: 1)	(SEQ ID NO: 1995)
51	SEQ ID NO: 1	TGGATATCGTAGGGTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1996)
52	SEQ ID NO: 1	TGGATATTGTAGGGTAG
	(SEQ ID NO: 1)	(SEQ ID NO: 1997)
53	PROSTAGLANDIN E2 RECEPTOR, EP4	AGTGTATCGTTTTTCGG
	SUBTYPE (PROSTANOID EN RECEPTOR)	(SEQ ID NO: 1858)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
54	PROSTAGLANDIN E2 RECEPTOR, EP4	TAGTGTATTGTTTTTTGG
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1859)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
55	PROSTAGLANDIN E2 RECEPTOR, EP4	TTCGTTTACGGTAGTT
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1218)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
56	PROSTAGLANDIN E2 RECEPTOR, EP4	ATTTTTGTTTATGGTAGTT
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1219)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
57	PROSTAGLANDIN E2 RECEPTOR, EP4	TGCGTATCGTTAGTTA
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1860)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
58	PROSTAGLANDIN E2 RECEPTOR EP4	AGGTTGTGTATTGTTAG
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1861)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
59	PROSTAGLANDIN E2 RECEPTOR, EP4	AGGTAATCGAGGCGGT
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1998)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
60	PROSTAGLANDIN E2 RECEPTOR, EP4	AGGTAATTGAGGTGGT
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1999)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
61	PROSTAGLANDIN E2 RECEPTOR, EP4	ATTATTTCGGCGGTGA
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1862)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
62	PROSTAGLANDIN E2 RECEPTOR, EP4	GATTATTTTGGTGGTGA
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1863)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
63	PROSTAGLANDIN E2 RECEPTOR, EP4	GGCGTCGAAAGTCGTT
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 2000)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
64	PROSTAGLANDIN E2 RECEPTOR, EP4	GGTGTTGAAAGTTGTTG
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 2001)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
65	PROSTAGLANDIN E2 RECEPTOR, EP4	TAAGTCGCGTAAGGAG
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1864)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
66	PROSTAGLANDIN E2 RECEPTOR, EP4	AAGTTGTGTAAGGAGTA
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1865)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
67	PROSTAGLANDIN E2 RECEPTOR, EP4	TAATCGTTTGTTTACGT
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 2002)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
68	PROSTAGLANDIN E2 RECEPTOR, EP4	AATTGTTTGTTTATGTAGT
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 2003)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
69	PROSTAGLANDIN E2 RECEPTOR, EP4	GTATCGCGAGTTTGGA
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1866)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
70	PROSTAGLANDIN E2 RECEPTOR, EP4	GTATTGTGAGTTTGGAG
	SUBTYPE (PROSTANOID EP4 RECEPTOR)	(SEQ ID NO: 1867)
	(PGE RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
71	ORPHAN NUCLEAR RECEPTOR NR5A2	TTACGGAGGCGTTTTA
	(ALPHA-1-FETOPROTEIN TRANSCRIPTION)	(SEQ ID NO: 2004)
	FACTOR) (HEPATOCYTIC
	TRANSCRIPTION FACTOR) (B1-BINDING
	FACTOR) (HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
72	ORPHAN NUCLEAR RECEPTOR NR5A2	TTTTATGGAGGTGTTTT
	(ALPHA-1-FETOPROTEIN TRANSCRIPTION	(SEQ ID NO: 2005)
	FACTOR) (HEPATOCYTIC
	TRANSCRIPTION FACTOR) (B1-BINDING
	FACTOR) (HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
73	ORPHAN NUCLEAR RECEPTOR NR5A2	AGGCGAATTTATCGGG
	(ALPHA-1-FETOPROTEIN TRANSCRIPTION	(SEQ ID NO: 2006)
	FACTOR) (HEPATOCYTIC
	TRANSCRIPTION FACTOR) (B1-BINDING
	FACTOR) (HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
74	ORPHAN NUCLEAR RECEPTOR NR5A2	GGTGAATTTATTGGGG
	(ALPHA-1-FETOPROTEIN TRANSCRIPTION	(SEQ ID NO: 2007)
	FACTOR) (HEPATOCYTIC
	TRANSCRIPTION FACTOR) (B1-BINDING
	FACTOR) (HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
75	ORPHAN NUCLEAR RECEPTOR NR5A2	TAGTCGAAGTAGGCGT
	(ALPHA-1-FETOPROTEIN TRANSCRIPTION	(SEQ ID NO: 2008)
	FACTOR) (HEPATOCYTIC
	TRANSCRIPTION FACTOR) (B1-BINDING
	FACTOR) (HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
76	ORPHAN NUCLEAR RECEPTOR NR5A2	TAGTTGAAGTAGGTGTT
	(ALPHA-1-FETOPROTEIN TRANSCRIPTION	(SEQ ID NO: 2009)
	FACTOR) (HEPATOCYTIC
	TRANSCRIPTION FACTOR) (B1-BINDING
	FACTOR) (HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
77	ORPHAN NUCLEAR RECEPTOR NR5A2	TTTTCGACGAAGTTTT
	(ALPHA-1-FETOPROTEIN TRANSCRIPTION	(SEQ ID NO: 2010)
	FACTOR) (HEPATOCYTIC
	TRANSCRIPTION FACTOR) (B1-BINDING
	FACTOR) (HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
78	ORPHAN NUCLEAR RECEPTOR NR5A2	TTTTGATGAAGTTTTGTT
	(ALPHA-1-1-tTOPROTEIN TRANSCRIPTION	(SEQ ID NO: 2011)
	FACTOR) (HEPATOCYTIC
	TRANSCRIPTION FACTOR) (B1-BINDING
	FACTOR) (HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
79	LIM DOMAIN KINASE 1 (EC 2.7.1.37)	TGTAGTCGGGAGGTTA
	(LIMK-1)	(SEQ ID NO: 2012)
	(SEQ ID NO: 12)
80	LIM DOMAIN KINASE 1 (EC 2.7.1.37)	TGTAGTTGGGAGGTTA
	(LIMK-1)	(SEQ ID NO: 2013)
	(SEQ ID NO: 12)
81	LIM DOMAIN KINASE 1 (EC 2.7.1.37)	GGATTATCGCGGGGGT
	(LIMK-1)	(SEQ ID NO: 2014)
	(SEQ ID NO: 12)
82	LIM DOMAIN KINASE 1 (EC 2.7.1.37)	GGATTATTGTGGGGGT
	(LIMK-1)	(SEQ ID NO: 2015)
	(SEQ ID NO: 12)
83	LIM DOMAIN KINASE 1 (EC 2.7.1.37)	GTCGGTAGTTTATCGGAT
	(LIMK-1)	(SEQ ID NO: 2016)
	(SEQ ID NO: 12)
84	LIM DOMAIN KINASE 1 (EC 2.7.1.37)	GTTGGTAGTTTATTGGAT
	(LIMK-1)	(SEQ ID NO: 2017)
	(SEQ ID NO: 12)
85	LIM DOMAIN KINASE 1 (EC 2.7.1.37)	TAGGAGACGTTACGTT
	(LIMK-1)	(SEQ ID NO: 2018)
	(SEQ ID NO: 12)
86	LIM DOMAIN KINASE 1 (EC 2.7.1.37)	AGATGTTATGTTAGGGT
	(LIMK-1)	(SEQ ID NO: 2019)
	(SEQ ID NO: 12)
87	KOX7	TAATTAGGCGCGAGGT
	(SEQ ID NO: 49)	(SEQ ID NO: 1220)
88	KOX7	TTAGGTGTGAGGTAGA
	(SEQ ID NO: 49)	(SEQ ID NO: 1221)
89	KOX7	TTAAAGTCGTGGGCGG
	(SEQ ID NO: 49)	(SEQ ID NO: 1222)
90	KOX7	TTAAAGTTGTGGGTGG
	(SEQ ID NO: 49)	(SEQ ID NO: 1223)
91	KOX7	GGTCGGGTTATAACGTA
	(SEQ ID NO: 49)	(SEQ ID NO: 1224)
92	KOX7	GGGTTGGGTTATAATGT
	(SEQ ID NO: 49)	(SEQ ID NO: 1225)
93	KOX7	TAAACGTTTTTCGGGA
	(SEQ ID NO: 49)	(SEQ ID NO: 1226)
94	KOX7	GGTAAATGTTTTTTGGG
	(SEQ ID NO: 49)	(SEQ ID NO: 1227)
95	BCL11B	TAGGTTTCGATTCGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 2020)
96	BCL11B	TTAGGTTTTGATTTGTTT
	(SEQ ID NO: 50)	(SEQ ID NO: 2021)
97	BCL11B	AAGTCGTCGGAGTTAG
	(SEQ ID NO: 50)	(SEQ ID NO: 2022)
98	BCL11B	GTGAAGTTGTTGGAGT
	(SEQ ID NO: 50)	(SEQ ID NO: 2023)
99	BCL11B	TTGAGGCGTTACGGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 2024)
100	BCL11B	TTGAGGTGTTATGGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 2025)
101	BCL11B	TTCGGGACGAAAATAA
	(SEQ ID NO: 50)	(SEQ ID NO: 1228)
102	BCL11B	AAGATTTTTGGATGAA
	(SEQ ID NO: 50)	(SEQ ID NO: 1229)
103	BCL11B	GTTTTCGTTTACGGAT
	(SEQ ID NO: 50)	(SEQ ID NO: 1230)
104	BCL11B	TGTTTTTGTTTATGGATT
	(SEQ ID NO: 50)	(SEQ ID NO: 1231)
105	SEQ ID NO: 51	TAAATTTCGGACGAGT
	(SEQ ID NO: 51)	(SEQ ID NO: 1232)
106	SEQ ID NO: 51	TTTAAATTTTGGATGAGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1233)
107	SEQ ID NO: 51	TTTACGGAGTTTCGGT
	(SEQ ID NO: 51)	(SEQ ID NO: 1234)
108	SEQ ID NO: 51	TTTTATGGAGTTTTGGT
	(SEQ ID NO: 51)	(SEQ ID NO: 1235)
109	SEQ ID NO: 51	GTCGGGGTCGATTCGA
	(SEQ ID NO: 51)	(SEQ ID NO: 1868)
110	SEQ ID NO: 51	GTTGGGGTTGATTTGAT
	(SEQ ID NO: 51)	(SEQ ID NO: 1869)
111	SEQ ID NO: 51	AGGATTCGTTTGCGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1870)
112	SEQ ID NO: 51	AAGGATTTGTTTGTGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1871)
113	SEQ ID NO: 51	TAGACGTTAGAGAACGT
	(SEQ ID NO: 51)	(SEQ ID NO: 1236)
114	SEQ ID NO: 51	AGATGTTAGAGAATGTTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1237)
115	MGC34831	ATTAGCGTTTGGCGTT
	(SEQ ID NO: 52)	(SEQ ID NO: 1872)
116	MGC34831	AATTAGTGTTTGGTGTT
	(SEQ ID NO: 52)	(SEQ ID NO: 1873)
117	MGC34831	GTTTAGCGACGGTCGT
	(SEQ ID NO: 52)	(SEQ ID NO: 1874)
118	MGC34831	TGTTTAGTGATGGTTGT
	(SEQ ID NO: 52)	(SEQ ID NO: 1875)
119	MGC34831	GTCGGACGGATTTATA
	(SEQ ID NO: 52)	(SEQ ID NO: 2210)
120	MGC34831	TGGTTGGATGGATTTAT
	(SEQ ID NO: 52)	(SEQ ID NO: 2211)
121	MGC34831	TTCGTTTTTCGGGATA
	(SEQ ID NO: 52)	(SEQ ID NO: 1238)
122	MGC34831	TTTGTTTTTTGGGATATG
	(SEQ ID NO: 52)	(SEQ ID NO: 1239)
123	COL5A1	AGGGATAGCGTTTTTT
	(SEQ ID NO: 53)	(SEQ ID NO: 1240)
124	COL5A1	AGGGATAGTGTTTTTTG
	(SEQ ID NO: 53)	(SEQ ID NO: 1241)
125	COL5A1	TAAGTGTTCGGGGGTA
	(SEQ ID NO: 53)	(SEQ ID NO: 1242)
126	COL5A1	TAAGTGTTTGGGGGTA
	(SEQ ID NO: 53)	(SEQ ID NO: 1243)
127	COL5A1	TACGAGGCGGGTAAAT
	(SEQ ID NO: 53)	(SEQ ID NO: 1244)
128	COL5A1	GTTTATGAGGTGGGTA
	(SEQ ID NO: 53)	(SEQ ID NO: 1245)
129	COL5A1	TATAGGCGTTTAGTTTG
	(SEQ ID NO: 53)	(SEQ ID NO: 1246)
130	COL5A1	ATTATAGGTGTTTAGTTTG
	(SEQ ID NO: 53)	(SEQ ID NO: 1247)
131	COL5A1	TTAAATCGGGTAGGGT
	(SEQ ID NO: 53)	(SEQ ID NO: 1248)
132	COL5A1	TTTAAATTGGGTAGGGT
	(SEQ ID NO: 53)	(SEQ ID NO: 1249)
133	SEQ ID NO: 54	TGTTATCGCGTAGGTT
	(SEQ ID NO: 54)	(SEQ ID NO: 1250)
134	SEQ ID NO: 54	GTGTTATTGTGTAGGTT
	(SEQ ID NO: 54)	(SEQ ID NO: 1251)
135	SEQ ID NO: 54	AGCGATGTATTCGTTT
	(SEQ ID NO: 54)	(SEQ ID NO: 1252)
136	SEQ ID NO: 54	GAGAGTGATGTATTTGT
	(SEQ ID NO: 54)	(SEQ ID NO: 1253)
137	SEQ ID NO: 54	TGTGTAGCGGCGATTA
	(SEQ ID NO: 54)	(SEQ ID NO: 1876)
138	SEQ ID NO: 54	GTGTGTAGTGGTGATT
	(SEQ ID NO: 54)	(SEQ ID NO: 1877)
139	SEQ ID NO: 54	ATTAGCGTTTGGTCGG
	(SEQ ID NO: 54)	(SEQ ID NO: 1878)
140	SEQ ID NO: 54	ATTAGTGTTTGGTTGGG
	(SEQ ID NO: 54)	(SEQ ID NO: 1879)
141	SEQ ID NO: 54	GACGGGGCGAGTTAGT
	(SEQ ID NO: 54)	(SEQ ID NO: 1254)
142	SEQ ID NO: 54	GATGGGGTGAGTTAGT
	(SEQ ID NO: 54)	(SEQ ID NO: 1255)
143	PDLIM1	GATTCGCGGGGATAGA
	(SEQ ID NO: 55)	(SEQ ID NO: 1256)
144	PDLIM1	GATTTGTGGGGATAGA
	(SEQ ID NO: 55)	(SEQ ID NO: 1257)
145	PDLIM1	TAATCGCGAGGGTTAG
	(SEQ ID NO: 55)	(SEQ ID NO: 1258)
146	PDLIM1	GGTAATTGTGAGGGTT
	(SEQ ID NO: 55)	(SEQ ID NO: 1259)
147	PDLIM1	TAGGTCGCGTAGTCGT
	(SEQ ID NO: 55)	(SEQ ID NO: 1880)
148	PDLIM1	TTAGGTTGTGTAGTTGT
	(SEQ ID NO: 55)	(SEQ ID NO: 1881)
149	PDLIM1	GAGTTTCGTCGAGAGA
	(SEQ ID NO: 55)	(SEQ ID NO: 1260)
150	PDLIM1	GGAGTTTTGTTGAGAGA
	(SEQ ID NO: 55)	(SEQ ID NO: 1261)
151	PDLIM1	AGAGCGCGAGTTAGAT
	(SEQ ID NO: 55)	(SEQ ID NO: 1262)
152	PDLIM1	AGAGAGTGTGAGTTAGA
	(SEQ ID NO: 55)	(SEQ ID NO: 1263)
153	MSF	GTTTCGAAATTGGCGT
	(SEQ ID NO: 13)	(SEQ ID NO: 2026)
154	MSF	TTTGAAATTGGTGTGG
	(SEQ ID NO: 13)	(SEQ ID NO: 2027)
155	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 2028)
156	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 2029)
157	MSF	TTACGGTTCGATTTTG
	(SEQ ID NO: 13)	(SEQ ID NO: 2030)
158	MSF	TATGGTTTGATTTTGGG
	(SEQ ID NO: 13)	(SEQ ID NO: 2031)
159	MSF	TTCGTACGTAGGTTTT
	(SEQ ID NO: 13)	(SEQ ID NO: 1264)
160	MSF	TTTGTTTGTATGTAGGTT
	(SEQ ID NO: 13)	(SEQ ID NO: 1265)
161	MSF	TAGGAAAGCGTACGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1266)
162	MSF	AGGAAAGTGTATGTATTT
	(SEQ ID NO: 13)	(SEQ ID NO: 1267)
163	SEQ ID NO: 14	TAAGGCGTTTTCGATA
	(SEQ ID NO: 14)	(SEQ ID NO: 2032)
164	SEQ ID NO: 14	GTAAGGTGTTTTTGATAT
	(SEQ ID NO: 14)	(SEQ ID NO: 2033)
165	SEQ ID NO: 14	TGGGTGTACGCGTGAA
	(SEQ ID NO: 14)	(SEQ ID NO: 2034)
166	SEQ ID NO: 14	TGTATGTGTGAAGGGG
	(SEQ ID NO: 14)	(SEQ ID NO: 2035)
167	SEQ ID NO: 14	AAATACGTATTTTCGGT
	(SEQ ID NO: 14)	(SEQ ID NO: 1268)
168	SEQ ID NO: 14	ATATGTATTTTTGGTAGTT
	(SEQ ID NO: 14)	(SEQ ID NO: 1269)
169	SEQ ID NO: 15	AATCGTGCGGTTGATA
	(SEQ ID NO: 15)	(SEQ ID NO: 1882)
170	SEQ ID NO: 15	TGTAGAATTGTGTGGT
	(SEQ ID NO: 15)	(SEQ ID NO: 1883)
171	SEQ ID NO: 15	TTGCGTAGAAAATTCGAG
	(SEQ ID NO: 15)	(SEQ ID NO: 1884)
172	SEQ ID NO: 15	TTGTGTAGAAAATTTGAG
	(SEQ ID NO: 15)	(SEQ ID NO: 1885)
173	SEQ ID NO: 15	AAAATTCGAGGTCGGG
	(SEQ ID NO: 15)	(SEQ ID NO: 1886)
174	SEQ ID NO: 15	AAAATTTGAGGTTGGG
	(SEQ ID NO: 15)	(SEQ ID NO: 1887)
175	SEQ ID NO: 15	AATAGGCGATGTACGG
	(SEQ ID NO: 15)	(SEQ ID NO: 2214)
176	SEQ ID NO: 15	TAGGTGATGTATGGGT
	(SEQ ID NO: 15)	(SEQ ID NO: 2215)
177	SEQ ID NO: 15	TAATCGAGTTTAGCGG
	(SEQ ID NO: 15)	(SEQ ID NO: 2216)
178	SEQ ID NO: 15	TTAATTGAGTTTAGTGGT
	(SEQ ID NO: 15)	(SEQ ID NO: 2217)
179	SEQ ID NO: 16	ATCGTTGGTCGGATTT
	(SEQ ID NO: 16)	(SEQ ID NO: 2036)
180	SEQ ID NO: 16	TAGGATTGTTGGTTGGA
	(SEQ ID NO: 16)	(SEQ ID NO: 2037)
181	SEQ ID NO: 16	AGGAGTTTTCGTGTCGT
	(SEQ ID NO: 16)	(SEQ ID NO: 2038)
182	SEQ ID NO: 16	AGGAGTTTTTGTGTTGT
	(SEQ ID NO: 16)	(SEQ ID NO: 2039)
183	SEQ ID NO: 16	TTACGGATAGGGCGAT
	(SEQ ID NO: 16)	(SEQ ID NO: 2040)
184	SEQ ID NO: 16	TATGGATAGGGTGATTT
	(SEQ ID NO: 16)	(SEQ ID NO: 2041)
185	SEQ ID NO: 16	AGGCGTTGTCGGTGAT
	(SEQ ID NO: 16)	(SEQ ID NO: 2042)
186	SEQ ID NO: 16	AGGTGTTGTTGGTGATA
	(SEQ ID NO: 16)	(SEQ ID NO: 2043)
187	SEQ ID NO: 16	AAGTAGATCGGGACGA
	(SEQ ID NO: 16)	(SEQ ID NO: 1270)
188	SEQ ID NO: 16	TAGATTGGGATGAGGA
	(SEQ ID NO: 16)	(SEQ ID NO: 1271)
189	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 2044)
190	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 2045)
191	SEQ ID NO: 17	ATTTAGTCGTGCGTTT
	(SEQ ID NO: 17)	(SEQ ID NO: 2046)
192	SEQ ID NO: 17	TGATTTAGTTGTGTGTT
	(SEQ ID NO: 17)	(SEQ ID NO: 2047)
193	SEQ ID NO: 17	GGTGATTTCGACGGTT
	(SEQ ID NO: 17)	(SEQ ID NO: 1272)
194	SEQ ID NO: 17	AGGTGATTTTGATGGTT
	(SEQ ID NO: 17)	(SEQ ID NO: 1273)
195	SEQ ID NO: 17	AGTAGCGTAATTTCGA
	(SEQ ID NO: 17)	(SEQ ID NO: 1274)
196	SEQ ID NO: 17	AGTGTAATTTTGAGGTG
	SEQ ID NO: 17)	(SEQ ID NO: 1275)
197	SEQ ID NO: 17	TATGGCGCGTATGTAT
	(SEQ ID NO: 17)	(SEQ ID NO: 1276)
198	SEQ ID NO: 17	GATTATGGTGTGTATGT
	(SEQ ID NO: 17)	(SEQ ID NO: 1277)
199	SEQ ID NO: 18	TTTACGCGGGGTTTTA
	(SEQ ID NO: 18)	(SEQ ID NO: 2048)
200	SEQ ID NO: 18	TTTATGTGGGGTTTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2049)
201	SEQ ID NO: 18	TTACGTCGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2050)
202	SEQ ID NO: 18	TTTTATGTTGTTATTAGGT
	(SEQ NO: 18)	(SEQ ID NO: 2051)
203	SEQ ID NO: 18	TATTTGGACGTCGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2052)
204	SEQ ID NO: 18	TATTTGGATGTTGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2053)
205	SEQ ID NO: 18	GAGGCGTATTAGGTCGG
	(SEQ ID NO: 18)	(SEQ ID NO: 2054)
206	SEQ ID NO: 18	AGGTGTATTAGGTTGGG
	(SEQ ID NO: 18)	(SEQ ID NO: 2055)
207	SEQ ID NO: 18	AAAGCGGAGTCGTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2056)
208	SEQ ID NO: 18	AGTGGAGTTGTTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2057)
209	SEQ ID NO: 19	AGGTTTTCGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2058)
210	SEQ ID NO: 19	TAGGTTTTTGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2059)
211	SEQ ID NO: 19	TTTGATATCGAGGGAG
	(SEQ ID NO: 19)	(SEQ ID NO: 2198)
212	SEQ ID NO: 19	TTTGATATTGAGGGAGG
	(SEQ ID NO: 19)	(SEQ ID NO: 2199)
213	SEQ ID NO: 19	GGTGTACGGAGGAAAG
	(SEQ ID NO: 19)	(SEQ ID NO: 2200)
214	SEQ ID NO: 19	GGTGTATGGAGGAAAG
	(SEQ ID NO: 19)	(SEQ ID NO: 2201)
215	SEQ ID NO: 19	TGAGATTCGTTTTTTAAA
	(SEQ ID NO: 19)	(SEQ ID NO: 2060)
216	SEQ ID NO: 19	GGTGAGATTTGTTTTTTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2061)
217	PRDM6	AGTTTTAAGCGTTTGGT
	(SEQ ID NO: 20)	(SEQ ID NO: 2062)
218	PRDM6	AGTTTTAAGTGTTTGGT
	(SEQ ID NO: 20)	(SEQ ID NO: 2063)
219	PRDM6	GAAGTTCGGATTTCGG
	(SEQ ID NO: 20)	(SEQ ID NO: 2064)
220	PRDM6	GGAAGTTTGGATTTTGG
	(SEQ ID NO: 20)	(SEQ ID NO: 2065)
221	PRDM6	TTGTCGGGTTACGGGA
	(SEQ ID NO: 20)	(SEQ ID NO: 2066)
222	PRDM6	GTTGGGTTATGGGAGA
	(SEQ ID NO: 20)	(SEQ ID NO: 2067)
223	PRDM6	TTCGTAGAATTGTCGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2068)
224	PRDM6	TTTGTAGAATTGTTGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2069)
225	RAP2B	AGATGTTTCGATTTGTT
	(SEQ ID NO: 21)	(SEQ ID NO: 1278)
226	RAP2B	GAGATGTTTTGATTTGTT
	(SEQ ID NO: 21)	(SEQ ID NO: 1279)
227	RAP2B	GGGTAATCGTTAGATTT
	(SEQ ID NO: 21)	(SEQ ID NO: 1280)
228	RAP2B	GGTAATTGTTAGATTTGG
	(SEQ ID NO: 21)	(SEQ ID NO: 1281)
229	RAP2B	GGTCGGGTAATCGTTA
	(SEQ ID NO: 21)	(SEQ ID NO: 2070)
230	RAP2B	GTTGGGTAATTGTTAGA
	(SEQ ID NO: 21)	(SEQ ID NO: 2071)
231	RAP2B	AGGAAGCGTTTTCGTT
	(SEQ ID NO: 21)	(SEQ ID NO: 2072)
232	RAP2B	AGAGGAAGTGTTTTTGT
	(SEQ ID NO: 21)	(SEQ ID NO: 2073)
233	NR2E1	AATGTAGCGGCGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2074)
234	NR2E1	TAAATGTAGTGGTGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2075)
235	NR2E1	GTCGTTATCGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2076)
236	NR2E1	GTTGTTATTGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2077)
237	NR2E1	GACGTAAGTTTCGGGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2078)
238	NR2E1	GGATGTAAGTTTTGGG
	(SEQ ID NO: 22)	(SEQ ID NO: 2079)
239	NR2E1	TTTTTAGTCGCGAGAA
	(SEQ ID NO: 22)	(SEQ ID NO: 2080)
240	NR2E1	TTTTTAGTTGTGAGAAGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2081)
241	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2082)
242	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2083)
243	NR2E1	AGGCGAGTCGGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2084)
244	NR2E1	AGGTGAGTTGGAGTTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2085)
245	NR2E1	TAAGTCGAGCGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2086)
246	NR2E1	TAGTAAGTTGAGTGAGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2087)
247	NR2E1	AGGGACGCGAAAATTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2088)
248	NR2E1	GGAGGGATGTGAAAAT
	(SEQ ID NO: 22)	(SEQID NO: 2089)
249	PCDH7	ATCGTAGTCGGTTTTA
	(SEQ ID NO: 23)	(SEQ ID NO: 2090)
250	PCDH7	GATTATTGTAGTTGGTTT
	(SEQ ID NO: 23)	(SEQ ID NO: 2091)
251	PCDH7	AAAGTGTAGCGTTATTT
	(SEQ ID NO: 23)	(SEQ ID NO: 1282)
252	PCDH7	AAAGTGTAGTGTTATTTAT
	(SEQ ID NO: 23)	(SEQ ID NO: 1283)
253	PCDH7	TTGGAAATTTCGATATTAT
	(SEQ ID NO: 23)	(SEQ ID NO: 1284)
254	PCDH7	TGGAAATTTTGATATTATTT
	(SEQ ID NO: 23)	(SEQ ID NO: 1285)
255	DKK3	ATTCGTTTTAGTTCGAG
	(SEQ ID NO: 24)	(SEQ ID NO: 1888)
256	DKK3	ATTTGTTTTAGTTTGAGT
	(SEQ ID NO: 24)	(SEQ ID NO: 1889)
257	DKK3	TTCGATCGTTTTAGGA
	(SEQ ID NO: 24)	(SEQ ID NO: 1890)
258	DKK3	AGTTTTGATTGTTTTAGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1891)
259	DKK3	TTTCGGAACGCGATTA
	(SEQ ID NO: 24)	(SEQ ID NO: 1286)
260	DKK3	GTGTTTTGGAATGTGA
	(SEQ ID NO: 24)	(SEQ ID NO: 1287)
261	DKK3	ATTCGTTCGGAGACGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1892)
262	DKK3	TTTGTTTGGAGATGGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1893)
263	DKK3	GAAAAGACGCGATTTT
	(SEQ ID NO: 24)	(SEQ ID NO: 1894)
264	DKK3	GAAAAGATGTGATTTTATT
	(SEQ ID NO: 24)	(SEQ ID NO: 1895)
265	RTTN	AATGGTCGTGTTACGT
	(SEQ ID NO: 25)	SEQ ID NO: 1288)
266	RTTN	ATGGTTGTGTTATGTTT
	(SEQ ID NO: 25)	(SEQ ID NO: 1289)
267	RTTN	TAGATTGACGGGACGA
	(SEQ ID NO: 25)	(SEQ ID NO: 2228)
268	RTTN	TAGATTGATGGGATGAG
	(SEQ ID NO: 25)	(SEQ ID NO: 2229)
269	RTTN	TAGTGGCGCGGTAGTT
	(SEQ ID NO: 25)	(SEQ ID NO: 2092)
270	RTTN	TAGTGGTGTGGTAGTTT
	(SEQ ID NO: 25)	(SEQ ID NO: 2093)
271	RTTN	TAGGACGTGTTTTCGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2094)
272	RTTN	AGGATGTGTTTTTGGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2095)
273	RTTN	TTGCGGAATTTATCGTT
	(SEQ ID NO: 25)	(SEQ ID NO: 1290)
274	RTTN	TGTGGAATTTATTGTTTT
	(SEQ ID NO: 25)	(SEQ ID NO: 1291)
275	SNAP25	TATTTCGAGTTAGAGTTACGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2096)
276	SNAP25	TATTTTGAGTTAGAGTTATGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2097)
277	SNAP25	ATACGGAATATCGTATTT
	(SEQ ID NO: 33)	(SEQ ID NO: 2098)
278	SNAP25	GTGTATATATGGAATATTGT
	(SEQ ID NO: 33)	(SEQ ID NO: 2099)
279	SNAP25	GTTATTATTCGGTACGT
	(SEQ ID NO: 33)	(SEQ ID NO: 2202)
280	SNAP25	AGTTATTATTTGGTATGTAT
	(SEQ ID NO: 33)	(SEQ ID NO: 2203)
281	SEQ ID NO: 26	TTAAGTATCGAGGCGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2100)
282	SEQ ID NO: 26	TTTTAAGTATTGAGGTGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2101)
283	SEQ ID NO: 26	AATTTTGGTCGTTTAGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2102)
284	SEQ ID NO: 26	AAATTTTGGTTGTTTAGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2103)
285	SEQ ID NO: 26	TTCGTATTGACGTTAAT
	(SEQ ID NO: 26)	(SEQ ID NO: 2104)
286	SEQ ID NO: 26	TTTGTATTGATGTTAATAGA
	(SEQ ID NO: 26)	(SEQ ID NO: 2105)
287	GIRK2	AGTTGTTCGTAGGCGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2106)
288	GIRK2	AGTTGTTTGTAGGTGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2107)
289	GIRK2	TTATTTCGTTCGTAGTT
	(SEQ ID NO: 27)	(SEQ ID NO: 2108)
290	GIRK2	TTTGTTTGTAGTTAGGTA
	(SEQ ID NO: 27)	(SEQ ID NO: 2109)
291	GIRK2	TTGAAATTCGTACGGG
	(SEQ ID NO: 27)	(SEQ ID NO: 1292)
292	GIRK2	AAATTTGTATGGGGGG
	(SEQ ID NO: 27)	(SEQ ID NO: 1293)
293	GIRK2	TTAGTCGAAAGGCGAG
	(SEQ ID NO: 27)	(SEQ ID NO: 2110)
294	GIRK2	TAGTTGAAAGGTGAGG
	(SEQ ID NO: 27)	(SEQ ID NO: 2111)
295	SEQ ID NO: 28	GAGTAACGCGTGTGAT
	(SEQ ID NO: 28)	(SEQ ID NO: 1294)
296	SEQ ID NO: 28	TATGAGTAATGTGTGTG
	(SEQ ID NO: 28)	(SEQ ID NO: 1295)
297	SEQ ID NO: 28	TTTTCGGTAAGTTTACGG
	(SEQ ID NO: 28)	(SEQ ID NO: 1296)
298	SEQ ID NO: 28	TTTTTGGTAAGTTTATGG
	(SEQ ID NO: 28)	(SEQ ID NO: 1297)
299	SEQ ID NO: 28	ATAAGACGGAGTTCGT
	(SEQ ID NO: 28)	(SEQ ID NO: 1298)
300	SEQ ID NO: 28	AAGATGGAGTTTGTTTG
	(SEQ ID NO: 28)	(SEQ ID NO: 1299)
301	SEQ ID NO: 28	ATTAGGCGAGTTTCGT
	(SEQ ID NO: 28)	(SEQ ID NO: 2112)
302	SEQ ID NO: 28	TTAGGTGAGTTTTGTTT
	(SEQ ID NO: 28)	(SEQ ID NO: 2113)
303	SEQ ID NO: 28	TATCGACGTTTTTGGT
	(SEQ ID NO: 28)	(SEQ ID NO: 1896)
304	SEQ ID NO: 28	TATTGATGTTTTTGGTTT
	(SEQ ID NO: 28)	(SEQ ID NO: 1897)
305	SEQ ID NO: 28	ATTCGGTGAAGCGATT
	(SEQ ID NO: 28)	(SEQ ID NO: 1300)
306	SEQ ID NO: 28	ATTTGGTGAAGTGATTT
	(SEQ ID NO: 28)	(SEQ ID NO: 1301)
307	SEQ ID NO: 28	GTTCGTAGCGGTAGGT
	(SEQ ID NO: 28)	(SEQ ID NO: 1302)
308	SEQ ID NO: 28	TTTGTAGTGGTAGGTGA
	(SEQ ID NO: 28)	(SEQ ID NO: 1303)
309	SEQ ID NO: 28	TGGACGGAGACGAAAG
	(SEQ ID NO: 28)	(SEQ ID NO: 1304)
310	SEQ ID NO: 28	GGATGGAGATGAAAGGA
	(SEQ ID NO: 28)	(SEQ ID NO: 1305)
311	SEQ ID NO: 29	TTGATGCGGAGTTCGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1898)
312	SEQ ID NO: 29	TTGATGTGGAGTTTGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1899)
313	SEQ ID NO: 29	TTCGAAGCGTGTATTA
	(SEQ ID NO: 29)	(SEQ ID NO: 2188)
314	SEQ ID NO: 29	GGGTTTGAAGTGTGTA
	(SEQ ID NO: 29)	(SEQ ID NO: 2189)
315	SEQ ID NO: 29	TTTTCGCGTTTGCGAA
	(SEQ ID NO: 29)	(SEQ ID NO: 2190)
316	SEQ ID NO: 29	TTTGTGTTTGTGAAAGG
	(SEQ ID NO: 29)	(SEQ ID NO: 2191)
317	SEQ ID NO: 29	TAGGAACGGTAGGCGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1900)
318	SEQ ID NO: 29	TAGGAATGGTAGGTGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1901)
319	SEQ ID NO: 29	GTCGGAGGCOTTTGAG
	(SEQ ID NO: 29)	(SEQ ID NO: 1902)
320	SEQ ID NO: 29	GTTGGAGGTGTTTGAGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1903)
321	ARL7	TAGATTTCGTAGTTTTTTA
	(SEQ ID NO: 30)	(SEQ ID NO: 1904)
322	ARL7	TAGATTTTGTAGTTTTTTAA
	(SEQ ID NO: 30)	(SEQ ID NO: 1905)
323	ARL7	TGGGTACGTTTACGGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1906)
324	ARL7	TGGGTATGTTTATGGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1907)
325	ARL7	GAAGAAATCGTTTTTGT
	SSEQ ID NO: 30)	(SEQ ID NO: 1908)
326	ARL7	GAAGAAATTGTTTTTGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1909)
327	ARL7	TAGTAGGATCGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1910)
328	ARL7	ATAGTAGGATTGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1911)
329	SEQ ID NO: 31	TTTACGTAGGGCGATT
	(SEQ ID NO: 31)	(SEQ ID NO: 2114)
330	SEQ ID NO: 31	ATTTTTATGTAGGGTGAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2115)
331	SEQ ID NO: 31	AACGTTGCGTTGGGTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1912)
332	SEQ ID NO: 31	AATGTTGTGTTGGGTAA
	(SEQ ID NO: 31)	(SEQ ID NO: 1913)
333	SEQ ID NO: 31	TAGCGTTTCGTGGTTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1914)
334	SEQ ID NO: 31	GTAGTGTTTTGTGGTTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1915)
335	SEQ ID NO: 31	GATAGGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2116)
336	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2117)
337	SEQ ID NO: 31	TTCGGGCGTTTTATAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2118)
338	SEQ ID NO: 31	GGTTTGGGTGTTTTATA
	(SEQ ID NO: 31)	(SEQ ID NO: 2119)
339	THH	TTCGGAAGAAAAGCGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1916)
340	THH	TTTGGAAGAAAAGTGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1917)
341	THH	GTTCGTTGGCGTAAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1918)
342	THH	GGTTTGTTGGTGTAAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1919)
343	THH	AGTACGTGTATATCGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1306)
344	THH	TAGTATGTGTATATTGGAA
	(SEQ ID NO: 32)	(SEQ ID NO: 1307)
345	THH	TATTCGGAAGTGATCGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1920)
346	THH	TATTTGGAAGTGATTGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1921)
347	HOXB13	GTCGTTATTATTTCGAGG
	(SEQ ID NO: 34)	(SEQ ID NO: 2120)
348	HOXB13	GTTGTTATTATTTTGAGGA
	(SEQ ID NO: 34)	(SEQ ID NO: 2121)
349	HOXB13	TTCGTAGAATCGAAGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2220)
350	HOXB13	TAATTTGTAGAATTGAAGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2221)
351	HOXB13	TTACGATTGAGCGTAT
	(SEQ ID NO: 34)	(SEQ ID NO: 2222)
352	HOXB13	TATGATTGAGTGTATAGG
	(SEQ ID NO: 34)	(SEQ ID NO: 2223)
353	HOXB13	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2122)
354	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2123)
355	HOXB13	TTGGTCGCGTAGTAAA
	(SEQ ID NO: 34)	(SEQ ID NO: 2124)
356	HOXB13	TGGTTGTGTAGTAAAGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2125)
357	(SEQ ID NO: 35)	GGAGGTGCGAATTTAA
		(SEQ ID NO: 2126)
358	(SEQ ID NO: 35)	GGGAGGTGTGAATTTA
		(SEQ ID NO: 2127)
359	(SEQ ID NO: 35)	AAATAGTCGTTTGGGA
		(SEQ ID NO: 2128)
360	(SEQ ID NO: 35)	AAATAGTTGTTTGGGAG
		(SEQ ID NO: 2129)
361	(SEQ ID NO: 35)	AGAAAATATACGAGATTTAT
		(SEQ ID NO: 2130)
362	(SEQ ID NO: 35)	AGAAAATATATGAGATTTATT
		(SEQ ID NO: 2131)
363	(SEQ ID NO: 35)	TAAAGACGGGAAGAGA
		(SEQ ID NO: 2132)
364	(SEQ ID NO: 35)	ATAAAGATGGGAAGAGA
		(SEQ ID NO: 2133)
365	(SEQ ID NO: 36)	TTCGTTGGAGATCGTAA
		(SEQ ID NO: 2192)
366	(SEQ ID NO: 36)	GTTTGTTGGAGATTGTA
		(SEQ ID NO: 2193)
367	(SEQ ID NO: 36)	TTATTTGCGTTTCGAA
		(SEQ ID NO: 2218)
368	(SEQ ID NO: 36)	AATTATTTGTGTTTTGAAT
		(SEQ ID NO: 2219)
369	(SEQ ID NO: 36)	TTGTCGTGATAGCGTT
		(SEQ ID NO: 1308)
370	(SEQ ID NO: 36)	TTTGTTGTGATAGTGTT
		(SEQ ID NO: 1309)
371	(SEQ ID NO: 36)	GGACGTTGCGATTGTA
		(SEQ ID NO: 2194)
372	(SEQ ID NO: 36)	GATGTTGTGATTGTAGT
		(SEQ ID NO: 2195)
373	MGC10561	ATATTTAGCGTAGTTATTT
	(SEQ ID NO: 37)	(SEQ ID NO: 2204)
374	MGC10561	TAGTATATTTAGTGTAGTTAT
	(SEQ ID NO: 37)	(SEQ ID NO: 2205)
375	MGC10561	TTTTTTACGTTAAGGGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2134)
376	MGC10561	TTTTTATGTTAAGGGGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2135)
377	MGC10561	TTTGTTTTTCGAGTAGA
	(SEQ ID NO: 37)	(SEQ ID NO: 2136)
378	MGC10561	TGTTTTTTGAGTAGAGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2137)
379	LMX1A	GTCGGGTTTTTCGGAA
	(SEQ ID NO: 38)	(SEQ ID NO: 2138)
380	LMX1A	GTTGGGTTTTTTGGAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2139)
381	LMX1A	GTCGAGATTTTATCGAAA
	(SEQ ID NO: 38)	(SEQ ID NO: 2140)
382	LMX1A	GTTGAGATTTTATTGAAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2141)
383	LMX1A	TTCGTTTTTAACGTGG
	(SEQ ID NO: 38)	(SEQ ID NO: 2224)
384	LMX1A	TTTGTTTTTAATGTGGTT
	(SEQ ID NO: 38)	(SEQ ID NO: 2225)
385	LMX1A	AGTATTCGGGCGGGTA
	(SEQ ID NO: 38)	(SEQ ID NO: 2142)
386	LMX1A	GTAGTATTTGGGTGGG
	(SEQ ID NO: 38)	(SEQ ID NO: 2143)
387	LMX1A	AACGAAATTACGTGTAT
	(SEQ ID NO: 38)	(SEQ ID NO: 2144)
388	LMX1A	TGAAATGAAATTATGTGTA
	(SEQ ID NO: 38)	(SEQ ID NO: 2145)
389	SEMP3	TATTCGGATCGGGTTT
	(SEQ ID NO: 39)	(SEQ ID NO: 1922)
390	SENP3	TTTATTTGGATTGGGTT
	(SEQ ID NO: 39)	(SEQ ID NO: 1923)
391	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1924)
392	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1925)
393	SENP3	AGGACGTTTTTGATCGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1926)
394	SENP3	AGGATGTTTTTGATTGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1927)
395	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1928)
396	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1929)
397	GS1	GAAGCGACGTTTATTT
	(SEQ ID NO: 40)	(SEQ ID NO: 1310)
398	GS1	GGGAAGTGATGTTTATT
	(SEQ ID NO: 40)	(SEQ ID NO: 1311)
399	GS1	TGCGAGTTAGCGGTTA
	(SEQ ID NO: 40)	(SEQ ID NO: 2146)
400	GS1	TTGTGAGTTAGTGGTT
	(SEQ ID NO: 40)	(SEQ ID NO: 2147)
401	GS1	AATCGTTAGTTCGGTT
	(SEQ ID NO: 40)	(SEQ ID NO: 1312)
402	GS1	TGAATTGTTAGTTTGGT
	(SEQ ID NO: 40)	(SEQ ID NO: 1313)
403	GS1	TAGAGGTTCGAGCGTA
	(SEQ ID NO: 40)	(SEQ ID NO: 1314)
404	GS1	AGAGGTTTGAGTGTAG
	(SEQ ID NO: 40)	(SEQ ID NO: 1315)
405	GS1	AGTTTCGAGGTTTTCGG
	(SEQ ID NO: 40)	(SEQ ID NO: 2148)
406	GS1	AAGTTTTGAGGTTTTTGG
	(SEQ ID NO: 40)	(SEQ ID NO: 2149)
407	TTTF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2150)
408	TTTF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2151)
409	TTTF1	TTTTTGCGTAAACGTA
	(SEQ ID NO: 41)	(SEQ ID NO: 1316)
410	TTTF1	TTGTGTAAATGTAGGGT
	(SEQ ID NO: 41)	(SEQ ID NO: 1317)
411	TTTF1	GGTTCGTTTAAGTTCGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2152)
412	TTTF1	GGTTTGTTTAAGTTTGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2153)
413	TTTF1	TTAGGTCGCGTTTGTA
	(SEQ ID NO: 41)	(SEQ ID NO: 2154)
414	TTTF1	AGGTTGTGTTTGTAGA
	(SEQ ID NO: 41)	(SEQ ID NO: 2155)
415	TTTF1	TATTTCGTTTTCGTAATT
	(SEQ ID NO: 41)	(SEQ ID NO: 2156)
416	TTTF1	TTTGTTTTTGTAATTAGATT
	(SEQ ID NO: 41)	(SEQ ID NO: 2157)
417	SEQ ID NO: 42	AGGTCGAATAAAGCGT
	(SEQ ID NO: 42)	(SEQ ID NO: 2212)
418	SEQ ID NO: 42	GAGGTTGAATAAAGTGT
	(SEQ ID NO: 42)	(SEQ ID NO: 2213)
419	SEQ ID NO: 42	TTCGGAAGTTTAACGAGG
	(SEQ ID NO: 42)	(SEQ ID NO: 1318)
420	SEQ ID NO: 42	TTTGGAAGTTTAATGAGG
	(SEQ ID NO: 42)	(SEQ ID NO: 1319)
421	SEQ ID NO: 42	GAGTCGGGTTGCGATG
	(SEQ ID NO: 42)	(SEQ ID NO: 1930)
422	SEQ ID NO: 42	GGAGTTGGGTTGTGAT
	(SEQ ID NO: 42)	(SEQ ID NO: 1931)
423	SEQ ID NO: 42	ATGGGTTGCGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1932)
424	SEQ ID NO: 42	ATGGGTTGTGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1933)
425	DDX51	TAGGCGAGCGTTAGGT
	(SEQ ID NO: 43)	(SEQ ID NO: 2206)
426	DDX51	GGTGAGTGTTAGGTTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2207)
427	DDX51	AGATTTTCGGCGAGAT
	(SEQ ID NO: 43)	(SEQ ID NO: 2158)
428	DDX51	ATTTTTGGTGAGATAGG
	(SEQ ID NO: 43)	(SEQ ID NO: 2159)
429	DDX51	TACGTGTGGTTTTCGGTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2160)
430	DDX51	TATGTGTGGTTTTTGGTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2161)
431	DDX51	TGCGTTTATCGTTTTAG
	(SEQ ID NO: 43)	(SEQ ID NO: 1320)
432	DDX51	TGTGTTTATTGTTTTAGG
	(SEQ ID NO: 43)	(SEQ ID NO: 1321)
433	DDX51	AACGTGCGGGGTTTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2162)
434	DDX51	TGAATGTGTGGGGTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2163)
435	(SEQ ID NO: 117)	TAGCGGTTTTTTAGCGTA
		(SEQ ID NO: 1934)
436	(SEQ ID NO: 117)	AGTGGTTTTTTAGTGTAT
		(SEQ ID NO: 1935)
437	(SEQ ID NO: 117)	AGATGCGCGGGTAGAT
		(SEQ ID NO: 1936)
438	(SEQ ID NO: 117)	AGATGTGTGGGTAGAT
		(SEQ ID NO: 1937)
439	(SEQ ID NO: 117)	AGATAGTTCGTATTCGT
		(SEQ ID NO: 1938)
440	(SEQ ID NO: 117)	GTAGATAGTTTGTATTTGT
		(SEQ ID NO: 1939)
441	(SEQ ID NO: 117)	TTTGTTCGTAACGTTT
		(SEQ ID NO: 1940)
442	(SEQ ID NO: 117)	TGTTTGTAATGTTTAGAG
		(SEQ ID NO: 1941)
443	Q8NAN2	AGTTTCGCGAGGGGTT
	(SEQ ID NO: 44)	(SEQ ID NO: 1322)
444	Q8NAN2	AGAGTTTTGTGAGGGG
	(SEQ ID NO: 44)	(SEQ ID NO: 1323)
445	Q8NAN2	TTTTTACGTTAGAGGGA
	(SEQ ID NO: 44)	(SEQ ID NO: 1324)
446	Q8NAN2	TTTTTATGTTAGAGGGAG
	(SEQ ID NO: 44)	(SEQ ID NO: 1325)
447	SEQ ID NO: 45	AGCGAACGTTTATTTT
	(SEQ ID NO: 45)	(SEQ ID NO: 2164)
448	SEQ ID NO: 45	TAGGAGAGTGAATGTTT
	(SEQ ID NO: 45)	(SEQ ID NO: 2165)
449	SEQ ID NO:45	TAATGTCGATCGGATT
	(SEQ ID NO: 45)	(SEQ ID NO: 1326)
450	SEQ ID NO: 45	ATGTTGATTGGATTTGT
	(SEQ ID NO: 45)	(SEQ ID NO: 1327)
451	SEQ ID NO: 45	TGTAGTATCGGGGGAG
	(SEQ ID NO: 45)	(SEQ ID NO: 2208)
452	SEQ ID NO: 45	TGTAGTATTGGGGGAG
	(SEQ ID NO: 45)	(SEQ ID NO: 2209)
453	SEQ ID NO: 45	TTTTTTACGGGCGATA
	(SEQ ID NO: 45)	(SEQ ID NO: 1328)
454	SEQ ID NO: 45	TTTTATGGGTGATAGGT
	(SEQ ID NO: 45)	(SEQ ID NO: 1329)
455	SEQ ID NO: 46	GAGTCGGGTTATCGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2166)
456	SEQ ID NO: 46	GGAGTTGGGTTATTGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2167)
457	SEQ ID NO: 46	TTACGGATGTTTCGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2168)
458	SEQ ID NO: 46	TTTATGGATGTTTTGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2169)
459	SEQ ID NO: 46	TGACGTATTTTCGGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2170)
460	SEQ ID NO: 46	GGTGATGTATTTTTGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2171)
461	SEQ ID NO: 46	ATAGTCGGAATCGTTG
	(SEQ ID NO: 46)	(SEQ ID NO: 2172)
462	SEQ ID NO: 46	TAGTTGGAATTGTTGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2173)
463	O60279	AGTAAACGAATAAGAAGT
	(SEQ ID NO: 47)	(SEQ ID NO: 1942)
464	O60279	AAGTAAATGAATAAGAAGT
	(SEQ ID NO: 47)	(SEQ ID NO: 1943)
465	O60279	TACGTTTTTTCGGATTA
	(SEQ ID NO: 47)	(SEQ ID NO: 1944)
466	O60279	TATGTTTTTTTGGATTAAG
	(SEQ ID NO: 47)	(SEQ ID NO: 1945)
467	O60279	TAATTATCGGCGGTGT
	(SEQ ID NO: 47)	(SEQ ID NO: 1946)
468	O60279	ATTATTGGTGGTGTTTT
	(SEQ ID NO: 47)	(SEQ ID NO: 1947)
469	O60279	GGACGGCGGAAAATTA
	(SEQ ID NO: 47)	(SEQ ID NO: 1948)
470	O60279	AGGGATGGTGGAAAAT
	(SEQ ID NO: 47)	(SEQ ID NO: 1949)
471	SEQ ID NO: 48	TATTTGGCGATTCGGA
	(SEQ ID NO: 48)	(SEQ ID NO: 1950)
472	SEQ ID NO: 48	TGGTGATTTGGAGATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1951)
473	SEQ ID NO: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1952)
474	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1953)
475	SEQ ID NO: 48	AACGAATTTTTCGATATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1954)
476	SEQ ID NO: 48	TTTAATGAATTTTTTGATATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1955)
477	SEQ ID NO: 48	AAAATCGTATGCGTGT
	SEQ ID NO: 48)	(SEQ ID NO: 1956)
478	SEQ ID NO: 48	GAAAATTGTATGTGTGTG
	(SEQ ID NO: 48)	(SEQ ID NO: 1957)
479	SEQ ID NO: 9	AGGTATTTCGCGATAT
	(SEQ ID NO: 9)	(SEQ ID NO: 1330)
480	SEQ ID NO: 9	AGGTATTTTGTGATATTTT
	(SEQ ID NO: 91)	(SEQ ID NO: 1331)
481	SEQ ID NO: 9	GTTTTTCGATTTACGTT
	(SEQ ID NO: 9)	(SEQ ID NO: 1332)
482	SEQ ID NO: 9	TAGGTTTTTTGATTTATGT
	(SEQ ID NO: 9)	(SE1 ID NO: 1333)
483	SEQ ID NO: 9	TTACGGTTCGGTTATT
	(SEQ ID NO: 9)	(SEQ ID NO: 1334)
484	SEQ ID NO: 9	AGGTTTTATGGTTTGGT
	(SEQ ID NO: 9)	(SEQ ID NO: 1335)
485	SEQ ID NO: 9	GTTTCGCGTTTAGGGA
	(SEQ ID NO: 9)	(SEQ ID NO: 1958)
486	SEQ ID NO: 9	GTTTTGTGTTTAGGGAT
	(SEQ ID NO: 9)	(SEQ ID NO: 1959)
487	SEQ ID NO: 9	AGTGTTCGTCGTAGTT
	(SEQ ID NO: 9)	(SEQ ID NO: 1960)
488	SEQ ID NO: 9	TGAGTGTTTGTTGTAGT
	(SEQ ID NO: 9)	(SEQ ID NO: 1961)
489	SEQ ID NO: 2	ATTGGGTTTCGCGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2174)
490	SEQ ID NO: 2	ATTGGGTTTTGTGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2175)
491	SEQ ID NO: 2	TAGTAGTCGGCGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2176)
492	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2177)
493	SEQ ID NO: 2	TGTCGTACGTTATGTT
	(SEQ ID NO: 2)	(SEQ ID NO: 2226)
494	SEQ ID NO: 2	GGTGTTGTATGTTATGT
	(SEQ ID NO: 2)	(SEQ ID NO: 2227)
495	SEQ ID NO: 2	TTGATTGGCGGACGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1699)
496	SEQ ID NO: 2	TTGATTGGTGGATGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1700)
497	SEQ ID NO: 3	TTGCGTTAATTCGGTA
	(SEQ ID NO: 3)	(SEQ ID NO: 2178)
498	SEQ ID NO: 3	AATTTGTGTTAATTTGGT
	(SEQ ID NO: 3)	(SEQ ID NO: 2179)
499	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2180)
500	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2181)
501	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2182)
502	SEQ ID NO: 3	GGTTGAAGAGTTGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2183)
503	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2184)
504	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2185)
505	SEQ ID NO: 4	TTTTGTTCGCGTTGAA
	(SEQ ID NO: 4)	(SEQ ID NO: 1962)
506	SEQ ID NO: 4	TTGTTTGTGTTGAAGTA
	(SEQ ID NO: 4)	(SEQ ID NO: 1963)
507	SEQ ID NO: 4	GGGTCGCGAGGTAGTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1964)
508	SEQ ID NO: 4	TGGGTTGTGAGGTAGT
	(SEQ ID NO: 4)	(SEQ ID NO: 1965)
509	SEQ ID NO: 4	TTTGTGCGACGTTATT
	(SEQ ID NO: 4)	(SEQ ID NO: 1966)
510	SEQ ID NO: 4	GGTTTGTGTGATGTTAT
	(SEQ ID NO: 4)	(SEQ ID NO: 1967)
511	SEQ ID NO: 4	ATGGCGGTTTCGATTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1968)
512	SEQ ID NO: 4	GATGGTGGTTTTGATTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1969)
513	HS3ST2	GAATCGGAGAGGCGAG
	(SEQ ID NO: 113)	(SEQ ID NO: 1664)
514	HS3ST2	AATTGGAGAGGTGAGG
	(SEQ ID NO: 113)	(SEQ ID NO: 1665)
515	HS3ST2	GGGTAATCGTTTGGTA
	(SEQ ID NO: 113)	(SEQ ID NO: 1666)
516	HS3ST2	GGGTAATTGTTTGGTAT
	(SEQ ID NO: 113)	(SEQ ID NO: 1667)
517	PRDM2	TGTAGAGACGACGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1668)
518	PRDM2	ATTGTAGAGATGATGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1669)
519	PRDM2	AGAGCGCGGTAGTAGT
	(SEQ ID NO: 114)	(SEQ ID NO: 1670)
520	PRDM2	TGAGAGTGTGGTAGTA
	(SEQ ID NO: 114)	(SEQ ID NO: 1671)
521	PRDM2	TGTTCGCGATGTTTTA
	(SEQ ID NO: 114)	(SEQ ID NO: 1672)
522	PRDM2	TGTTTGTGATGTTTTAGT
	(SEQ ID NO: 114)	(SEQ ID NO: 1673)
523	PRDM2	AGTATATAAACGTAGATTTT
	(SEQ ID NO: 114)	(SEQ ID NO: 1674)
524	PRDM2	AAGTATATAAATGTAGATTTT
	(SEQ ID NO: 114)	(SEQ ID NO: 1675)
525	ALX4	AAGTCGATCGTTTTGT
	(SEQ ID NO: 64)	(SEQ ID NO: 1676)
526	ALX4	TGGAAGTTGATTGTTTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1677)
527	ALX4	ATATCGTTCGGGGGAA
	(SEQ ID NO: 64)	(SEQ ID NO: 1827)
528	ALX4	ATTGTTTGGGGGAATT
	(SEQ ID NO: 6)	(SEQ ID NO: 1336)
529	ALX4	TATTGCGAGGATTCGG
	(SEQ ID NO: 64)	(SEQ ID NO: 1678)
530	ALX4	ATTGTGAGGATTTGGT
	(SEQ ID NO: 64)	(SEQ ID NO: 1679)
531	ALX4	TTCGTAGCGTAGGGTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1680)
532	ALX4	TTTGTAGTGTAGGGTTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1681)
533	LEF1	TGAGATTTCGTTTATTGA
	(SEQ ID NO: 63)	(SEQ ID NO: 1337)
534	LEF1	ATTGAGATTTTGTTTATTG
	(SEQ ID NO: 63)	(SEQ ID NO: 1338)
535	LEF1	TTGTTTTTAACGAAATTAT
	(SEQ ID NO: 63)	(SEQ ID NO: 1339)
536	LEF1	TGTTTTTAATGAAATTATTTA
	(SEQ ID NO: 63)	(SEQ ID NO: 1340)
537	LEF1	TTGGAAGTCGAAGAGA
	(SEQ ID NO: 63)	(SEQ ID NO: 1341)
538	LEF1	TTTGGAAGTTGAAGAGA
	(SEQ ID NO: 63)	(SEQ ID NO: 1342)
539	LEF1	TGGATTTTTCGAGTAATT
	(SEQ ID NO: 63)	(SEQ ID NO: 1343)
540	LEF1	TTGGATTTTTTGAGTAATT
	(SEQ ID NO: 63)	(SEQ ID NO: 1344)
541	SCGB3A1	GATAGACGAGTGAGGA
	(SEQ ID NO: 115)	(SEQ ID NO: 1345)
542	SCBG3A1	GATAGATGAGTGACGAT
	(SEQ ID NO: 115)	(SEQ ID NO: 1346)
543	SCGB3A1	TATTGGCGTCGAGGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 1828)
544	SCGB3A1	TATTGGTGTTGAGGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 1829)
545	SCGB3A1	GGCGTAGAAGGCGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 1823)
546	SCGB3A1	GGTGTAGAAGGTGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 1824)
547	SCGB3A1	TAGTGTTCGACGTTGT
	(SEQ ID NO: 115)	(SEQ ID NO: 1468)
548	SCGB3A1	TAGTGTTTGATGTTGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 1469)
549	SASH1	TAGATTCGAGGTGCGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1470)
550	SASH1	TAGATTTGAGGTGTGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1471)
551	SASH1	ATTCGGTATTCGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1472)
552	SASH1	ATTTGGTATTTGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1473)
553	SASH1	ATTGGGACGTACGGTT
	(SEQ ID NO: 102)	(SEQ ID NO: 1785)
554	SASH1	GATTGGGATGTATGGT
	(SEQ ID NO: 102)	(SEQ ID NO: 1786)
555	SASH1	AGTCGGAATCGGAGTT
	(SEQ ID NO: 102)	(SEQ ID NO: 1474)
556	SASH1	GTTGGAATTGGAGTTTA
	(SEQ ID NO: 102)	(SEQ ID NO: 1475)
557	S100A7	TATAGTCGGGGTGATA
	(SEQ ID NO: 96)	(SEQ ID NO: 1682)
558	S100A7	TTTATAGTTGGGGTGAT
	(SEQ ID NO: 96)	(SEQ ID NO: 1683)
559	S100A7	AGTCGGGCGTTAGTAA
	(SEQ ID NO: 96)	(SEQ ID NO: 1684)
560	S100A7	GAGTTGGGTGTTAGTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1685)
561	S100A7	GGATGGCGGAAGTTTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1686)
562	S100A7	GGATGGTGGAAGTTTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1687)
563	APC	GATTCGTATTTCGTAGT
	(SEQ ID NO: 65)	(SEQ ID NO: 1688)
564	APC	TTTGTATTTTGTAGTGGG
	(SEQ ID NO: 65)	(SEQ ID NO: 1347)
565	APC	AGCGTTTTGGTTCGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1689)
566	APC	AGTGTTTTGGTTTGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1690)
567	APC	TTAATCGGCGGGTTTT
	(SEQ ID NO: 65)	(SEQ ID NO: 1691)
568	APC	AGTTAATTGGTGGGTT
	(SEQ ID NO: 65)	(SEQ ID NO: 1692)
569	APC	ATTTTCGAGTTCGGTA
	(SEQ ID NO: 65)	(SEQ ID NO: 1693)
570	APC	TTTTTGAGTTTGGTAGT
	(SEQ ID NO: 65)	(SEQ ID NO: 1694)
571	ARH1/NOEY2	TGTTATCGTTAACGATT
	(SEQ ID NO: 97)	(SEQ ID NO: 1476)
572	ARH1/NOEY2	AGGTGTTATTGTTAATGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1477)
573	ARH1/NOEY2	TAAAACGTTCGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1478)
574	ARH1/NOEY2	TTTAAAATGTTTGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1479)
575	ARH1/NOEY2	TGTATTCGTCGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1480)
576	ARH1/NOEY2	AATGTATTTGTTGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1481)
577	ARH1/NOEY2	TTAGACGGAGTTCGGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1482)
578	ARH1/NOEY2	TAGATGGAGTTTGGAGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1483)
579	ARH1/NOEY2	TAGACGTAGGCGTATT
	(SEQ ID NO: 97)	(SEQ ID NO: 1484)
580	ARH1/NOEY2	GGGTAGATGTAGGTGT
	(SEQ ID NO: 97)	(SEQ ID NO: 1485)
581	BRCA2	AGTATACGTATTATTCGG
	(SEQ ID NO: 56)	(SEQ ID NO: 1348)
582	BRCA2	AGTATATGTATTATTTGGAA
	(SEQ ID NO: 56)	(SEQ ID NO: 1349)
583	BRCA2	TAGAAGTTCGCGTTAT
	(SEQ ID NO: 56)	(SEQ ID NO: 1350)
584	BRCA2	GAAGTTTGTGTTATAAGT
	(SEQ ID NO: 56)	(SEQ ID NO: 1351)
585	BRCA2	TATCGTCGTAAAAGATAT
	(SEQ ID NO: 56)	(SEQ ID NO: 1352)
586	BRCA2	GATTTATTGTTGTAAAAGAT
	(SEQ ID NO: 56)	(SEQ ID NO: 1353)
587	BRCA2	ATTCGTTTTAGAGGCGTA
	(SEQ ID NO: 56)	(SEQ ID NO: 1695)
588	BRCA2	ATTTGTTTTAGAGGTGTA
	(SEQ ID NO: 56)	(SEQ ID NO: 1696)
589	BRCA2	TTTCGTTACGTTGGAT
	(SEQ ID NO: 56)	(SEQ ID NO: 1354)
590	BRCA2	TTTTTGTTATGTTGGATT
	(SEQ ID NO: 56)	(SEQ ID NO: 1355)
591	CDH1	TATAGACGCGGTGATT
	(SEQ ID NO: 79)	(SEQ ID NO: 1356)
592	CDH1	TATAGATGTGGTGATTTT
	(SEQ ID NO: 79)	(SEQ ID NO: 1357)
593	CDH1	TTGACGGTTCGTTTAT
	(SEQ ID NO: 79)	(SEQ ID NO: 1358)
594	CDH1	GGAGTTGATGGTTTGT
	(SEQ ID NO: 79)	(SEQ ID NO: 1359)
595	CDH1	ATTAGTAGCGCGGATT
	(SEQ ID NO: 79)	(SEQ ID NO: 1360)
596	CDH1	AATTAGTAGTGTGGATTT
	(SEQ ID NO: 79)	(SEQ ID NO: 1361)
597	CDH1	AGGTATCGTTTTTCGT
	(SEQ ID NO: 79)	(SEQ ID NO: 1832)
598	CDH1	GAGGTATTGTTTTTTGTA
	(SEQ ID NO: 79)	(SEQ ID NO: 1833)
599	CDH1	TTCGGAGGTATCGTTT
	(SEQ ID NO: 79)	(SEQ ID NO: 1362)
600	CDH1	TTTTGGAGGTATTGTTT
	(SEQ ID NO: 79)	(SEQ ID NO: 1363)
601	CDKN1A	AGCGTATTAACGTAGG
	(SEQ ID NO: 67)	(SEQ ID NO: 1364)
602	CDKN1A	TTTAGTGTATTAATGTAGG
	(SEQ ID NO: 67)	(SEQ ID NO: 1365)
603	CDKN1A	TGTAGTACGCGAGGTT
	(SEQ ID NO: 67)	(SEQ ID NO: 1366)
604	CDKN1A	TGTAGTATGTGAGGTTT
	(SEQ ID NO: 67)	(SEQ ID NO: 1367)
605	CDKN1A	ATTAGGGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1494)
606	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1495)
607	CDKN1A	TTCGTCGAGGTATCGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1368)
608	CDKN1A	TTTGTTGAGGTATTGAG
	(SEQ ID NO: 67)	(SEQ ID NO: 1369)
609	DAPK1	ATAGATCGTTTAGCGT
	(SEQ ID NO: 98)	(SEQ ID NO: 1370)
610	DAPK1	ATTGTTTAGTGTTTGGG
	(SEQ ID NO: 98)	(SEQ ID NO: 1371)
611	DAPK1	TTTTATTTCGCGAGGA
	(SEQ ID NO: 98)	(SEQ ID NO: 1372)
612	DAPK1	TATTTTGTGAGGAGGG
	(SEQ ID NO: 98)	(SEQ ID NO: 1373)
613	DAPK1	TTTCGGAGATTCGGTT
	(SEQ ID NO: 98)	(SEQ ID NO: 1502)
614	DAPK1	TTTGGAGATTTGGTTTT
	(SEQ ID NO: 98)	(SEQ ID NO: 1503)
615	DAPK1	TTTTAGCGTCGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1504)
616	DAPK1	TTTTAGTGTTGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1505)
617	SEQ ID NO: 2	TAGGGGTTCGATTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 1834)
618	SEQ ID NO: 2	AGGGGTTTGATTAGGG
	(SEQ ID NO: 2)	(SEQ ID NO: 1835)
619	SEQ ID NO: 2	TTGAATTGCGGTTAGA
	(SEQ ID NO: 2)	(SEQ ID NO: 1803)
620	SEQ ID NO: 2	TTGAATTGTGGTTAGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1804)
621	SEQ ID NO: 2	TAGGTATACGAAAGAGTA
	(SEQ ID NO: 2)	(SEQ ID NO: 1697)
622	SEQ ID NO: 2	TTAGGTATATGAAAGAGTA
	(SEQ ID NO: 2)	(SEQ ID NO: 1698)
623	SID NO: 2	TGTGGTACGTTATGTT
	(SEQ ID NO: 2)	(SEQ ID NO: 2226)
624	SEQ ID NO: 2	GGTGTTGTATGTTATGT
	(SEQ ID NO: 2)	(SEQ ID NO: 2227)
625	SEQ ID NO: 2	TTGATTGGCGGACGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1699)
626	SEQ ID NO: 2	TTGATTGGTGGATGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1700)
627	EYA4	GGTATAAAATCGTAAATTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1506)
628	EYA4	GGGTATAAAATTGTAAATTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1507)
629	EYA4	TATGTAGTCGCGTAGT
	(SEQ ID NO: 58)	(SEQ ID NO: 1508)
630	EYA4	TTTATGTAGTTGTGTAGT
	(SEQ ID NO: 58)	(SEQ ID NO: 1509)
631	EYA4	GTTTAGATACGAAATGTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1510)
632	EYA4	GTTTAGATATGAAATGTTAT
	(SEQ ID NO: 58)	(SEQ ID NO: 1511)
633	EYA4	AGTTTTGACGTCGTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1512)
634	EYA4	TTGATGTTGTTTTGGAA
	(SEQ ID NO: 58)	(SEQ ID NO: 1513)
635	FHIT	TTTTCGTTTTACGAGG
	(SEQ ID NO: 76)	(SEQ ID NO: 1374)
636	FHIT	TTTTGTTTTATGAGGGT
	(SEQ ID NO: 76)	(SEQ ID NO: 1375)
637	FHIT	TTTAAGTATCGATTTTAGT
	(SEQ ID NO: 76)	(SEQ ID NO: 1787)
638	FHIT	TAAGTATTGATTTTAGTTTTA
	(SEQ ID NO: 76)	(SEQ ID NO: 1788)
639	FHIT	GTTACGTTAGCGGGTT
	(SEQ ID NO: 76)	(SEQ ID NO: 1514)
640	FHIT	GGTTATGTTAGTGGGT
	(SEQ ID NO: 76)	(SEQ ID NO: 1515)
641	FHIT	TTCGGGGACGTTATAG
	(SEQ ID NO: 76)	(SEQ ID NO: 1516)
642	FHIT	GGTTTGGGGATGTTAT
	(SEQ ID NO: 76)	(SEQ ID NO: 1517)
643	GSTP1	GGCGATTTCGGGGATT
	(SEQ ID NO: 59)	(SEQ ID NO: 1518)
644	GSTP1	GGTGATTTTGGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1519)
645	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1520)
646	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1521)
647	GSTP1	AGTTCGCGGGATTTTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1522)
648	GSTP1	GGAGTTTGTGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1523)
649	GSTP1	AGTTTTCGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1524)
650	GSTP1	TAGTTTTTGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1525)
651	HIC1	TTTTGTCGTACGGAAT
	(SEQ ID NO: 85)	(SEQ ID NO: 1376)
652	HIC1	AGTTTTTGTTGTATGGA
	(SEQ ID NO: 85)	(SEQ ID NO: 1377)
653	HIC1	TATCGAAGTTTTCGGG
	(SEQ ID NO: 85)	(SEQ ID NO: 1526)
654	HIC1	TATTGAAGTTTTTGGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1527)
655	HIC1	TAGCGGTTATTTCGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1528)
656	HIC1	TTTAGTGGTTATTTTGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1529)
657	HIC1	TACGTTTTTCGTAGCGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1530)
658	HIC1	ATTATGTTTTTTGTAGTGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1531)
659	HIC1	TTCGGTTTTGTCGTATA
	(SEQ ID NO: 85)	(SEQ ID NO: 1532)
660	HIC1	TTTGGTTTTGTTGTATAG
	(SEQ ID NO: 85)	(SEQ ID NO: 1533)
661	IGFBP7	TAGTCGCGGAATGTTA
	(SEQ ID NO: 94)	(SEQ ID NO: 1701)
662	IGFBP7	TTGGTAGTTGTGGAAT
	(SEQ ID NO: 94)	(SEQ ID NO: 1702)
663	IGFBP7	ATTTTTTCGCGGGTAT
	(SEQ ID NO: 94)	(SEQ ID NO: 1703)
664	IGFBP7	TTTTTGTGGGTATTTTAG
	(SEQ ID NO: 94)	(SEQ ID NO: 1704)
665	IGFBP7	GGTATATTCGACGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1705)
666	IGFBP7	GGGTATATTTGATGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1706)
667	IGFBP7	GGTACGAGCGTTTTTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1707)
668	IGFBP7	TGGGTATGAGTGTTTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1708)
669	IGFBP7	AAAGCGTATTTAATTCGT
	(SEQ ID NO: 94)	(SEQ ID NO: 1709)
670	GFBP7	AGTGTATTTAATTTGTGTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1710)
671	MLH1	AAGTCGTTTTGACGTA
	(SEQ ID NO: 89)	(SEQ ID NO: 1378)
672	MLH1	TAAGTTGTTTTGATGTAG
	(SEQ ID NO: 89)	(SEQ ID NO: 1379)
673	MLH1	AGGCGGCGATAGATTA
	(SEQ ID NO: 89)	(SEQ ID NO: 1534)
674	MLH1	ATGAGGTGGTGATAGA
	(SEQ ID NO: 89)	(SEQ ID NO: 1535)
675	MLH1	TATCGTTTTTCGGAGG
	(SEQ ID NO: 89)	(SEQ ID NO: 1380)
676	MLH1	TATTGTTTTTTGGAGGT
	(SEQ ID NO: 89)	(SEQ ID NO: 1381)
677	MLH1	TAGAGTTTCGTCGATT
	(SEQ ID NO: 89)	(SEQ ID NO: 1382)
678	MLH1	AGAGTTTTGTTGATTTTT
	(SEQ ID NO: 89)	(SEQ ID NO: 1383)
679	PGR	TTTCGAGGTCGGATTT
	(SEQ ID NO: 83)	(SEQ ID NO: 1536)
680	PGR	TTTGAGGTTGGATTTTT
	(SEQ ID NO: 83)	(SEQ ID NO: 1537)
681	PGR	GTGTCGTTTAGTCGTA
	(SEQ ID NO: 83)	(SEQ ID NO: 1539)
682	PGR	GTTGTTTAGTTGTAGGT
	(SEQ ID NO: 83)	(SEQ ID NO: 1539)
683	PGR	TTCGACGAAAAGACGT
	(SEQ ID NO: 83)	(SEQ ID NO: 1789)
684	PGR	TTTTTTCGACGAAAAGA
	(SEQ ID NO: 83)	(SEQ ID NO: 1540)
685	PGR	AGGATTTTTTTGATGAAA
	(SEQ ID NO: 83)	(SEQ ID NO: 1541)
686	PGR	TTTTTGATGAAAAGATGT
	(SEQ ID NO: 83)	(SEQ ID NO: 1790)
687	SERPINB5	TTATTAACGTGTTTGAGA
	(SEQ ID NO: 68)	(SEQ ID NO: 1542)
688	SERPINB5	TTATTAATGTGTTTGAGAA
	(SEQ ID NO: 68)	(SEQ ID NO: 1543)
689	SERPINB5	ATTGTCGTACGTATGT
	(SEQ ID NO: 68)	(SEQ ID NO: 1544)
690	SERPINB5	AGAGGATTGTTGTATGTA
	(SEQ ID NO: 68)	(SEQ ID NO: 1545)
691	SERPINB5	TTTTTTGTTCGAATATGT
	(SEQ ID NO: 68)	(SEQ ID NO: 1546)
692	SERPINB5	TTTGTTTGAATATGTTGG
	(SEQ ID NO: 68)	(SEQ ID NO: 1547)
693	RARB	ATCGAAAGTTTATTCGTATA
	(SEQ ID NO: 88)	(SEQ ID NO: 1791)
694	RARB	TTATTGAAAGTTTATTTGTA
	(SEQ ID NO: 88)	(SEQ ID NO: 1792)
695	RARB	ATGTCGAGAACGCGAG
	(SEQ ID NO: 88)	(SEQ ID NO: 1548)
696	RARB	GGATGTTGAGAATGTGA
	(SEQ ID NO: 88)	(SEQ ID NO: 1549)
697	RARB	AGCGATTCGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1550)
698	RARB	AGTGATTTGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1551)
699	RARB	TAGGATTCGGAACGTA
	(SEQ ID NO: 88)	(SEQ ID NO: 1552)
700	RARB	GGTAGGATTTGGAATGT
	(SEQ ID NO: 88)	(SEQ ID NO: 1553)
701	SFN	TAGTACGGTGTCGTAT
	(SEQ ID NO: 69)	(SEQ ID NO: 1554)
702	SFN	GTTTAGTATGGTGTTGT
	(SEQ ID NO: 69)	(SEQ ID NO: 1555)
703	SFN	TACGTATTTCGGGTTT
	(SEQ ID NO: 69)	(SEQ ID NO: 1556)
704	SFN	TATTTATGTATTTTGGGTT
	(SEQ ID NO: 69)	(SEQ ID NO: 1557)
705	SFN	TTCGTTTTTCGTAGGAG
	(SEQ ID NO: 69)	(SEQ ID NO: 1558)
706	SFN	TTTGTTTTTTGTAGGAGA
	(SEQ ID NO: 69)	(SEQ ID NO: 1559)
707	SFN	TTTATAGCGTTCGGTT
	(SEQ ID NO: 69)	(SEQ ID NO: 1830)
708	SFN	ATAGTGTTTGGTTTGTT
	(SEQ ID NO: 69)	(SEQ ID NO: 1831)
709	SOD2	GTCGTTTAGTCGGTTTA
	(SEQ ID NO: 105)	(SEQ ID NO: 1711)
710	SOD2	GTTGTTTAGTTGGTTTAT
	(SEQ ID NO: 105)	(SEQ ID NO: 1712)
711	SOD2	TATTAGGCGGTTGCGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1713)
712	SOD2	TATTAGGTGGTTGTGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1714)
713	SOD2	TACGGTTCGAAGGTTT
	(SEQ ID NO: 105)	(SEQ ID NO: 1715)
714	SOD2	AGTTGGTATGGTTTGA
	(SEQ ID NO: 105)	(SEQ ID NO: 1716)
715	SOD2	GTTTCGGTAATTTCGT
	(SEQ ID NO: 105)	(SEQ ID NO: 1384)
716	SOD2	GGTTTTGGTAATTTTGTT
	(SEQ ID NO: 105)	(SEQ ID NO: 1385)
717	TERT	AAGACGTATTGTTCGT
	(SEQ ID NO: 92)	(SEQ ID NO: 1386)
718	TERT	AAGATGTATTGTTTGTTG
	(SEQ ID NO: 92)	(SEQ ID NO: 1387)
719	TERT	AGGTGTACGGTTTCGT
	(SEQ ID NO: 92)	(SEQ ID NO: 1793)
720	TERT	AGGTGTATGGTTTTGT
	(SEQ ID NO: 92)	(SEQ ID NO: 1794)
721	TERT	TATAACGAACGTCGTT
	(SEQ ID NO: 92)	(SEQ ID NO: 1795)
722	TERT	AGGTATAATGAATGTTGT
	(SEQ ID NO: 92)	(SEQ ID NO: 1796)
723	TERT	ATTACGCGTAGTGTTT
	(SEQ ID NO: 92)	(SEQ ID NO: 1388)
724	TERT	TGGGAATTATGTGTAGT
	(SEQ ID NO: 92)	(SEQ ID NO: 1389)
725	TGFBR2	AAGACGGTTAGGTCGG
	(SEQ ID NO: 93)	(SEQ ID NO: 1825)
726	TGFBR2	AAGATGGTTAGGTTGG
	(SEQ ID NO: 93)	(SEQ ID NO: 1826)
727	TGFBR2	TTTTATTTCGAAGCGG
	(SEQ ID NO: 93)	(SEQ ID NO: 1390)
728	TGFBR2	TTTGAAGTGGGTTTATT
	(SEQ ID NO: 93)	(SEQ ID NO: 1391)
729	TGFBR2	ATGGGGCGGACGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1560)
730	TGFBR2	ATGGGGTGGATGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1561)
731	TGFBR2	ATAACGTATTAGGAGCGG
	(SEQ ID NO: 93)	(SEQ ID NO: 1392)
732	TGFBR2	ATAATGTATTAGGAGTGG
	(SEQ ID NO: 93)	(SEQ ID NO: 1393)
733	THRB	GAGCGTCGTAAGAATT
	(SEQ ID NO: 106)	(SEQ ID NO: 1394)
734	THRB	GGAGTGTTGTAAGAATT
	(SEQ ID NO: 106)	(SEQ ID NO: 1395)
735	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1562)
736	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1563)
737	THRB	TTTAATCGTAGCGGTT
	(SEQ ID NO: 106)	(SEQ ID NO: 1396)
738	THRB	AATTGTAGTGGTTTTGT
	(SEQ ID NO: 106)	(SEQ ID NO: 1397)
739	THRB	TAGCGTCGAATTTAGT
	(SEQ ID NO: 106)	(SEQ ID NO: 1398)
740	THRB	TTAGTGTTGAATTTAGTG
	(SEQ ID NO: 106)	(SEQ ID NO: 1399)
741	TIMP3	TTATTAACGGAGGAAGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1564)
742	TIMP3	TATTAATGGAGGAAGGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1565)
743	TIMP3	TTCGTTATGTGTACGGAA
	(SEQ ID NO: 1031)	(SEQ ID NO: 1566)
744	TIMP3	TTTGTTATGTGTATGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1567)
745	TIMP3	GAGTATTTCGAGTTTGT
	(SEQ ID NO: 103)	(SEQ ID NO: 1568)
746	TIMP3	AGTATTTTGAGTTTGTATT
	(SEQ ID NO: 103)	(SEQ ID NO: 1569)
747	TIMP3	TAAGCGTTAATCGAGT
	(SEQ ID NO: 103)	(SEQ ID NO: 1570)
748	TIMP3	TAGGTAAGTGTTAATTGA
	(SEQ ID NO: 103)	(SEQ ID NO: 1571)
749	TP53	AGGATTTTCGTCGATT
	(SEQ ID NO: 80)	(SEQ ID NO: 1400)
750	TP53	TTAGGATTTTTGTTGATTT
	(SEQ ID NO: 80)	(SEQ ID NO: 1401)
751	TP53	TAATTCGTTTGTCGGA
	(SEQ ID NO: 80)	(SEQ ID NO: 1402)
752	TP53	ATTTGTTTGTTGGAGGA
	(SEQ ID NO: 80)	(SEQ ID NO: 1403)
753	TP53	TGGATAGTCGTTATGAT
	(SEQ ID NO: 80)	(SEQ ID NO: 1404)
754	TP53	TTGGATAGTTGTTATGAT
	(SEQ ID NO: 80)	(SEQ ID NO: 1405)
755	TP53	AATTTTTGCGAGGTTT
	(SEQ ID NO: 80)	(SEQ ID NO: 1406)
756	TP53	TAATTTTTGTGAGGTTTT
	(SEQ ID NO: 80)	(SEQ ID NO: 1407)
757	TP73	TAGGATTCGCGTTTTT
	(SEQ ID NO: 86)	(SEQ ID NO: 1572)
758	TP73	GGTAGGATTTGTGTTTT
	(SEQ ID NO: 86)	(SEQ ID NO: 1573)
759	TP73	TTTTTCGCGAGCGTTA
	(SEQ ID NO: 86)	(SEQ ID NO: 1408)
760	TP73	TTTTGTGAGTGTTAAGT
	(SEQ ID NO: 86)	(SEQ ID NO: 1409)
761	TP73	GGGTCGATTTAATTTCGA
	(SEQ ID NO: 86)	(SEQ ID NO: 1410)
762	TP73	GGGTTGATTTAATTTTGA
	(SEQ ID NO: 86)	(SEQ ID NO: 1411)
763	TP73	TTTCGGAGTTGCGAGT
	(SEQ ID NO: 86)	(SEQ ID NO: 1574)
764	TP73	TAGTTTTGGAGTTGTGA
	(SEQ ID NO: 86)	(SEQ ID NO: 1575)
765	NME1	AGTCGAGATTGCGTTA
	(SEQ ID NO: 107)	(SEQ ID NO: 1805)
766	NME1	AGTTGAGATTGTGTTAG
	(SEQ ID NO: 107)	(SEQ ID NO: 1806)
767	NME1	ATCGTTTGAATTCGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 1807)
768	NME1	ATTGTTTGAATTTGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 1808)
769	NME1	AATTCGAGATTAGTTCGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1717)
770	NME1	AATTTGAGATTAGTTTGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1718)
771	NME1	TTTTAGTACGTTGGAAA
	(SEQ ID NO: 107)	(SEQ ID NO: 1809)
772	NM31	TTAGTATGTTGGAAAGTA
	(SEQ ID NO: 107)	(SEQ ID NO: 1810)
773	CDH13	TAAAACGAGGGAGCGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1576)
774	CDH13	AAAATGAGGGAGTGTT
	(SEQ ID NO: 70)	(SEQ ID NO: 1577)
775	CDH13	TAGTCGCGTGTATGAA
	(SEQ ID NO: 70)	(SEQ ID NO: 1578)
776	CDH13	TGTAGTTGTGTGTATGA
	(SEQ ID NO: 70)	(SEQ ID NO: 1579)
777	CDH13	ATGAAAACGTCGTCG
	(SEQ ID NO: 70)	(SEQ ID NO: 1580)
778	CDH13	AATGAAAATGTTGTTGG
	(SEQ ID NO: 70)	(SEQ ID NO: 1581)
779	CDH13	TAGTCGAGAATTTCGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1582)
780	CDH13	TGTAGTTGAGAATTTTGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1583)
781	THBS1	TTGGCGCGTAATTTTT
	(SEQ ID NO: 81)	(SEQ ID NO: 1811)
782	THBS1	TGTTTGGTGTGTAATTT
	(SEQ ID NO: 81)	(SEQ ID NO: 1812)
783	THBS1	TAAAGGGGCGTTCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1719)
784	THBS1	AAGGGGTGTTTGTATT
	(SEQ ID NO: 81)	(SEQ ID NO: 1720)
785	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1721)
786	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1722)
787	THBS1	TTGTGCGTTCGGAGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1723)
788	THBS1	TGTGTTTGGAGTAGAG
	(SEQ ID NO: 81)	(SEQ ID NO: 1724)
789	TMS1/ASC	TTCGTTTCGGAGTCGA
	(SEQ ID NO: 84)	(SEQ ID NO: 1584)
790	TMS1/ASC	TTTGTTTTGGAGTTGAT
	(SEQ ID NO: 84)	(SEQ ID NO: 1585)
791	TMS1/ASC	TTCGGAGTCGATTTTT
	(SEQ ID NO: 84)	(SEQ ID NO: 1412)
792	TMS1/ASC	GTTTTGGAGTTGATTTTT
	(SEQ ID NO: 84)	(SEQ ID NO: 1413)
793	TMS1/ASC	ATTTGATCGTCGAGGA
	(SEQ ID NO: 84)	(SEQ ID NO: 1414)
794	TMS1/ASC	TTGATTGTTGAGGAGT
	(SEQ ID NO: 84)	(SEQ ID NO: 1415)
795	TMS1/ASC	AGGGTTACGGGCGTAT
	(SEQ ID NO: 84)	(SEQ ID NO: 1416)
796	TMS1/ASC	AGGGTTATGGGTGTAT
	(SEQ ID NO: 84)	(SEQ ID NO: 1417)
797	ESR1	AAATCGGCGGGTTATT
	(SEQ ID NO: 75)	(SEQ ID NO: 1725)
798	ESR1	AGAAATTGGTGGGTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1726)
799	ESR1	AGATCGTGTTTTCGTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1836)
800	ESR1	ATTGTGTTTTTGTAGGG
	(SEQ ID NO: 75)	(SEQ ID NO: 1837)
801	ESR1	AGTTGCGGACGGTTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1727)
802	ESR1	AGTTGTGGATGGTTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1728)
803	IL6	AGATGTCGTCGAGGAT
	(SEQ ID NO: 99)	(SEQ ID NO: 1813)
804	IL6	ATGTTGTTGAGGATGTA
	(SEQ ID NO: 99)	(SEQ ID NO: 1814)
805	IL6	TATGCGTATCGGGTTT
	(SEQ ID NO: 99)	(SEQ ID NO: 1418)
806	IL6	ATGTGTATTGGGTTTTT
	(SEQ ID NO: 99)	(SEQ ID NO: 1419)
807	IL6	TTCGGTTATACGTAGG
	(SEQ ID NO: 99)	(SEQ ID NO: 1729)
808	IL6	TTTTGGTTATATGTAGGG
	(SEQ ID NO: 99)	(SEQ ID NO: 1730)
809	IL6	AGTTTAGTCGGTTTCGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1731)
810	IL6	AGTTTAGTTGGTTTTGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1732)
811	APAF1	GATTCGCGAAGATTTG
	(SEQ ID NO: 82)	(SEQ ID NO: 1420)
812	APAF1	GATTTGTGAAGATTTGAG
	(SEQ ID NO: 82)	(SEQ ID NO: 1421)
813	APAF1	GTGTCGTAGCGGTATT
	(SEQ ID NO: 82)	(SEQ ID NO: 1586)
814	APF1	GGTGTTGTAGTGGTAT
	(SEQ ID NO: 82)	(SEQ ID NO: 1587)
815	APAF1	AGTAGCGTCGGGTTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1588)
816	APAF1	GAGTAGTGTTGGGTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1589)
817	APAF1	TGGACGTTTATTTCGT
	(SEQ ID NO: 82)	(SEQ ID NO: 1422)
818	APAF1	GTGGATGTTTATTTTGTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1423)
819	CASP8	AGGTAACGGTTTAGAG
	(SEQ ID NO: 71)	(SEQ ID NO: 1424)
820	CASP8	AGGTAATGGTTTAGAGA
	(SEQ ID NO: 71)	(SEQ ID NO: 1425)
821	CASP8	TGTATTCGAGGCGGTA
	(SEQ ID NO: 71)	(SEQ ID NO: 1733)
822	CASP8	TTGTATTTGAGGTGGT
	(SEQ ID NO: 71)	(SEQ ID NO: 1734)
823	CASP8	ATTTTTTAAACGGGTTTA
	(SEQ ID NO: 71)	(SEQ ID NO: 1735)
824	CASP8	TTTTAAATGGGTTTATAGG
	(SEQ ID NO: 71)	(SEQ ID NO: 1736)
825	CASP8	ATCGTAGTTTTCGAGT
	(SEQ ID NO: 71)	(SEQ ID NO: 1737)
826	CASP8	ATTGTAGTTTTTGAGTTT
	(SEQ ID NO: 71)	(SEQ ID NO: 1738)
827	SYK	GAAGTTATCGCGTTGG
	(SEQ ID NO: 60)	(SEQ ID NO: 1590)
828	SYK	AGAAGTTATTGTGTTGG
	(SEQ ID NO: 60)	(SEQ ID NO: 1591)
829	SYK	GATCGATGCGGTTTAT
	(SEQ ID NO: 60)	(SEQ ID NO: 1592)
830	SYK	GGGATTGATGTGGTTT
	(SEQ ID NO: 60)	(SEQ ID NO: 1593)
831	SYK	GGCGTTTTAGTCGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1594)
832	SYK	GGTGTTTTAGTTGATTTT
	(SEQ ID NO: 60)	(SEQ ID NO: 1595)
833	SYK	TTATTCGGTCGGGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1596
834	SYK	TTTATTTGGTTGGGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1597)
835	HOXA5	TTCGAGTTCGGTTGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1739)
836	HOXA5	GTTTGAGTTTGGTTGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1740)
837	HOXA5	TAGTTTTCGGTCGGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1741)
838	HOXA5	TAGTTTTTGGTTGGAAG
	(SEQ ID NO: 78)	(SEQ ID NO: 1742)
839	HOXA5	TAATTCGATTTCGGTTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1743)
840	HOXA5	TTTAATTTGATTTTGGTTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1744)
841	HOXA5	ATCGGTAGTTGACGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1745)
842	HOXA5	ATTGGTAGTTGATGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1746)
843	FABP3	GATGGGCGTATTAGTT
	(SEQ ID NO: 77)	(SEQ ID NO: 1598)
844	FABP3	GGGATGGGTGTATTAG
	(SEQ ID NO: 77)	(SEQ ID NO: 1599)
845	FABP3	GTGATGCGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1600)
846	FABP3	GTGATGTGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1601)
847	FABP3	TAAAGCGGTAGTTCGG
	(SEQ ID NO: 77)	(SEQ ID NO: 1602)
848	FABP3	AAGTGGTAGTTTGGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1603)
849	FABP3	TATTGGCGTTGACGTA
	(SEQ ID NO: 77)	(SEQ ID NO: 1604)
850	FABP3	TGGTGTTGATGTAGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1605)
851	RASSF1A	TACGGGTATTTTCGCGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1606)
852	RASSF1A	ATATGGGTATTTTTGTGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1607)
853	RASSF1A	AGAGCGCGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1608)
854	RASSF1A	GAGAGTGTGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1609)
855	RASSF1A	AGTAAATCGGATTAGGA
	(SEQ ID NO: 90)	(SEQ ID NO: 1610)
856	RASSF1A	AGTAAATTGGATTAGGAG
	(SEQ ID NO: 90)	(SEQ ID NO: 1611)
857	RARA	TTCGGGATGTACGTTT
	(SEQ ID NO: 108)	(SEQ ID NO: 1747)
858	RARA	TTTGGGATGTATGTTTT
	(SEQ ID NO: 108)	(SEQ ID NO: 1748)
859	RARA	GAATTAGTATCGGTTTTT
	(SEQ ID NO: 108)	(SEQ ID NO: 1749)
860	RARA	ATTAGTATTGGTTTTTGG
	(SEQ ID NO: 108)	(SEQ ID NO: 1750)
861	RARA	AAAGTTTCGTTTAAGGT
	(SEQ ID NO: 108)	(SEQ ID NO: 1426)
862	RARA	AAAGTTTTGTTTAAGGTG
	(SEQ ID NO: 108)	(SEQ ID NO: 1427)
863	RARA	TTTCGGCGAGTAAAGT
	(SEQ ID NO: 108)	(SEQ ID NO: 1428)
864	RARA	TTTTTGGTGAGTAAAGT
	(SEQ ID NO: 108)	(SEQ ID NO: 1429)
865	TWIST	AGTAAAGGCGTTGCGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1612)
866	TWIST	AGTAAAGGTGTTGTGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1613)
867	TWIST	TATTTTTCGAGGCGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1614)
868	TWIST	TTTTGAGGTGTAGTTTT
	(SEQ ID NO: 100)	(SEQ ID NO: 1615)
869	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1616)
870	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1617)
871	TWIST	TAGGTCGGGACGTAAA
	(SEQ ID NO: 100)	(SEQ ID NO: 1618)
872	TWIST	AGTAGGTTGGGATGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1619)
873	AR	TTAAGAGGCGAAAAGT
	(SEQ ID NO: 61)	(SEQ ID NO: 1430)
874	AR	AAGAGGTGAAAAGTAGT
	(SEQ ID NO: 61)	(SEQ ID NO: 1431)
875	AR	AATATGCGAAGGTAATT
	(SEQ ID NO: 61)	(SEQ ID NO: 1432)
876	AR	TTAAAATATGTGAAGGTAA
	(SEQ ID NO: 61)	(SEQ ID NO: 1433)
877	AR	AAGTAAGCGGTTGTAT
	(SEQ ID NO: 61)	(SEQ ID NO: 1434)
878	AR	AAGTAAGTGGTTGTATAT
	(SEQ ID NO: 61)	(SEQ ID NO: 1435)
879	AR	ATTGAGCGTTTATGTG
	(SEQ ID NO: 61)	(SEQ ID NO: 1436)
880	AR	ATTGAGTGTTTATGTGT
	(SEQ ID NO: 61)	(SEQ ID NO: 1437)
881	ESR2	GAGTATTTTCGAATCGA
	(SEQ ID NO: 91)	(SEQ ID NO: 1620)
882	ESR2	GGAGTATTTTTGAATTGA
	(SEQ ID NO: 91)	(SEQ ID NO: 1621)
883	ESR2	ATAAGCGATTTAACGAT
	(SEQ ID NO: 91)	(SEQ ID NO: 1622)
884	ESR2	AAGTGATTTAATGATAAGT
	(SEQ ID NO: 91)	(SEQ ID NO: 1623)
885	ESR2	ATTTCGAGGATTACGT
	(SEQ ID NO: 91)	(SEQ ID NO: 1438)
886	ESR2	ATATTTTGAGGATTATGTT
	(SEQ ID NO: 91	(SEQ ID NO: 1439)
887	ESR2	TTTACGTGATCGAGTT
	(SEQ ID NO: 91)	(SEQ ID NO: 1624)
888	ESR2	AGTTTATGTGATTGAGTT
	(SEQ ID NO: 91)	(SEQ ID NO: 1625)
889	PLAU	TATTTGTCGCGTTGAT
	(SEQ ID NO: 62)	(SEQ ID NO: 1626)
890	PLAU	ATTTGTTGTGTTGATGA
	(SEQ ID NO: 62)	(SEQ ID NO: 1627)
891	PLAU	TGTAATTCGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1628)
892	PLAU	TTGTAATTTGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1629)
893	PLAU	TTGGAGATCGCGTTTT
	(SEQ ID NO; 62)	(SEQ ID NO: 1630)
894	PLAU	TTGGAGATTGTGTTTTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1631)
895	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1632)
896	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1633)
897	STAT1	GTTATTTTCGAGAGTTG
	(SEQ ID NO: 109)	(SEQ ID NO: 1634)
898	STAT1	GTTATTTTTGAGAGTTGT
	(SEQ ID NO: 109)	(SEQ ID NO: 1635)
899	STAT1	AGGTTAACGTTCGTAT
	(SEQ ID NO: 109)	(SEQ ID NO: 1440)
900	STAT1	TTAGGTTAATGTTTGTATT
	(SEQ ID NO: 109)	(SEQ ID NO: 1441)
901	STAT1	TAATTTCGATAGTTTTGG
	(SEQ 1D NO: 109)	(SEQ ID NO: 1442)
902	STAT1	TATAATTTTGATAGTTTTGG
	(SEQ ID NO: 109)	(SEQ ID NO: 1443)
903	STAT1	ATATGATTTCGGAATTTTA
	(SEQ ID NO: 109)	(SEQ ID NO: 1797)
904	STAT1	ATATGATTTTGGAATTTTAA
	(SEQ ID NO: 109)	(SEQ ID NO: 1798)
905	BRCA1	AGTTTCGAGAGACGTT
	(SEQ ID NO: 66)	(SEQ ID NO: 1636)
906	BRCA1	AGAGTTTTGAGAGATGT
	(SEQ ID NO: 66)	(SEQ ID NO: 1637
907	BRCA1	TTTCGTGGTAACGGAA
	(SEQ ID NO: 66)	(sEQ ID NO: 1638)
908	BRCA1	TTTGTGGTAATGGAAAA
	(SEQ ID NO: 66)	(SEQ ID NO: 1639)
909	BRCA1	AAAGCGCGGGAATTAT
	(SEQ ID NO: 66)	(SEQ ID NO: 1640)
910	BRCA1	GGAAAAGTGTGGGAAT
	(SEQ ID NO: 66)	(SEQ ID NO: 1641)
911	BRCA1	TTTACGTTATTCGGGG
	(SEQ ID NO: 66)	(SEQ ID NO: 1444)
912	BRCA1	TATGTTATTTGGGGGTA
	(SEQ ID NO: 66)	(SEQ ID NO: 1445)
913	LOT1	ATGGGTACGTTTAAGG
	(SEQ ID NO: 95)	(SEQ ID NO: 1642)
914	LOT1	TGGGTATGTTTAAGGG
	(SEQ ID NO: 95)	(SEQ ID NO: 1643)
915	LOT1	AAATTAGTTACGTTATTTAA
	(SEQ ID NO: 95)	(SEQ ID NO: 1644)
916	LOT1	TGAAATTAGTTATGTTATTTA
	(SEQ ID NO: 95)	(SEQ ID NO: 1645)
917	LOT1	GAGTTTCGTGGTTGAA
	(SEQ ID NO: 95)	(SEQ ID NO: 1799)
918	LOT1	GAGTTTTGTGGTTGAA
	(SEQ ID NO: 95)	(SEQ ID NO: 1800)
919	LOT1	ATGTCGGTTATTACGT
	(SEQ ID NO: 95)	(SEQ ID NO: 1646)
920	LOT1	TGTTGGTTATTATGTAGA
	(SEQ ID NO: 95)	(SEQ ID NO: 1647)
921	PRSS8	AGTTGGCGGAGTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1648)
922	PRSS8	AGTTGGTGGAGTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1649)
923	PRSS8	ATTTTGCGTGGTTAGA
	(SEQ ID NO: 72)	(SEQ ID NO: 1446)
924	PRSS8	GATTTTGTGTGGTTAGA
	(SEQ ID NO: 72)	(SEQ ID NO: 1447)
925	PRSS8	TTGGTGATTCGTTTATAT
	(SEQ ID NO: 72)	(SEQ ID NO: 1650)
926	PRSS8	GTTGGTGATTTGTTTATA
	(SEQ ID NO: 72)	(SEQ ID NO: 1651)
927	PRSS8	TGTTCGTTTCGGATAT
	(SEQ ID NO: 72)	(SEQ ID NO: 1652)
928	PRSS8	TTTGTTTTGGATATTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1653)
929	SNCG	TGCGGTAGTATTCGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1751)
930	SNCG	TGTGGTAGTATTTGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1752)
931	SNCG	TATCGGGGATAGTCGTT
	(SEQ ID NO: 73)	(SEQ ID NO: 1815)
932	SNCG	TATTGGGGATAGTTGTT
	(SEQ ID NO: 73)	(SEQ ID NO: 1816)
933	SNCG	TATCGGCGTTAATAGG
	(SEQ ID NO: 73)	(SEQ ID NO: 1817)
934	SNCG	TATTGGTGTTAATAGGAG
	(SEQ ID NO: 73)	(SEQ ID NO: 1818)
935	SNCG	ATTGTACGTAGGGTTG
	(SEQ ID NO: 73)	(SEQ ID NO: 1819)
936	SNCG	TTTTATTGTATGTAGGGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1820)
937	TPM1	TTGATTCGCGTTCGTA
	(SEQ ID NO: 110)	(SEQ ID NO: 1654)
938	TPM1	TGATTTGTGTTTGTAGA
	(SEQ ID NO: 110)	(SEQ ID NO: 1655)
939	TPM1	AAGAGTCGTTTTAGGT
	(SEQ ID NO: 110)	(SEQ ID NO: 1448)
940	TPM1	TAAGAGTTGTTTTAGGTT
	(SEQ ID NO: 110)	(SEQ ID NO: 1449)
941	TPM1	GTCGAGAGCGTATTGA
	(SEQ ID NO: 110)	(SEQ ID NO: 1450)
942	TPM1	GGTGTTGAGAGTGTAT
	(SEQ ID NO: 110)	(SEQ ID NO: 1451)
943	TPM1	GGCGACGCGTATTTAT
	(SEQ ID NO: 110)	(SEQ ID NO: 1452)
944	TPM1	GGGGTGATGTGTATTT
	(SEQ ID NO: 110)	(SEQ ID NO: 1453)
945	GPC3	AATAGTCGCGTTTAGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1753)
946	GPC3	TAGTTGTGTTTAGGGAT
	(SEQ ID NO: 118)	(SEQ ID NO: 1754)
947	GPC3	TTTAACGTAGTTTTGATCGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1755)
948	GPC3	TTTAATGTAGTTTTGATTGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1756)
949	GPC3	TTTTTCGGGAATCGTT
	(SEQ ID NO: 118)	(SEQ ID NO: 1454)
950	GPC3	AGTTTTTTGGGAATTGT
	(SEQ ID NO: 118)	(SEQ ID NO: 1455)
951	GPC3	TTCGAGCGCGTTGATT
	(SEQ ID NO: 118)	(SEQ ID NO: 1456)
952	GPC3	TAGGTTTGAGTGTGTT
	(SEQ ID NO: 118)	(SEQ ID NO: 1457)
953	CLDN7	TTACGTTAAGTCGGGT
	(SEQ ID NO: 87)	(SEQ ID NO: 1757)
954	CLDN7	AGTTATGTTAAGTTGGG
	(SEQ ID NO: 87)	(SEQ ID NO: 1758)
955	CLDN7	TAGCGTTTTAGGCGTA
	(SEQ ID NO: 87)	(SEQ ID NO: 1759)
956	CLDN7	TAGTGTTTTAGGTGTATT
	(SEQ ID NO: 87)	(SEQ ID NO: 1760)
957	CLDN7	TTAGGGGCGTTTCGTA
	(SEQ ID NO: 87)	(SEQ ID NO: 1761)
958	CLDN7	TTAGGGGTGTTTTGTAG
	(SEQ ID NO: 87)	(SEQ ID NO: 1762)
959	CLDN7	TAGAATTCGGCGGGGA
	(SEQ ID NO: 87)	(SEQ ID NO: 1763)
960	CLDN7	TAGAATTTGGTGGGGA
	(SEQ ID NO: 87)	(SEQ ID NO: 1764)
961	SLC19A1	TATAAGTTCGTACGGG
	(SEQ ID NO: 116)	(SEQ ID NO: 1458)
962	SLC19A1	ATAAGTTTGTATGGGTTA
	(SEQ ID NO: 116)	(SEQ ID NO: 1459)
963	SLC19A1	GTCGTGCGGTTTTTAA
	(SEQ ID NO: 116)	(SEQ ID NO: 1656)
964	SLC19A1	GGTTGTGTGGTTTTTAA
	(SEQ ID NO: 116)	(SEQ ID NO: 1657)
965	SLC19A1	TTACGAAGGCGGTTTA
	(SEQ ID NO: 116)	(SEQ ID NO: 1658)
966	SLC19A1	TTTTATGAAGGTGGTTT
	(SEQ ID NO: 116)	(SEQ ID NO: 1659)
967	SLC19A1	GGTTCGATTCGCGTTT
	(SEQ ID NO: 116)	(SEQ ID NO: 1460)
968	SLC19A1	TGGGTTTGATTTGTGTT
	(SEQ ID NO: 116)	(SEQ ID NO: 1461)
969	GJB2	GGATTTCGTCGGTATT
	(SEQ ID NO: 111)	(SEQ ID NO: 1660)
970	GJB2	GGGGATTTTGTTGGTA
	(SEQ ID NO: 111)	(SEQ ID NO: 1661)
971	GJB2	TTTCGCGATTCGAATA
	(SEQ ID NO: 111)	(SEQ ID NO: 1462)
972	GJB2	TAGTTTTTGTGATTTGAA
	(SEQ ID NO: 111)	(SEQ ID NO: 1463)
973	GJB2	TTTCGTATTATGCGGA
	(SEQ ID NO: 111)	(SEQ ID NO: 1801)
974	GJB2	TTTGTATTATGTGGAGTA
	(SEQ ID NO: 111)	(SEQ ID NO: 1802)
975	GJB2	GAATTTCGTTTACGGT
	(SEQ ID NO: 111)	(SEQ ID NO: 1662)
976	GJB2	TTGAATTTTGTTTATGGT
	(SEQ ID NO: 111)	(SEQ ID NO: 1663)
977	SLIT2	TTCGATAGTTAACGATG
	(SEQ ID NO: 112)	(SEQ ID NO: 1765)
978	SLIT2	TTTGATAGTTAATGATGGT
	(SEQ ID NO: 112)	(SEQ ID NO: 1766)
979	SLIT2	ATTTCGTCGTAGTTTG
	(SEQ ID NO: 112)	(SEQ ID NO: 1767)
980	SLIT2	TTTTGTTGTAGTTTGGA
	(SEQ ID NO: 112)	(SEQ ID NO: 1768)
981	SLIT2	TAGCGGGTTCGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1769)
982	SLIT2	TTAGTGGGTTTGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1770)
983	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1771)
984	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1772)
985	IGSF4	AGGTAGATCGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1773)
986	IGSF4	AGGTAGATTGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1774)
987	IGSF4	TAGTCGTAGAGTCGGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1775)
988	IGSF4	GTTGTAGAGTTGGGTT
	(SEQ ID NO: 74)	(SEQ ID NO: 1776)
989	IGSF4	TTAGCGGTAGATTCGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1464)
990	IGSF4	AGTGGTAGATTTGGGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1465)
991	IGSF4	TAGGTTTTCGGATTGA
	(SEQ ID NO: 74)	(SEQ ID NO: 1777)
992	IGSF4	GTAGGTTTTTGGATTGA
	(SEQ ID NO: 74)	(SEQ ID NO: 1778)
993	MCT1	ATTTTACGTAGGCGTT
	(SEQ ID NO: 101)	(SEQ ID NO: 1779)
994	MCT1	GATTTTATGTAGGTGTTT
	(SEQ ID NO: 101)	(SEQ ID NO: 1780)
995	MCT1	AGTTAGTCGCGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1781)
996	MCT1	AGAGTTAGTTGTGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1782)
997	MCT1	AGTCGTTATTCGGAAA
	(SEQ ID NO: 101)	(SEQ ID NO: 1821)
998	MCT1	TGTAGTTGTTATTTGGAA
	(SEQ ID NO: 101)	(SEQ ID NO: 1822)
999	MCT1	TATACGAGGAAGGTCGG
	(SEQ ID NO: 101)	(SEQ ID NO: 1783)
1000	MCT1	TATATGAGGAAGGTTGG
	(SEQ ID NO: 101)	(SEQ ID NO: 1784)
1001	CCND2	AACGTTATTAGATCGTAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1466)
1002	CCND2	AGAAATGTTATTAGATTGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1467)
1003	CCND2	TTAGGGTCGATCGTGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1486)
1004	CCND2	TAGGGTTGATTGTGTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1487)
1005	CCND2	TTATCGTAGTCGGTTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1488)
1006	CCND2	GATTTTATTGTAGTTGGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1489)
1007	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1490)
1008	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1491)
1009	CCND2	AAGGATCGAGCGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1492)
1010	CCND2	AAGGATTGAGTGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1493)
1011	CDKN2A	GGCGTTGTTTAACGTAT
	(SEQ ID NO: 57)	(SEQ ID NO: 1496)
1012	CDKN2A	GGGTGTTGTTTAATGTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1497)
1013	CDKN2A	AATAGTTACGGTCGGA
	(SEQ ID NO: 57)	(SEQ ID NO: 1498)
1014	CDKN2A	AGTTATGGTTGGAGGT
	(SEQ ID NO: 57)	(SEQ ID NO: 1499)
1015	CDKN2A	GTCGGAGGTCGATTTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1500)
1016	CDKN2A	GGTTGGAGGTTGATTTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1501)

TABLE 3
Genes and sequences
		Sense	Antisense	Sense	Antisense
		methylated	methylated	unmethylated	unmethylated
	Genomic	converted	converted	converted	converted
Gene	SEQ ID NO:	SEQ ID NO:	SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
Genomic region	1	493	494	729	730
Genomic region	2	495	496	731	732
Genomic region	3	497	498	733	734
Genomic region	4	499	500	735	736
Genomic region	5	501	502	737	738
Genomic region	6	503	504	739	740
Genomic region	7	505	506	741	742
Genomic region	8	507	508	743	744
Genomic region	9	509	510	745	746
PROSTAGLANDIN E2 RECEPTOR	10	511	512	747	748
ORPHAN NUCLEAR RECEPTOR	11	513	514	749	750
NR5A2
LIM DOMAIN KINASE 1 (LIMK-1)	12	515	516	751	752
MSF	13	517	518	753	754
Genomic region	14	519	520	755	756
Genomic region	15	521	522	757	758
Genomic region	16	523	524	759	760
Genomic region	17	525	526	761	762
Genomic region	18	527	528	763	764
Genomic region	19	529	530	765	766
PRDM6	20	531	532	767	768
RAP2B	21	533	534	769	770
NR2E1	22	535	536	771	772
PCDH7	23	537	538	773	774
DKK3	24	539	540	775	776
RTTN	25	541	542	777	778
Genomic region	26	543	544	779	780
GIRK2	27	545	546	781	782
Genomic region	28	547	548	783	784
Genomic region	29	549	550	785	786
ARL7	30	551	552	787	788
Genomic region	31	553	554	789	790
THH	32	555	556	791	792
SNAP25	33	557	558	793	794
HOXB13	34	559	560	795	796
Genomic region	35	561	562	797	798
Genomic region	36	563	564	799	800
MGC10561	37	565	566	801	802
LMX1A	38	567	568	803	804
SENP3	39	569	570	805	806
GS1	40	571	572	807	808
T1TF1	41	573	574	809	810
SEQ ID NO: 42	42	575	576	811	812
DDX51	43	577	578	813	814
Q8NAN2	44	579	580	815	816
Genomic region	45	581	582	817	818
Genomic region	46	583	584	819	820
O60279	47	585	586	821	822
Genomic region	48	587	588	823	824
KOX7	49	589	590	825	826
BCL11B	50	591	592	827	828
Genomic region	51	593	594	829	830
MGC34831	52	595	596	831	832
COL5A1	53	597	598	833	834
Genomic region	54	599	600	835	836
PDLIM1	55	601	602	837	838
BRCA2	56	603	604	839	840
CDKN2A	57	605	606	841	842
EYA4	58	607	608	843	844
GSTP1	59	609	610	845	846
SYK	60	611	612	847	848
AR	61	613	614	849	850
PLAU	62	615	616	851	852
LEF1	63	617	618	853	854
ALX4	64	619	620	855	856
APC	65	621	622	857	858
BRCA1	66	623	624	859	860
CDKN1A	67	625	626	861	862
SERPINB5	68	627	628	863	864
SFN	69	629	630	865	866
CDH13	70	631	632	867	868
CASP8	71	633	634	869	870
PRSS8	72	635	636	871	872
SNCG	73	637	638	873	874
IGSF4	74	639	640	875	876
ESR1	75	641	642	877	878
FHIT	76	643	644	879	880
FABP3	77	645	646	881	882
HOXA5	78	647	648	883	884
CDH1	79	649	650	885	886
TP53	80	651	652	887	888
THBS1	81	653	654	889	890
APAF1	82	655	656	891	892
PGR	83	657	658	893	894
TMS1/ASC	84	659	660	895	896
HIC1	85	661	662	897	898
TP73	86	663	664	899	900
CLDN7	87	665	666	901	902
RARB	88	667	668	903	904
MLH1	89	669	670	905	906
RASSF1A	90	671	672	907	908
ESR2	91	673	674	909	910
TERT	92	675	676	911	912
TGFBR2	93	677	678	913	914
IGFBP7	94	679	680	915	916
LOT1	95	681	682	917	918
S100A7	96	683	684	919	920
ARH1/NOEY2	97	685	686	921	922
DAPK1	98	687	688	923	924
IL6	99	689	690	925	926
TWIST	100	691	692	927	928
MCT1	101	693	694	929	930
SASH1	102	695	696	931	932
TIMP3	103	697	698	933	934
CCND2	104	699	700	935	936
SOD2	105	701	702	937	938
THRB	106	703	704	939	940
NME1	107	705	706	941	942
RARA	108	707	708	943	944
STAT1	109	709	710	945	946
TPM1	110	711	712	947	948
GJB2	111	713	714	949	950
SLIT2	112	715	716	951	952
HS3ST2	113	717	718	953	954
PRDM2	114	719	720	955	956
SCGB3A1	115	721	722	957	958
SLC19A1	116	723	724	959	960
Genomic region	117	725	726	961	962
GPC3	118	727	728	963	964

TABLE 4
Breast cancer vs. all other controls Chip 1
									n
	SEQ ID					P-value	P-value	n	Significant
Gene Name	NO:	Accuracy	Sensitivity	Specificity	p-value	(Bonferroni)	FDR	Oligos	oligos
PRDM2	SEQ ID	0.781	0.798	0.754	3.34E−39	2.04E−37	2.04E−37	4	3
	NO: 114
PLAU	SEQ ID	0.769	0.781	0.751	3.87E−35	2.36E−33	1.38E−33	4	4
	NO: 62
GSTP1	SEQ ID	0.733	0.627	0.894	2.85E−32	1.74E−30	579E−31	4	4
	NO: 59
SLIT2	SEQ ID	0.756	0.779	0.72	9.67E−32	5.90E−30	1.47E−30	4	4
	NO: 112
CCND2	SEQ ID	0.732	0.724	0.745	4.10E−27	2.50E−25	5.00E−26	6	4
	NO: 104
HOXA5	SEQ ID	0.689	0.676	0.71	5.15E−24	3.14E−22	5.23E−23	4	2
	NO: 78
RASSF1A	SEQ ID	0.727	0.702	0.766	7.95E−24	4.85E−22	6.93E−23	3	3
	NO: 90
HS3ST2	SEQ ID	0.739	0.825	0.609	1.62E−22	9.90E−21	1.24E−21	2	2
	NO: 113
ARH1/NOEY2	SEQ ID	0.737	0.685	0.815	8.93E−20	5.45E−18	6.06.E−19	5	5
	NO: 97
SCGB3A1	SEQ ID	0.706	0.711	0.697	1.02E−18	6.19E−17	6.19E−18	4	1
	NO: 115
THBS1	SEQ ID	0.722	0.829	0.56	1.41E−18	8.59E−17	7.81E−18	4	3
	NO: 81
TIMP3	SEQ ID	0.667	0.623	0.735	3.62E−18	2.21E−16	1.84E−17	4	4
	NO: 103
IGSF4	SEQ ID	0.696	0.713	0.669	3.23E−17	1.97E−15	1.52E−16	4	2
	NO: 74
CDKN1A	SEQ ID	0.67	0.748	0.551	8.09E−17	4.93E−15	3.52E−16	4	1
	NO: 67
IGFBP7	SEQ ID	0.681	0.746	0.582	1.67E−16	1.02E−14	6.78E−16	5	3
	NO: 94
SYK	SEQ ID	0.685	0.678	0.694	5.57E−16	3.40E−14	2.12E−15	4	3
	NO: 60
HIC1	SEQ ID	0.645	0.707	0.55	6.28E−16	3.83E−14	2.25E−15	5	4
	NO: 85
TMS1/ASC	SEQ ID	0.673	0.765	0.533	2.40E−15	1.47E−13	8.15E−15	4	1
	NO: 84
TWIST	SEQ ID	0.659	0.771	0.487	3.17E−15	1.93E−13	9.99E−15	4	3
	NO: 100
APAF1	SEQ ID	0.656	0.65	0.665	3.27E−15	2.00E−13	9.99E−15	5	2
	NO: 82
THRB	SEQ ID	0.68	0.721	0.619	6.19E−15	3.78E−13	1.80E−14	4	1
	NO: 106
CDH13	SEQ ID	0.685	0.676	0.698	1.20E−14	7.33E−13	3.33E−14	4	3
	NO: 70
GJB2	SEQ ID	0.626	0.537	0.761	2.06E−14	1.26E−12	5.47E−14	4	1
	NO: 111
ALX4	SEQ ID	0.685	0.833	0.46	2.29E−14	1.40E−12	5.82E−14	4	3
	NO: 64
SERPINB5	SEQ ID	0.716	0.87	0.481	7.91E−14	4.82E−12	1.93E−13	3	3
	NO: 68
FABP3	SEQ ID	0.658	0.603	0.742	8.69E−13	5.30E−11	2.04E−12	4	3
	NO: 77
DAPK1	SEQ ID	0.65	0.764	0.478	2.40E−11	1.47E−09	5.43E−11	2	1
	NO: 98
FHIT	SEQ ID	0.63	0.6	0.675	5.00E−11	3.05E−09	1.09E−10	3	1
	NO: 76
MCT1	SEQ ID	0.667	0.743	0.552	1.37E−10	8.33E−09	2.87E−10	4	3
	NO: 101
APC	SEQ ID	0.595	0.431	0.844	6.33E−10	3.86E−08	1.29E−09	4	4
	NO: 65
CDKN2A	SEQ ID	0.614	0.479	0.819	6.73E−10	4.11E−08	1.32E−09	3	3
	NO: 57
EYA4	SEQ ID	0.627	0.803	0.358	2.35E−09	1.43E−07	4.48E−09	4	1
	NO: 58
S100A7	SEQ ID	0.658	0.627	0.704	5.32E−09	3.25E−07	9.84E−09	3	2
	NO: 96
GPC3	SEQ ID	0.623	0.653	0.578	1.17E−08	7.11E−07	2.09E−08	4	1
	NO: 118
SLC19A1	SEQ ID	0.603	0.598	0.61	2.17E−08	1.32E−06	3.78E−08	3	2
	NO: 116
SOD2	SEQ ID	0.632	0.657	0.592	4.55E−08	2.77E−06	7.71E−08	4	2
	NO: 105
ESR2	SEQ ID	0.544	0.337	0.857	6.27E−08	3.82E−06	1.03E−07	4	1
	NO: 91
LOT1	SEQ ID	0.605	0.594	0.621	4.53E−07	2.76E−05	7.28E−07	4	2
	NO: 95
SASH1	SEQ ID	0.613	0.619	0.605	4.76E−07	2.90E−05	7.45E−07	4	2
	NO: 102
TGFBR2	SEQ ID	0.609	0.554	0.692	4.89E−07	2.98E−05	7.46E−07	4	1
	NO: 93
CLDN7	SEQ ID	0.622	0.716	0.48	1.83E−06	1.11E−04	2.72E−06	4	1
	NO: 87
RARA	SEQ ID	0.564	0.483	0.686	5.30E−06	3.23E−04	7.70E−06	4	1
	NO: 108
IL6	SEQ ID	0.601	0.586	0.624	1.47E−05	8.98E−04	2.09E−05	4	0
	NO: 99
PRSS8	SEQ ID	0.558	0.595	0.502	3.66E−05	2.23E−03	5.07E−05	4	0
	NO: 72
CASP8	SEQ ID	0.579	0.53	0.653	3.98E−05	2.43E−03	5.40E−05	4	1
	NO: 71
SFN	SEQ ID	0.599	0.677	0.479	4.24E−05	2.58E−03	5.62E−05	4	1
	NO: 69
RARB	SEQ ID	0.549	0.474	0.662	4.61E−05	2.81E−03	5.98E−05	4	1
	NO: 88
NME1	SEQ ID	0.59	0.635	0.522	1.46E−04	8.91E−03	1.86E−04	4	1
	NO: 107
ELK1	SEQ ID	0.596	0.677	0.473	1.88E−04	1.15E−02	2.34E−04	5	0
	NO: 2
PGR	SEQ ID	0.592	0.63	0.532	7.29E−04	4.44E−02	8.89E−04	4	0
	NO: 83
BRCA1	SEQ ID	0.543	0.468	0.658	4.79E−03	2.92E−01	5.72E−03	4	0
	NO: 66
ESR1	SEQ ID	0.606	0.654	0.533	6.06E−03	3.69E−01	7.10E−03	3	1
	NO: 75
STAT1	SEQ ID	0.583	0.646	0.488	9.12E−03	5.56E−01	1.05E−02	4	0
	NO: 109
SNCG	SEQ ID	0.566	0.676	0.398	2.04E−02	1.00E+00	2.31E−02	4	0
	NO: 73
MLH1	SEQ ID	0.53	0.414	0.706	2.60E−02	1.00E+00	2.88E−02	4	0
	NO: 89
BRCA2	SEQ ID	0.565	0.567	0.562	3.43E−02	1.00E+00	3.74E−02	5	0
	NO: 56
TP73	SEQ ID	0.534	0.496	0.592	4.43E−02	1.00E+00	4.74E−02	4	0
	NO: 86
TERT	SEQ ID	0.537	0.5	0.592	1.16E−01	1.00E+00	1.22E−01	4	0
	NO: 92
TP53	SEQ ID	0.513	0.44	0.625	2.09E−01	1.00E+00	2.16E−01	4	0
	NO: 80
TPM1	SEQ ID	0.518	0.405	0.689	2.35E−01	1.00E+00	2.39E−01	4	0
	NO: 110
CDH1	SEQ ID	0.482	0.51	0.44	6.17E−01	1.00E+00	6.17E−01	5	0
	NO: 79

TABLE 5
Breast cancer vs. all other controls Chip 2
SEQ ID					P-value	P-value	n	n Significant
NO:	Accuracy	Sensitivity	Specificity	p-value	(Bonferroni)	FDR	Oligos	oligos
SEQ ID	0.773	0.764	0.786	1.02E−37	5.50E−36	5.50E−36	4	3
NO: 12
SEQ ID	0.777	0.821	0.712	1.01E−32	5.47E−31	2.73E−31	6	6
NO: 6
SEQ ID	0.754	0.73	0.789	3.11E−32	1.68E−30	5.60E−31	4	4
NO: 3
SEQ ID	0.722	0.7	0.754	1.43E−28	7.72E−27	1.93E−27	5	5
NO: 18
SEQ ID	0.753	0.824	0.65	2.18E−26	1.18E−24	2.36E−25	5	3
NO: 7
SEQ ID	0.74	0.797	0.658	3.97E−26	2.15E−24	3.58E−25	5	4
NO: 41
SEQ ID	0.726	0.677	0.796	1.87E−25	1.01E−23	1.44E−24	8	8
NO: 22
SEQ ID	0.727	0.74	0.707	2.74E−25	1.48E−23	1.85E−24	4	4
NO: 46
SEQ ID	0.681	0.622	0.767	6.60E−22	3.56E−20	3.96E−21	4	3
NO: 13
SEQ ID	0.69	0.647	0.753	1.06E−21	5.74E−20	5.74E−21	5	5
NO: 31
SEQ ID	0.695	0.684	0.711	4.06E−21	2.19E−19	1.99E−20	5	2
NO: 34
SEQ ID	0.714	0.702	0.733	1.58E−20	8.52E−19	7.10E−20	4	3
NO: 27
SEQ ID	0.697	0.816	0.521	3.12E−20	1.69E−18	1.30E−19	9	8
NO: 10
SEQ ID	0.69	0.818	0.502	9.42E−20	5.09E−18	3.63E−19	5	3
NO: 38
SEQ ID	0.684	0.745	0.593	1.06E−19	5.74E−18	3.83E−19	4	3
NO: 47
SEQ ID	0.703	0.716	0.683	1.39E−19	7.49E−18	4.68E−19	4	4
NO: 117
SEQ ID	0.723	0.746	0.69	1.47E−19	7.95E−18	4.68E−19	4	4
NO: 48
SEQ ID	0.695	0.586	0.855	7.60E−19	4.10E−17	2.28E−18	4	4
NO: 30
SEQ ID	0.692	0.641	0.766	1.66E−18	8.95E−17	4.71E−18	4	3
NO: 4
SEQ ID	0.678	0.695	0.654	1.70E−17	9.16E−16	4.58E−17	4	4
NO: 39
SEQ ID	0.683	0.741	0.598	1.83E−17	9.88E−16	4.70E−17	5	4
NO: 1
SEQ ID	0.686	0.78	0.549	8.08E−16	4.37E−14	1.98E−15	4	4
NO: 35
SEQ ID	0.697	0.687	0.711	1.66E−15	8.97E−14	3.90E−15	4	1
NO: 43
SEQ ID	0.659	0.597	0.75	1.15E−14	6.21E−13	2.59E−14	5	2
NO: 54
SEQ ID	0.657	0.648	0.67	3.14E−14	1.70E−12	6.79E−14	5	2
NO: 25
SEQ ID	0.667	0.648	0.695	6.97E−14	3.76E−12	1.45E−13	4	2
NO: 42
SEQ ID	0.684	0.727	0.621	1.53E−13	8.25E−12	3.05E−13	5	3
NO: 29
SEQ ID	0.642	0.704	0.551	1.74E−13	9.38E−12	3.35E−13	4	1
NO: 2
SEQ ID	0.631	0.623	0.643	4.22E−12	2.28E−10	7.85E−12	3	1
NO: 32
SEQ ID	0.64	0.609	0.686	6.07E−12	3.28E−10	1.07E−11	3	1
NO: 23
SEQ ID	0.652	0.64	0.67	6.12E−12	3.30E−10	1.07E−11	4	4
NO: 11
SEQ ID	0.631	0.614	0.655	8.28E−11	4.47E−09	1.40E−10	5	2
NO: 16
SEQ ID	0.643	0.652	0.631	1.68E−10	9.09E−09	2.75E−10	5	1
NO: 17
SEQ ID	0.639	0.613	0.677	3.66E−10	1.97E−08	5.81E−10	7	2
NO: 28
SEQ ID	0.615	0.524	0.749	8.46E−10	4.57E−08	1.31E−09	4	1
NO: 51
SEQ ID	0.595	0.539	0.677	2.07E−09	1.12E−07	3.11E−09	4	1
NO: 19
SEQ ID	0.626	0.806	0.363	2.96E−09	1.60E−07	4.32E−09	4	1
NO: 20
SEQ ID	0.607	0.496	0.769	8.74E−09	4.72E−07	1.24E−08	3	1
NO: 14
SEQ ID	0.614	0.505	0.774	6.78E−08	3.66E−06	9.39E−08	5	3
NO: 24
SEQ ID	0.598	0.468	0.789	1.33E−07	7.20E−06	1.80E−07	3	0
NO: 33
SEQ ID	0.599	0.5	0.743	2.21E−07	1.19E−05	2.90E−07	5	2
NO: 50
SEQ ID	0.644	0.75	0.489	1.03E−06	5.57E−05	1.33E−06	3	1
NO: 26
SEQ ID	0.597	0.668	0.492	1.15E−05	6.21E−04	1.44E−05	5	0
NO: 15
SEQ ID	0.6	0.569	0.646	1.78E−05	9.59E−04	2.18E−05	5	1
NO: 40
SEQ ID	0.582	0.635	0.504	2.43E−05	1.31E−03	2.91E−05	3	1
NO: 37
SEQ ID	0.603	0.538	0.698	3.25E−05	1.75E−03	3.81E−05	5	1
NO: 9
SEQ ID	0.592	0.613	0.561	5.90E−05	3.18E−03	6.77E−05	5	3
NO: 5
SEQ ID	0.64	0.863	0.315	1.41E−04	7.61E−03	1.59E−04	5	0
NO: 8
SEQ ID	0.606	0.695	0.475	1.72E−03	9.31E−02	1.90E−03	4	0
NO: 52
SEQ ID	0.57	0.516	0.649	1.14E−02	6.14E−01	1.23E−02	4	0
NO: 21
SEQ ID	0.521	0.54	0.493	2.59E−02	1.00E+00	2.74E−02	4	0
NO: 36
SEQ ID	0.514	0.332	0.78	2.98E−02	1.00E+00	3.09E−02	5	0
NO: 55
SEQ ID	0.553	0.65	0.411	6.73E−02	1.00E+00	6.86E−02	4	0
NO: 45
SEQ ID	0.496	0.402	0.632	5.14E−01	1.00E+00	5.14E−01	2	0
NO: 44

TABLE 6
Breast cancer vs. other cancer Chip 1
	SEQ ID					P-value	P-value	n	n Significant
Gene Name	NO:	Accuracy	Sensitivity	Specificity	p-value	(Bonferroni)	FDR	Oligos	oligos
PRDM2	SEQ ID	0.852	0.897	0.687	8.85E−26	5.40E−24	5.40E−24	4	1
	NO: 114
GSTP1	SEQ ID	0.686	0.638	0.862	2.40E−14	1.47E−12	7.34E−13	4	4
	NO: 59
ALX4	SEQ ID	0.77	0.821	0.583	4.88E−14	2.98E−12	9.92E−13	4	3
	NO: 64
HOXA5	SEQ ID	0.689	0.683	0.708	8.11E−13	4.95E−11	1.24E−11	4	2
	NO: 78
PLAU	SEQ ID	0.693	0.707	0.642	2.29E−12	1.40E−10	2.80E−11	4	3
	NO: 62
RASSF1A	SEQ ID	0.714	0.721	0.689	1.10E−10	6.68E−09	1.11E−09	3	3
	NO: 90
IGSF4	SEQ ID	0.716	0.735	0.644	2.13E−10	1.30E−08	1.86E−09	4	1
	NO: 74
SLIT2	SEQ ID	0.674	0.726	0.479	5.43E−10	3.31E−08	4.14E−09	4	2
	NO: 112
DAPK1	SEQ ID	0.713	0.757	0.549	1.05E−09	6.41E−08	7.13E−09	2	1
	NO: 98
CDKN1A	SEQ ID	0.693	0.725	0.576	1.34E−09	8.17E−08	8.17E−09	4	1
	NO: 67
IGFBP7	SEQ ID	0.7	0.702	0.693	2.79E−09	1.70E−07	1.55E−08	5	3
	NO: 94
THBS1	SEQ ID	0.735	0.791	0.528	4.76E−09	2.90E−07	2.42E−08	4	3
	NO: 81
CCND2	SEQ ID	0.688	0.707	0.617	3.74E−08	2.28E−06	1.75E−07	6	2
	NO: 104
APAF1	SEQ ID	0.631	0.632	0.628	1.20E−07	7.34E−06	5.25E−07	5	2
	NO: 82
EYA4	SEQ ID	0.719	0.748	0.613	1.82E−07	1.11E−05	7.40E−07	4	2
	NO: 58
SCGB3A1	SEQ ID	0.649	0.671	0.568	2.56E−07	1.56E−05	9.25E−07	4	1
	NO: 115
SYK	SEQ ID	0.647	0.653	0.625	2.65E−07	1.62E−05	9.25E−07	4	2
	NO: 60
HIC1	SEQ ID	0.654	0.69	0.524	2.73E−07	1.67E−05	9.25E−07	5	2
	NO: 85
CDH13	SEQ ID	0.573	0.503	0.831	3.52E−07	2.15E−05	1.13E−06	4	0
	NO: 70
TIMP3	SEQ ID	0.619	0.617	0.627	1.45E−06	8.84E−05	4.42E−06	4	3
	NO: 103
LOT1	SEQ ID	0.632	0.626	0.652	1.57E−06	9.56E−05	4.55E−06	4	1
	NO: 95
THRB	SEQ ID	0.723	0.776	0.53	1.89E−06	1.15E−04	5.24E−06	4	1
	NO: 106
TMS1/ASC	SEQ ID	0.702	0.781	0.411	2.77E−06	1.69E−04	7.34E−06	4	1
	NO: 84
IL6	SEQ ID	0.654	0.669	0.596	1.69E−05	1.03E−03	4.30E−05	4	1
	NO: 99
TWIST	SEQ ID	0.696	0.755	0.479	1.92E−05	1.17E−03	4.69E−05	4	2
	NO: 100
CLDN7	SEQ ID	0.63	0.67	0.482	3.67E−04	2.24E−02	8.62E−04	4	0
	NO: 87
FHIT	SEQ ID	0.601	0.613	0.556	7.43E−04	4.53E−02	1.63E−03	3	0
	NO: 76
ARH1/NOEY2	SEQ ID	0.634	0.646	0.587	7.50E−04	4.57E−02	1.63E−03	5	2
	NO: 97
PGR	SEQ ID	0.649	0.642	0.673	1.34E−03	8.17E−02	2.82E−03	4	0
	NO: 83
NME1	SEQ ID	0.588	0.597	0.556	2.10E−03	1.28E−01	4.27E−03	4	1
	NO: 107
SERPINB5	SEQ ID	0.665	0.709	0.503	3.24E−03	1.98E−01	6.38E−03	3	0
	NO: 68
GPC3	SEQ ID	0.619	0.651	0.503	3.42E−03	2.09E−01	6.52E−03	4	0
	NO: 118
ESR2	SEQ ID	0.395	0.267	0.869	3.53E−03	2.15E−01	6.53E−03	4	0
	NO: 91
MCT1	SEQ ID	0.713	0.818	0.321	9.75E−03	5.95E−01	1.75E−02	4	0
	NO: 101
HS3ST2	SEQ ID	0.749	0.892	0.22	1.07E−02	6.54E−01	1.84E−02	2	0
	NO: 113
GJB2	SEQ ID	0.543	0.516	0.642	1.08E−02	6.62E−01	1.84E−02	4	0
	NO: 111
ELK1	SEQ ID	0.603	0.634	0.49	2.21E−02	1.00E+00	3.61E−02	5	0
	NO: 2
STAT1	SEQ ID	0.618	0.651	0.496	2.25E−02	1.00E+00	3.61E−02	4	0
	NO: 109
TGFBR2	SEQ ID	0.608	0.669	0.382	2.34E−02	1.00E+00	3.66E−02	4	0
	NO: 93
TERT	SEQ ID	0.552	0.549	0.566	2.41E−02	1.00E+00	3.67E−02	4	0
	NO: 92
PRSS8	SEQ ID	0.578	0.592	0.525	4.66E−02	1.00E+00	6.93E−02	4	0
	NO: 72
SOD2	SEQ ID	0.587	0.602	0.534	6.76E−02	1.00E+00	9.82E−02	4	0
	NO: 105
S100A7	SEQ ID	0.568	0.594	0.47	7.29E−02	1.00E+00	1.03E−01	3	0
	NO: 96
FABP3	SEQ ID	0.504	0.466	0.648	7.78E−02	1.00E+00	1.08E−01	4	0
	NO: 77
SFN	SEQ ID	0.597	0.637	0.448	8.88E−02	1.00E+00	1.18E−01	4	0
	NO: 69
RARA	SEQ ID	0.442	0.369	0.711	8.97E−02	1.00E+00	1.18E−01	4	0
	NO: 108
CDH1	SEQ ID	0.539	0.559	0.463	9.06E−02	1.00E+00	1.18E−01	5	0
	NO: 79
APC	SEQ ID	0.578	0.605	0.476	1.21E−01	1.00E+00	1.54E−01	4	0
	NO: 65
BRCA2	SEQ ID	0.577	0.585	0.546	1.26E−01	1.00E+00	1.57E−01	5	0
	NO: 56
SASH1	SEQ ID	0.548	0.553	0.53	1.58E−01	1.00E+00	1.93E−01	4	0
	NO: 102
CASP8	SEQ ID	0.534	0.533	0.534	1.63E−01	1.00E+00	1.95E−01	4	0
	NO: 71
CDKN2A	SEQ ID	0.487	0.448	0.632	1.74E−01	1.00E+00	2.04E−01	3	0
	NO: 57
ESR1	SEQ ID	0.602	0.654	0.408	2.14E−01	1.00E+00	2.47E−01	3	0
	NO: 75
RARB	SEQ ID	0.577	0.622	0.413	2.61E−01	1.00E+00	2.95E−01	4	0
	NO: 88
SNCG	SEQ ID	0.573	0.635	0.342	3.53E−01	1.00E+00	3.92E−01	4	0
	NO: 73
BRCA1	SEQ ID	0.421	0.362	0.642	3.69E−01	1.00E+00	4.02E−01	4	0
	NO: 66
SLC19A1	SEQ ID	0.455	0.437	0.523	4.30E−01	1.00E+00	4.60E−01	3	0
	NO: 116
TP73	SEQ ID	0.484	0.463	0.559	5.24E−01	1.00E+00	5.51E−01	4	0
	NO: 86
TP53	SEQ ID	0.472	0.463	0.503	6.77E−01	1.00E+00	7.00E−01	4	0
	NO: 80
MLH1	SEQ ID	0.56	0.621	0.332	7.29E−01	1.00E+00	7.42E−01	4	0
	NO: 89
TPM1	SEQ ID	0.514	0.554	0.369	8.30E−01	1.00E+00	8.30E−01	4	0
	NO: 110

TABLE 7
Breast cancer vs. other cancer Chip 2
SEQ ID					P-value	P-value		n Significant
NO:	Accuracy	Sensitivity	Specificity	P-value	(Bonferroni)	FDR	n Oligos	oligos
SEQ ID	0.75	0.775	0.662	1.91E−14	1.03E−12	1.03E−12	5	4
NO: 38
SEQ ID	0.73	0.771	0.592	5.32E−13	2.87E−11	1.44E−11	4	4
NO: 35
SEQ ID	0.74	0.784	0.577	5.86E−12	3.17E−10	1.01E−10	4	3
NO: 12
SEQ ID	0.71	0.733	0.626	7.49E−12	4.05E−10	1.01E−10	4	4
NO: 39
SEQ ID	0.79	0.886	0.455	9.63E−11	5.20E−09	1.04E−09	9	5
NO: 10
SEQ ID	0.74	0.773	0.623	1.88E−10	1.01E−08	1.69E−09	3	3
NO: 26
SEQ ID	0.64	0.616	0.716	2.30E−10	1.24E−08	1.77E−09	5	5
NO: 8
SEQ ID	0.69	0.692	0.681	6.56E−10	3.54E−08	4.43E−09	8	6
NO: 22
SEQ ID	0.67	0.664	0.692	1.53E−09	8.24E−08	9.15E−09	5	2
NO: 18
SEQ ID	0.73	0.788	0.534	4.22E−09	2.28E−07	2.22E−08	4	1
NO: 47
SEQ ID	0.73	0.745	0.677	4.53E−09	2.44E−07	2.22E−08	5	3
NO: 5
SEQ ID	0.65	0.642	0.666	6.75E−09	3.65E−07	3.04E−08	4	2
NO: 3
SEQ ID	0.67	0.69	0.578	1.35E−08	7.29E−07	5.61E−08	5	2
NO: 1
SEQ ID	0.68	0.726	0.523	1.25E−06	6.76E−05	4.83E−06	6	2
NO: 6
SEQ ID	0.72	0.744	0.656	1.44E−06	7.76E−05	5.17E−06	5	1
NO: 41
SEQ ID	0.66	0.677	0.581	3.97E−06	2.15E−04	1.34E−05	3	1
NO: 33
SEQ ID	0.59	0.573	0.64	1.19E−05	6.44E−04	3.79E−05	4	2
NO: 13
SEQ ID	0.65	0.716	0.438	1.62E−05	8.72E−04	4.85E−05	4	0
NO: 2
SEQ ID	0.63	0.628	0.629	1.72E−05	9.26E−04	4.88E−05	5	1
NO: 25
SEQ ID	0.61	0.578	0.704	3.32E−05	1.79E−03	8.95E−05	5	1
NO: 54
SEQ ID	0.59	0.55	0.725	1.21E−04	6.55E−03	3.12E−04	4	4
NO: 30
SEQ ID	0.65	0.659	0.596	1.37E−04	7.39E−03	3.36E−04	3	1
NO: 32
SEQ ID	0.59	0.578	0.642	1.44E−04	7.75E−03	3.37E−04	5	1
NO: 31
SEQ ID	0.6	0.6	0.614	1.89E−04	1.02E−02	4.26E−04	3	0
NO: 23
SEQ ID	0.66	0.682	0.56	7.24E−04	3.91E−02	1.56E−03	5	0
NO: 34
SEQ ID	0.69	0.746	0.501	9.60E−04	5.18E−02	1.99E−03	4	1
NO: 48
SEQ ID	0.62	0.631	0.563	1.38E−03	7.44E−02	2.76E−03	4	0
NO: 27
SEQ ID	0.59	0.572	0.652	1.84E−03	9.95E−02	3.55E−03	7	1
NO: 28
SEQ ID	0.61	0.648	0.456	2.91E−03	1.57E−01	5.42E−03	5	0
NO: 7
SEQ ID	0.63	0.676	0.449	3.05E−03	1.65E−01	5.49E−03	4	0
NO: 42
SEQ ID	0.59	0.6	0.555	3.41E−03	1.84E−01	5.94E−03	3	0
NO: 37
SEQ ID	0.55	0.544	0.548	6.25E−03	3.37E−01	1.05E−02	4	0
NO: 19
SEQ ID	0.54	0.526	0.592	6.73E−03	3.63E−01	1.10E−02	4	0
NO: 46
SEQ ID	0.59	0.635	0.415	7.70E−03	4.16E−01	1.22E−02	5	0
NO: 29
SEQ ID	0.6	0.63	0.477	7.88E−03	4.26E−01	1.22E−02	4	0
NO: 20
SEQ ID	0.61	0.635	0.523	8.17E−03	4.41E−01	1.23E−02	5	0
NO: 17
SEQ ID	0.58	0.584	0.56	9.05E−03	4.89E−01	1.32E−02	5	0
NO: 16
SEQ ID	0.62	0.655	0.515	1.27E−02	6.88E−01	1.81E−02	4	0
NO: 45
SEQ ID	0.55	0.523	0.632	2.94E−02	1.00E+00	4.07E−02	4	0
NO: 4
SEQ ID	0.48	0.411	0.73	3.58E−02	1.00E+00	4.83E−02	3	0
NO: 14
SEQ ID	0.56	0.564	0.552	3.73E−02	1.00E+00	4.91E−02	5	0
NO: 15
SEQ ID	0.54	0.525	0.581	4.70E−02	1.00E+00	6.04E−02	4	0
NO: 43
SEQ ID	0.54	0.564	0.467	7.94E−02	1.00E+00	9.97E−02	5	0
NO: 40
SEQ ID	0.56	0.596	0.438	1.26E−01	1.00E+00	1.54E−01	4	0
NO: 11
SEQ ID	0.56	0.591	0.473	1.32E−01	1.00E+00	1.58E−01	5	0
NO: 9
SEQ ID	0.54	0.558	0.471	1.42E−01	1.00E+00	1.66E−01	4	0
NO: 36
SEQ ID	0.54	0.526	0.568	1.46E−01	1.00E+00	1.68E−01	4	0
NO: 117
SEQ ID	0.55	0.568	0.473	3.06E−01	1.00E+00	3.45E−01	5	0
NO: 55
SEQ ID	0.55	0.586	0.408	3.77E−01	1.00E+00	4.15E−01	4	0
NO: 51
SEQ ID	0.47	0.437	0.574	4.14E−01	1.00E+00	4.47E−01	5	0
NO: 50
SEQ ID	0.48	0.451	0.59	4.40E−01	1.00E+00	4.66E−01	4	0
NO: 21
SEQ ID	0.48	0.421	0.663	4.94E−01	1.00E+00	5.13E−01	5	0
NO: 24
SEQ ID	0.48	0.448	0.589	5.90E−01	1.00E+00	6.01E−01	4	0
NO: 52
SEQ ID	0.56	0.618	0.344	9.16E−01	1.00E+00	9.16E−01	2	0
NO: 44

TABLE 8
Breast cancer vs. lymphocytes Chip 1
									n
	SEQ ID					P-value	P-value	n	Significant
Gene Name	NO:	Accuracy	Sensitivity	Specificity	p-value	(Bonferroni)	FDR	Oligos	oligos
EYA4	SEQ ID	1	1	1	9.16E−39	5.59E−37	3.76E−37	4	4
	NO: 58
PRDM2	SEQ ID	0.984	0.985	0.971	1.23E−38	7.52E−37	3.76E−37	4	4
	NO: 114
SERPINB5	SEQ ID	0.986	0.984	0.996	3.96E−37	2.42E−35	8.05E−36	3	3
	NO: 68
TWIST	SEQ ID	0.962	0.962	0.964	8.80E−34	5.37E−32	1.34E−32	4	4
	NO: 100
STAT1	SEQ ID	0.97	0.973	0.936	9.90E−32	6.04E−30	1.21E−30	4	1
	NO: 109
ALX4	SEQ ID	0.949	0.953	0.911	2.21E−31	1.35E−29	2.24E−30	4	3
	NO: 64
IGFBP7	SEQ ID	0.941	0.941	0.939	1.24E−28	7.58E−27	1.08E−27	5	4
	NO: 94
DAPK1	SEQ ID	0.905	0.9	0.954	3.26E−26	1.99E−24	2.49E−25	2	1
	NO: 98
THBS1	SEQ ID	0.93	0.934	0.889	2.02E−25	1.23E−23	1.37E−24	4	2
	NO: 81
PLAU	SEQ ID	0.923	0.927	0.882	3.43E−24	2.09E−22	2.09E−23	4	3
	NO: 62
PRSS8	SEQ ID	0.871	0.881	0.775	2.25E−22	1.37E−20	1.25E−21	4	2
	NO: 72
S100A7	SEQ ID	0.886	0.879	0.95	3.83E−21	2.34E−19	1.95E−20	3	3
	NO: 96
SFN	SEQ ID	0.88	0.882	0.861	9.22E−20	5.62E−18	4.33E−19	4	3
	NO: 69
NME1	SEQ ID	0.807	0.802	0.854	1.53E−18	9.34E−17	6.67E−18	4	4
	NO: 107
SLIT2	SEQ ID	0.848	0.847	0.854	1.76E−18	1.08E−16	7.17E−18	4	4
	NO: 112
CDKN1A	SEQ ID	0.877	0.881	0.846	5.07E−18	3.09E−16	1.93E−17	4	1
	NO: 67
LOT1	SEQ ID	0.819	0.819	0.818	8.85E−17	5.40E−15	3.18E−16	4	3
	NO: 95
HOXA5	SEQ ID	0.808	0.807	0.821	4.95E−16	3.02E−14	1.68E−15	4	2
	NO: 78
CCND2	SEQ ID	0.822	0.822	0.825	7.82E−15	4.77E−13	2.51E−14	6	4
	NO: 104
IGSF4	SEQ ID	0.864	0.878	0.732	3.82E−14	2.33E−12	1.17E−13	4	1
	NO: 74
SCGB3A1	SEQ ID	0.807	0.798	0.886	4.11E−14	2.51E−12	1.19E−13	4	2
	NO: 115
RASSF1A	SEQ ID	0.759	0.74	0.939	4.74E−14	2.89E−12	1.31E−13	3	3
	NO: 90
HIC1	SEQ ID	0.856	0.867	0.754	5.66E−14	3.45E−12	1.50E−13	5	4
	NO: 85
GPC3	SEQ ID	0.771	0.768	0.793	1.27E−13	7.76E−12	3.23E−13	4	1
	NO: 118
SNCG	SEQ ID	0.793	0.781	0.914	7.47E−13	4.56E−11	1.82E−12	4	4
	NO: 73
APC	SEQ ID	0.769	0.761	0.846	8.49E−13	5.18E−11	1.99E−12	4	3
	NO: 65
GSTP1	SEQ ID	0.747	0.738	0.832	3.71E−12	2.26E−10	8.38E−12	4	3
	NO: 59
MCT1	SEQ ID	0.819	0.817	0.832	5.61E−12	3.42E−10	1.22E−11	4	2
	NO: 101
SLC19A1	SEQ ID	0.754	0.756	0.736	9.04E−12	5.52E−10	1.90E−11	3	2
	NO: 116
IL6	SEQ ID	0.807	0.81	0.786	1.08E−11	6.57E−10	2.19E−11	4	1
	NO: 99
HS3ST2	SEQ ID	0.776	0.774	0.793	5.22E−11	3.18E−09	1.03E−10	2	2
	NO: 113
FABP3	SEQ ID	0.753	0.752	0.761	1.73E−10	1.06E−08	3.30E−10	4	2
	NO: 77
SOD2	SEQ ID	0.777	0.787	0.686	5.83E−09	3.56E−07	1.08E−08	4	1
	NO: 105
THRB	SEQ ID	0.797	0.824	0.539	2.75E−08	1.67E−06	4.93E−08	4	1
	NO: 106
CDH13	SEQ ID	0.701	0.689	0.821	3.44E−08	2.10E−06	5.99E−08	4	4
	NO: 70
GJB2	SEQ ID	0.633	0.612	0.825	4.24E−08	2.58E−06	7.18E−08	4	1
	NO: 111
APAF1	SEQ ID	0.723	0.725	0.696	6.25E−08	3.81E−06	1.03E−07	5	1
	NO: 82
CLDN7	SEQ ID	0.728	0.73	0.704	1.66E−06	1.01E−04	2.66E−06	4	1
	NO: 87
ARH1/NOEY2	SEQ ID	0.713	0.699	0.843	2.18E−06	1.33E−04	3.41E−06	5	3
	NO: 97
SYK	SEQ ID	0.712	0.705	0.771	4.91E−06	2.99E−04	7.48E−06	4	2
	NO: 60
ESR1	SEQ ID	0.686	0.672	0.821	5.17E−06	3.15E−04	7.69E−06	3	1
	NO: 75
ELK1	SEQ ID	0.848	0.907	0.296	6.48E−06	3.95E−04	9.41E−06	5	0
	NO: 2
PGR	SEQ ID	0.757	0.77	0.632	9.28E−06	5.66E−04	1.32E−05	4	1
	NO: 83
FHIT	SEQ ID	0.665	0.663	0.686	3.60E−05	2.19E−03	4.99E−05	3	0
	NO: 76
TGFBR2	SEQ ID	0.634	0.634	0.639	4.05E−05	2.47E−03	5.49E−05	4	1
	NO: 93
TIMP3	SEQ ID	0.737	0.738	0.729	8.00E−05	4.88E−03	1.06E−04	4	1
	NO: 103
TERT	SEQ ID	0.626	0.615	0.725	9.27E−05	5.66E−03	1.20E−04	4	0
	NO: 92
TMS1/ASC	SEQ ID	0.746	0.777	0.454	2.42E−04	1.48E−02	3.08E−04	4	1
	NO: 84
CDKN2A	SEQ ID	0.718	0.714	0.761	7.51E−04	4.58E−02	9.35E−04	3	2
	NO: 57
SASH1	SEQ ID	0.61	0.601	0.7	2.93E−03	1.79E−01	3.57E−03	4	0
	NO: 102
BRCA1	SEQ ID	0.602	0.603	0.589	3.54E−03	2.16E−01	4.23E−03	4	0
	NO: 66
CASP8	SEQ ID	0.678	0.685	0.607	5.31E−03	3.24E−01	6.23E−03	4	0
	NO: 71
CDH1	SEQ ID	0.653	0.649	0.689	6.12E−03	3.73E−01	7.04E−03	5	0
	NO: 79
RARB	SEQ ID	0.493	0.471	0.704	1.43E−02	8.73E−01	1.62E−02	4	0
	NO: 88
ESR2	SEQ ID	0.504	0.484	0.7	1.79E−02	1.00E+00	1.99E−02	4	0
	NO: 91
TPM1	SEQ ID	0.556	0.538	0.718	1.30E−01	1.00E+00	1.42E−01	4	0
	NO: 110
RARA	SEQ ID	0.498	0.498	0.5	1.44E−01	1.00E+00	1.55E−01	4	0
	NO: 108
TP73	SEQ ID	0.521	0.524	0.489	3.04E−01	1.00E+00	3.20E−01	4	0
	NO: 86
BRCA2	SEQ ID	0.611	0.636	0.375	3.85E−01	1.00E+00	3.98E−01	5	0
	NO: 56
TP53	SEQ ID	0.583	0.6	0.425	3.95E−01	1.00E+00	3.98E−01	4	0
	NO: 80
MLH1	SEQ ID	0.471	0.467	0.507	3.98E−01	1.00E+00	3.98E−01	4	0
	NO: 89

TABLE 9
Breast cancer vs. lymphocytes Chip 2
SEQ ID					P-value	P-value		n Significant
NO:	Accuracy	Sensitivity	Specificity	P-value	(Bonferroni)	FDR	n Oligos	oligos
SEQ ID	0.997	0.998	0.985	3.34E−44	1.81E−42	1.81E−42	4	4
NO: 20
SEQ ID	0.992	0.997	0.953	2.65E−43	1.43E−41	7.16E−42	5	4
NO: 38
SEQ ID	0.981	0.985	0.95	1.18E−42	6.39E−41	1.86E−41	5	4
NO: 8
SEQ ID	0.992	0.995	0.976	1.38E−42	7.45E−41	1.86E−41	3	3
NO: 37
SEQ ID	0.977	0.986	0.909	4.54E−40	2.45E−38	4.91E−39	9	8
NO: 10
SEQ ID	0.964	0.97	0.926	1.48E−37	7.98E−36	1.33E−36	4	4
NO: 35
SEQ ID	0.963	0.968	0.926	2.48E−36	1.34E−34	1.91E−35	4	3
NO: 47
SEQ ID	0.936	0.942	0.894	6.90E−34	3.72E−32	4.65E−33	6	6
NO: 6
SEQ ID	0.922	0.92	0.935	6.99E−32	3.77E−30	4.19E−31	4	3
NO: 12
SEQ ID	0.922	0.927	0.882	5.28E−30	2.85E−28	2.85E−29	4	4
NO: 46
SEQ ID	0.915	0.917	0.903	2.25E−29	1.21E−27	1.10E−28	5	5
NO: 1
SEQ ID	0.919	0.916	0.935	3.12E−29	1.68E−27	1.40E−28	5	4
NO: 41
SEQ ID	0.93	0.927	0.95	4.54E−29	2.45E−27	1.88E−28	8	7
NO: 22
SEQ ID	0.902	0.894	0.968	1.16E−28	6.28E−27	4.48E−28	3	3
NO: 26
SEQ ID	0.901	0.897	0.929	2.78E−28	1.50E−26	1.00E−27	5	3
NO: 7
SEQ ID	0.883	0.882	0.888	1.97E−27	1.06E−25	6.39E−27	5	4
NO: 15
SEQ ID	0.887	0.877	0.965	2.01E−27	1.09E−25	6.39E−27	5	2
NO: 29
SEQ ID	0.89	0.892	0.871	2.51E−25	1.35E−23	7.52E−25	5	4
NO: 18
SEQ ID	0.877	0.879	0.856	4.95E−25	2.68E−23	1.41E−24	5	2
NO: 34
SEQ ID	0.864	0.856	0.921	4.95E−24	2.67E−22	1.34E−23	5	2
NO: 25
SEQ ID	0.857	0.856	0.862	1.17E−23	6.31E−22	3.01E−23	5	3
NO: 16
SEQ ID	0.852	0.85	0.868	2.85E−22	1.54E−20	7.01E−22	4	2
NO: 2
SEQ ID	0.83	0.825	0.865	5.73E−20	3.10E−18	1.35E−19	4	4
NO: 117
SEQ ID	0.829	0.826	0.85	1.05E−18	5.66E−17	2.36E−18	4	4
NO: 3
SEQ ID	0.822	0.817	0.856	1.20E−18	6.48E−17	2.59E−18	4	4
NO: 48
SEQ ID	0.824	0.818	0.871	2.48E−17	1.34E−15	5.15E−17	4	3
NO: 4
SEQ ID	0.801	0.805	0.771	3.41E−16	1.84E−14	6.69E−16	4	4
NO: 11
SEQ ID	0.853	0.845	0.915	3.47E−16	1.87E−14	6.69E−16	5	4
NO: 5
SEQ ID	0.757	0.745	0.844	1.83E−15	9.91E−14	3.42E−15	5	2
NO: 54
SEQ ID	0.742	0.728	0.844	6.80E−15	3.67E−13	1.22E−14	4	3
NO: 13
SEQ ID	0.783	0.774	0.856	1.57E−13	8.48E−12	2.74E−13	4	1
NO: 43
SEQ ID	0.777	0.772	0.809	1.77E−13	9.57E−12	2.99E−13	5	5
NO: 31
SEQ ID	0.783	0.766	0.906	2.28E−12	1.23E−10	3.73E−12	7	1
NO: 28
SEQ ID	0.744	0.752	0.691	2.54E−11	1.37E−09	4.04E−11	3	1
NO: 32
SEQ ID	0.753	0.742	0.832	4.05E−11	2.19E−09	6.25E−11	4	3
NO: 27
SEQ ID	0.702	0.698	0.738	1.12E−09	6.07E−08	1.68E−09	3	1
NO: 23
SEQ ID	0.757	0.753	0.782	1.15E−09	6.21E−08	1.68E−09	4	1
NO: 42
SEQ ID	0.654	0.634	0.803	1.35E−09	7.28E−08	1.92E−09	4	2
NO: 51
SEQ ID	0.714	0.713	0.721	2.47E−08	1.33E−06	3.41E−08	5	1
NO: 17
SEQ ID	0.713	0.728	0.603	6.09E−08	3.29E−06	8.22E−08	4	2
NO: 52
SEQ ID	0.656	0.623	0.906	7.96E−08	4.30E−06	1.05E−07	4	4
NO: 30
SEQ ID	0.643	0.608	0.903	1.26E−07	6.79E−06	1.62E−07	5	2
NO: 24
SEQ ID	0.684	0.683	0.688	7.22E−07	3.90E−05	9.07E−07	5	1
NO: 40
SEQ ID	0.63	0.609	0.791	9.04E−07	4.88E−05	1.11E−06	5	2
NO: 50
SEQ ID	0.667	0.664	0.685	1.55E−06	8.36E−05	1.86E−06	4	1
NO: 19
SEQ ID	0.617	0.597	0.765	8.69E−06	4.69E−04	1.02E−05	4	1
NO: 21
SEQ ID	0.597	0.575	0.762	1.12E−04	6.04E−03	1.29E−04	3	1
NO: 14
SEQ ID	0.603	0.579	0.785	1.35E−03	7.29E−02	1.52E−03	5	0
NO: 9
SEQ ID	0.481	0.45	0.721	1.01E−02	5.47E−01	1.12E−02	3	0
NO: 33
SEQ ID	0.588	0.583	0.626	1.21E−02	6.52E−01	1.30E−02	4	0
NO: 39
SEQ ID	0.472	0.445	0.674	1.94E−02	1.00E+00	2.06E−02	5	0
NO: 55
SEQ ID	0.596	0.595	0.603	2.85E−02	1.00E+00	2.96E−02	4	0
NO: 36
SEQ ID	0.501	0.509	0.444	3.22E−01	1.00E+00	3.29E−01	4	0
NO: 45
SEQ ID	0.343	0.309	0.606	8.51E−01	1.00E+00	8.51E−01	2	0
NO: 44

TABLE 10
DCIS vs. benign breast conditions Chip 1
	SEQ ID					P-value	P-value		n Significant
Gene Name	NO:	Accuracy	Sensitivity	Specificity	p-value	(Bonferroni)	FDR	n Oligos	oligos
HS3ST2	SEQ ID	0.88	0.795	0.905	1.10E−13	6.73E−12	6.73E−12	2	2
	NO: 113
SL1T2	SEQ ID	0.86	0.845	0.864	2.28E−13	1.39E−11	6.95E−12	4	4
	NO: 112
RASSF1A	SEQ ID	0.88	0.877	0.882	3.27E−12	2.00E−10	6.65E−11	3	3
	NO: 90
GSTP1	SEQ ID	0.88	0.691	0.942	3.25E−11	1.98E−09	4.96E−10	4	3
	NO: 59
GJB2	SEQ ID	0.82	0.732	0.843	1.17E−09	7.15E−08	1.43E−08	4	1
	NO: 111
IGFBP7	SEQ ID	0.84	0.786	0.861	1.48E−09	9.01E−08	1.50E−08	5	1
	NO: 94
CDH13	SEQ ID	0.83	0.741	0.851	5.67E−09	3.46E−07	4.94E−08	4	4
	NO: 70
ARH1/NOEY2	SEQ ID	0.84	0.777	0.857	1.57E−08	9.57E−07	1.20E−07	5	4
	NO: 97
SCGB3A1	SEQ ID	0.82	0.832	0.814	6.51E−08	3.97E−06	4.41E−07	4	1
	NO: 115
FHIT	SEQ ID	0.79	0.814	0.781	1.23E−07	7.50E−06	7.50E−07	3	1
	NO: 76
CCND2	SEQ ID	0.76	0.723	0.768	1.65E−07	1.00E−05	9.13E−07	6	2
	NO: 104
HIC1	SEQ ID	0.79	0.659	0.828	2.32E−07	1.41E−05	1.18E−06	5	1
	NO: 85
APC	SEQ ID	0.73	0.6	0.773	4.29E−07	2.62E−05	2.01E−06	4	4
	NO: 65
TIMP3	SEQ ID	0.77	0.605	0.82	5.93E−07	3.62E−05	2.58E−06	4	3
	NO: 103
IGSF4	SEQ ID	0.75	0.732	0.753	2.17E−06	1.32E−04	8.83E−06	4	1
	NO: 74
RARB	SEQ ID	0.77	0.614	0.818	2.53E−06	1.54E−04	9.65E−06	4	2
	NO: 88
PRDM2	SEQ ID	0.8	0.8	0.793	3.88E−06	2.36E−04	1.39E−05	4	1
	NO: 114
PLAU	SEQ ID	0.74	0.609	0.776	4.86E−06	2.96E−04	1.57E−05	4	2
	NO: 62
CDKN2A	SEQ ID	0.76	0.577	0.815	4.88E−06	2.98E−04	1.57E−05	3	0
	NO: 57
SLC19A1	SEQ ID	0.7	0.6	0.723	1.20E−05	7.35E−04	3.67E−05	3	0
	NO: 116
ELK1	SEQ ID	0.69	0.795	0.655	1.42E−05	8.67E−04	4.13E−05	5	0
	NO: 2
FABP3	SEQ ID	0.8	0.655	0.846	1.80E−05	1.10E−03	5.00E−05	4	2
	NO: 77
HOXA5	SEQ ID	0.75	0.618	0.785	2.40E−05	1.46E−03	6.36E−05	4	2
	NO: 78
SNCG	SEQ ID	0.7	0.655	0.708	4.07E−05	2.48E−03	1.03E−04	4	1
	NO: 73
TGFBR2	SEQ ID	0.76	0.65	0.789	4.35E−05	2.65E−03	1.06E−04	4	1
	NO: 93
PGR	SEQ ID	0.71	0.641	0.732	5.96E−05	3.64E−03	1.40E−04	4	1
	NO: 83
THRB	SEQ ID	0.68	0.545	0.726	1.72E−04	1.05E−02	3.88E−04	4	1
	NO: 106
EYA4	SEQ ID	0.74	0.741	0.741	3.42E−04	2.08E−02	7.44E−04	4	0
	NO: 58
APAF1	SEQ ID	0.72	0.659	0.736	5.53E−04	3.37E−02	1.16E−03	5	1
	NO: 82
SERPINB5	SEQ ID	0.69	0.573	0.719	6.00E−04	3.66E−02	1.22E−03	3	0
	NO: 68
SASH1	SEQ ID	0.69	0.527	0.742	7.38E−04	4.50E−02	1.45E−03	4	1
	NO: 102
MLH1	SEQ ID	0.73	0.659	0.751	8.31E−04	5.07E−02	1.58E−03	4	0
	NO: 89
CASP8	SEQ ID	0.65	0.645	0.654	1.86E−03	1.13E−01	3.43E−03	4	0
	NO: 71
RARA	SEQ ID	0.66	0.486	0.707	2.27E−03	1.38E−01	4.07E−03	4	0
	NO: 108
TERT	SEQ ID	0.67	0.664	0.67	2.89E−03	1.76E−01	5.04E−03	4	0
	NO: 92
SOD2	SEQ ID	0.69	0.591	0.72	3.25E−03	1.98E−01	5.50E−03	4	0
	NO: 105
SYK	SEQ ID	0.64	0.527	0.669	3.85E−03	2.35E−01	6.20E−03	4	0
	NO: 60
TWIST	SEQ ID	0.65	0.659	0.645	3.86E−03	2.36E−01	6.20E−03	4	0
	NO: 100
S100A7	SEQ ID	0.72	0.486	0.784	5.17E−03	3.15E−01	8.09E−03	3	0
	NO: 96
ESR2	SEQ ID	0.66	0.573	0.688	7.05E−03	4.30E−01	1.08E−02	4	0
	NO: 91
ESR1	SEQ ID	0.64	0.782	0.603	9.45E−03	5.76E−01	1.40E−02	3	0
	NO: 75
MCT1	SEQ ID	0.65	0.641	0.655	9.62E−03	5.87E−01	1.40E−02	4	0
	NO: 101
TP73	SEQ ID	0.65	0.641	0.649	1.06E−02	6.47E−01	1.50E−02	4	0
	NO: 86
TMS1/ASC	SEQ ID	0.57	0.568	0.564	1.54E−02	9.40E−01	2.14E−02	4	0
	NO: 84
THBS1	SEQ ID	0.58	0.618	0.566	1.82E−02	1.00E+00	2.47E−02	4	0
	NO: 81
PRSS8	SEQ ID	0.6	0.618	0.6	2.71E−02	1.00E+00	3.59E−02	4	0
	NO: 72
ALX4	SEQ ID	0.63	0.395	0.7	4.40E−02	1.00E+00	5.71E−02	4	0
	NO: 64
DAPK1	SEQ ID	0.57	0.6	0.559	7.28E−02	1.00E+00	9.25E−02	2	0
	NO: 98
TPM1	SEQ ID	0.59	0.473	0.63	9.68E−02	1.00E+00	1.21E−01	4	0
	NO: 110
CDKN1A	SEQ ID	0.59	0.645	0.577	1.09E−01	1.00E+00	1.33E−01	4	0
	NO: 67
CDH1	SEQ ID	0.58	0.436	0.628	1.28E−01	1.00E+00	1.53E−01	5	0
	NO: 79
IL6	SEQ ID	0.6	0.45	0.639	1.44E−01	1.00E+00	1.69E−01	4	0
	NO: 99
CLDN7	SEQ ID	0.55	0.609	0.526	1.88E−01	1.00E+00	2.16E−01	4	0
	NO: 87
GPC3	SEQ ID	0.52	0.482	0.532	2.00E−01	1.00E+00	2.26E−01	4	0
	NO: 118
STAT1	SEQ ID	0.56	0.618	0.545	4.52E−01	1.00E+00	5.01E−01	4	0
	NO: 109
SFN	SEQ ID	0.49	0.345	0.536	5.20E−01	1.00E+00	5.67E−01	4	0
	NO: 69
BRCA2	SEQ ID	0.55	0.423	0.581	5.57E−01	1.00E+00	5.96E−01	5	0
	NO: 56
NME1	SEQ ID	0.48	0.35	0.52	7.13E−01	1.00E+00	7.50E−01	4	0
	NO: 107
TP53	SEQ ID	0.51	0.409	0.545	7.47E−01	1.00E+00	7.72E−01	4	0
	NO: 80
BRCA1	SEQ ID	0.47	0.318	0.515	8.59E−01	1.00E+00	8.73E−01	4	0
	NO: 66
LOT1	SEQ ID	0.54	0.232	0.628	8.86E−01	1.00E+00	8.86E−01	4	0
	NO: 95

TABLE 11
DCIS vs. benign breast conditions Chip 2
SEQ ID					P-value	P-value		n Significant
NO	Accuracy	Sensitivity	Specificity	P-value	(Bonferroni)	FDR	n Oligos	oligos
SEQ ID	0.892	0.864	0.901	2.28E−16	1.23E−14	1.23E−14	4	3
NO: 27
SEQ ID	0.86	0.818	0.874	1.63E−13	8.80E−12	4.40E−12	4	3
NO: 12
SEQ ID	0.91	0.859	0.926	3.75E−13	2.03E−11	6.76E−12	4	3
NO: 46
SEQ ID	0.89	0.827	0.91	9.50E−12	5.13E−10	1.18E−10	4	3
NO: 3
SEQ ID	0.876	0.791	0.903	1.09E−11	5.88E−10	1.18E−10	4	4
NO: 117
SEQ ID	0.804	0.845	0.791	3.79E−11	2.05E−09	3.41E−10	4	2
NO: 48
SEQ ID	0.874	0.836	0.887	7.60E−11	4.10E−09	5.86E−10	5	3
NO: 41
SEQ ID	0.792	0.664	0.834	3.02E−10	1.63E−08	2.04E−09	4	4
NO: 4
SEQ ID	0.871	0.859	0.875	6.76E−10	3.65E−08	4.06E−09	6	5
NO: 6
SEQ ID	0.849	0.768	0.875	7.78E−10	4.20E−08	4.20E−09	5	2
NO: 24
SEQ ID	0.823	0.718	0.857	8.60E−10	4.65E−08	4.22E−09	5	5
NO: 31
SEQ ID	0.87	0.695	0.926	2.10E−09	1.14E−07	9.46E−09	4	1
NO: 51
SEQ ID	0.833	0.745	0.862	2.52E−09	1.36E−07	1.05E−08	5	3
NO: 7
SEQ ID	0.813	0.768	0.828	4.22E−09	2.28E−07	1.63E−08	4	3
NO: 13
SEQ ID	0.84	0.764	0.865	1.11E−08	6.01E−07	4.01E−08	4	3
NO: 30
SEQ ID	0.829	0.745	0.856	4.47E−08	2.42E−06	1.51E−07	4	1
NO: 42
SEQ ID	0.847	0.691	0.897	2.98E−07	1.61E−05	9.48E−07	5	1
NO: 16
SEQ ID	0.778	0.659	0.816	3.18E−07	1.72E−05	9.55E−07	5	1
NO: 34
SEQ ID	0.797	0.705	0.826	1.01E−06	5.43E−05	2.86E−06	8	4
NO: 22
SEQ ID	0.758	0.718	0.771	1.65E−06	8.91E−05	4.45E−06	5	1
NO: 17
SEQ ID	0.758	0.709	0.774	1.96E−06	1.06E−04	5.05E−06	5	2
NO: 54
SEQ ID	0.731	0.573	0.782	3.01E−06	1.62E−04	7.38E−06	5	1
NO: 50
SEQ ID	0.804	0.532	0.893	4.52E−06	2.44E−04	1.06E−05	3	0
NO: 33
SEQ ID	0.73	0.641	0.759	9.90E−06	5.35E−04	2.23E−05	5	0
NO: 38
SEQ ID	0.732	0.623	0.768	1.22E−05	6.61E−04	2.64E−05	9	1
NO: 10
SEQ ID	0.834	0.545	0.928	1.69E−05	9.11E−04	3.50E−05	5	0
NO: 9
SEQ ID	0.764	0.6	0.818	2.16E−05	1.16E−03	4.31E−05	5	2
NO: 18
SEQ ID	0.773	0.591	0.832	4.56E−05	2.46E−03	8.79E−05	3	1
NO: 23
SEQ ID	0.692	0.677	0.697	1.49E−04	8.06E−03	2.76E−04	4	1
NO: 2
SEQ ID	0.666	0.591	0.69	1.53E−04	8.27E−03	2.76E−04	3	1
NO: 32
SEQ ID	0.711	0.591	0.75	1.65E−04	8.90E−03	2.82E−04	5	0
NO: 29
SEQ ID	0.713	0.7	0.718	1.67E−04	9.03E−03	2.82E−04	4	1
NO: 39
SEQ ID	0.72	0.673	0.735	2.13E−04	1.15E−02	3.49E−04	4	1
NO: 43
SEQ ID	0.71	0.527	0.769	2.74E−04	1.48E−02	4.31E−04	4	1
NO: 11
SEQ ID	0.728	0.586	0.774	2.80E−04	1.51E−02	4.31E−04	4	0
NO: 47
SEQ ID	0.637	0.682	0.622	1.45E−03	7.84E−02	2.18E−03	3	0
NO: 26
SEQ ID	0.646	0.823	0.588	2.25E−03	1.21E−01	3.28E−03	4	0
NO: 52
SEQ ID	0.647	0.627	0.653	2.58E−03	1.40E−01	3.67E−03	5	0
NO: 25
SEQ ID	0.699	0.505	0.762	3.07E−03	1.66E−01	4.25E−03	3	0
NO: 14
SEQ ID	0.586	0.55	0.597	7.37E−03	3.98E−01	9.95E−03	4	0
NO: 20
SEQ ID	0.658	0.518	0.703	1.16E−02	6.27E−01	1.53E−02	4	0
NO: 19
SEQ ID	0.658	0.514	0.704	1.93E−02	1.00E+00	2.48E−02	7	0
NO: 28
SEQ ID	0.642	0.641	0.643	3.10E−02	1.00E+00	3.90E−02	5	0
NO: 8
SEQ ID	0.681	0.536	0.728	4.06E−02	1.00E+00	4.99E−02	5	0
NO: 40
SEQ ID	0.58	0.445	0.624	6.69E−02	1.00E+00	7.95E−02	5	0
NO: 1
SEQ ID	0.633	0.459	0.69	6.77E−02	1.00E+00	7.95E−02	4	0
NO: 35
SEQ ID	0.606	0.518	0.634	8.76E−02	1.00E+00	1.01E−01	5	0
NO: 15
SEQ ID	0.566	0.577	0.562	9.68E−02	1.00E+00	1.09E−01	4	0
NO: 36
SEQ ID	0.667	0.409	0.75	1.00E−01	1.00E+00	1.10E−01	5	0
NO: 55
SEQ ID	0.607	0.427	0.665	1.57E−01	1.00E+00	1.69E−01	4	0
NO: 45
SEQ ID	0.597	0.468	0.638	2.14E−01	1.00E+00	2.27E−01	5	0
NO: 5
SEQ ID	0.62	0.491	0.662	2.22E−01	1.00E+00	2.31E−01	4	0
NO: 21
SEQ ID	0.636	0.391	0.715	3.37E−01	1.00E+00	3.44E−01	3	0
NO: 37
SEQ ID	0.55	0.186	0.668	6.49E−01	1.00E+00	6.49E−01	2	0
NO: 44

TABLE 12
Chip 1 Breast cancer vs. benign breast conditions
							P-
	SEQ ID					P-value	value	n	n Significant
Gene Name	NO:	Accuracy	Sensitivity	Specificity	p-value	(Bonferroni)	FDR	Oligos	oligos
SLIT2	SEQ ID	0.836	0.829	0.861	3.16E−37	1.92E−35	0.00	4	4
	NO: 112
HS3ST2	SEQ ID	0.852	0.854	0.843	4.37E−33	2.66E−31	0.00	2	2
	NO: 113
HOXA5	SEQ ID	0.782	0.784	0.776	5.67E−28	3.46E−26	0.00	4	4
	NO: 78
ARH1/NOEY2	SEQ ID	0.771	0.727	0.924	2.55E−24	1.56E−22	0.00	5	5
	NO: 97
IGFBP7	SEQ ID	0.769	0.759	0.801	4.30E−24	2.62E−22	0.00	5	3
	NO: 94
PLAU	SEQ ID	0.774	0.765	0.805	3.29E−23	2.01E−21	0.00	4	3
	NO: 62
CDH13	SEQ ID	0.741	0.702	0.881	1.54E−20	9.42E−19	0.00	4	4
	NO: 70
TIMP3	SEQ ID	0.715	0.694	0.789	1.37E−19	8.34E−18	0.00	4	4
	NO: 103
CCND2	SEQ ID	0.729	0.716	0.776	7.23E−19	4.41E−17	0.00	6	4
	NO: 104
GSTP1	SEQ ID	0.686	0.632	0.88	3.12E−18	1.90E−16	0.00	4	4
	NO: 59
APC	SEQ ID	0.733	0.731	0.739	6.84E−18	4.18E−16	0.00	4	4
	NO: 65
SCGB3A1	SEQ ID	0.748	0.745	0.761	5.71E−16	3.48E−14	0.00	4	1
	NO: 115
GJB2	SEQ ID	0.679	0.638	0.824	9.16E−16	5.59E−14	0.00	4	1
	NO: 111
CDKN2A	SEQ ID	0.669	0.614	0.862	1.30E−15	7.94E−14	0.00	3	3
	NO: 57
PRDM2	SEQ ID	0.718	0.696	0.795	2.85E−14	1.74E−12	0.00	4	3
	NO: 114
FABP3	SEQ ID	0.691	0.651	0.834	1.33E−13	8.14E−12	0.00	4	4
	NO: 77
S100A7	SEQ ID	0.693	0.643	0.874	1.18E−12	7.22E−11	0.00	3	1
	NO: 96
SNCG	SEQ ID	0.68	0.681	0.676	1.65E−12	1.01E−10	0.00	4	4
	NO: 73
RASSF1A	SEQ ID	0.708	0.692	0.766	8.00E−12	4.88E−10	0.00	3	3
	NO: 90
TMS1/ASC	SEQ ID	0.71	0.735	0.619	9.47E−12	5.77E−10	0.00	4	1
	NO: 84
FHIT	SEQ ID	0.688	0.664	0.774	1.23E−11	7.48E−10	0.00	3	1
	NO: 76
SERPINB5	SEQ ID	0.698	0.696	0.703	1.23E−11	7.48E−10	0.00	3	1
	NO: 68
SYK	SEQ ID	0.699	0.708	0.669	1.52E−11	9.25E−10	0.00	4	2
	NO: 60
TWIST	SEQ ID	0.689	0.683	0.711	2.88E−11	1.76E−09	0.00	4	1
	NO: 100
HIC1	SEQ ID	0.669	0.672	0.659	3.46E−11	2.11E−09	0.00	5	3
	NO: 85
SLC19A1	SEQ ID	0.646	0.635	0.685	2.48E−10	1.52E−08	0.00	3	2
	NO: 116
APAF1	SEQ ID	0.667	0.653	0.715	2.85E−10	1.74E−08	0.00	5	1
	NO: 82
RARB	SEQ ID	0.602	0.56	0.751	8.36E−10	5.10E−08	0.00	4	3
	NO: 88
TGFBR2	SEQ ID	0.622	0.574	0.791	1.18E−09	7.19E−08	0.00	4	1
	NO: 93
MCT1	SEQ ID	0.719	0.748	0.616	1.42E−09	8.66E−08	0.00	4	2
	NO: 101
SOD2	SEQ ID	0.667	0.653	0.716	4.08E−09	2.49E−07	0.00	4	1
	NO: 105
THRB	SEQ ID	0.663	0.642	0.738	4.27E−09	2.61E−07	0.00	4	1
	NO: 106
IGSF4	SEQ ID	0.674	0.66	0.723	4.38E−09	2.67E−07	0.00	4	1
	NO: 74
SASH1	SEQ ID	0.657	0.656	0.661	7.22E−09	4.41E−07	0.00	4	2
	NO: 102
THBS1	SEQ ID	0.676	0.719	0.523	1.60E−08	9.76E−07	0.00	4	2
	NO: 81
ESR1	SEQ ID	0.694	0.724	0.585	3.85E−08	2.35E−06	0.00	3	2
	NO: 75
EYA4	SEQ ID	0.647	0.631	0.704	4.36E−08	2.66E−06	0.00	4	3
	NO: 58
RARA	SEQ ID	0.623	0.594	0.73	1.07E−07	6.51E−06	0.00	4	1
	NO: 108
CASP8	SEQ ID	0.611	0.6	0.649	1.45E−07	8.85E−06	0.00	4	1
	NO: 71
ALX4	SEQ ID	0.588	0.543	0.747	1.68E−07	1.02E−05	0.00	4	1
	NO: 64
ESR2	SEQ ID	0.55	0.5	0.731	1.27E−06	7.72E−05	0.00	4	0
	NO: 91
NME1	SEQ ID	0.581	0.538	0.732	1.60E−06	9.74E−05	0.00	4	2
	NO: 107
ELK1	SEQ ID	0.681	0.693	0.638	1.78E−06	1.08E−04	0.00	5	0
	NO: 2
MLH1	SEQ ID	0.535	0.468	0.773	1.80E−06	1.10E−04	0.00	4	1
	NO: 89
PGR	SEQ ID	0.636	0.645	0.601	2.41E−06	1.47E−04	0.00	4	2
	NO: 83
TERT	SEQ ID	0.663	0.668	0.642	2.07E−05	1.26E−03	0.00	4	2
	NO: 92
TP73	SEQ ID	0.625	0.624	0.63	6.76E−05	4.12E−03	0.00	4	1
	NO: 86
CLDN7	SEQ ID	0.622	0.638	0.566	1.52E−04	9.25E−03	0.00	4	1
	NO: 87
IL6	SEQ ID	0.567	0.552	0.622	2.09E−04	1.28E−02	0.00	4	0
	NO: 99
CDKN1A	SEQ ID	0.6	0.619	0.531	1.22E−03	7.43E−02	0.00	4	1
	NO: 67
GPC3	SEQ ID	0.563	0.565	0.557	1.41E−03	8.59E−02	0.00	4	0
	NO: 118
LOT1	SEQ ID	0.513	0.437	0.784	2.46E−03	1.50E−01	0.00	4	0
	NO: 95
STAT1	SEQ ID	0.61	0.616	0.586	3.20E−03	1.95E−01	0.00	4	0
	NO: 109
SFN	SEQ ID	0.545	0.549	0.53	5.58E−03	3.40E−01	0.01	4	0
	NO: 69
PRSS8	SEQ ID	0.542	0.532	0.578	6.37E−03	3.88E−01	0.01	4	0
	NO: 72
TPM1	SEQ ID	0.524	0.479	0.684	1.73E−02	1.00E+00	0.02	4	0
	NO: 110
BRCA2	SEQ ID	0.558	0.553	0.576	2.76E−02	1.00E+00	0.03	5	0
	NO: 56
BRCA1	SEQ ID	0.531	0.487	0.684	4.70E−02	1.00E+00	0.05	4	0
	NO: 66
TP53	SEQ ID	0.484	0.449	0.607	1.87E−01	1.00E+00	0.19	4	0
	NO: 80
CDH1	SEQ ID	0.534	0.534	0.531	3.69E−01	1.00E+00	0.38	5	0
	NO: 79
DAPK1	SEQ ID	0.46	0.466	0.439	9.43E−01	1.00E+00	0.94	2	0
	NO: 98

TABLE 13
Chip 2 Breast cancer vs. benign breast conditions
SEQ ID					P-value		n	n Significant
NO	Accuracy	Sensitivity	Specificity	P-value	(Bonferroni)	P-value FDR	Oligos	oligos
SEQ ID	0.86	0.839	0.94	2.44E−39	1.32E−37	1.32E−37	4	4
NO: 117
SEQ ID	0.852	0.839	0.899	5.84E−36	3.15E−34	1.58E−34	4	3
NO: 12
SEQ ID	0.821	0.801	0.899	6.41E−32	3.46E−30	1.15E−30	4	4
NO: 46
SEQ ID	0.858	0.85	0.89	1.94E−31	1.05E−29	2.61E−30	6	6
NO: 6
SEQ ID	0.838	0.828	0.878	1.08E−29	5.86E−28	1.17E−28	5	4
NO: 7
SEQ ID	0.834	0.815	0.906	2.11E−29	1.14E−27	1.66E−28	4	4
NO: 3
SEQ ID	0.824	0.821	0.837	2.16E−29	1.17E−27	1.66E−28	5	4
NO: 41
SEQ ID	0.802	0.787	0.857	7.96E−29	4.30E−27	5.37E−28	4	3
NO: 27
SEQ ID	0.825	0.816	0.862	1.14E−27	6.17E−26	6.85E−27	5	5
NO: 31
SEQ ID	0.767	0.752	0.822	4.61E−22	2.49E−20	2.49E−21	4	4
NO: 4
SEQ ID	0.73	0.686	0.897	1.82E−21	9.83E−20	8.94E−21	4	2
NO: 51
SEQ ID	0.773	0.762	0.816	4.66E−21	2.52E−19	2.10E−20	5	3
NO: 18
SEQ ID	0.761	0.745	0.824	9.81E−20	5.30E−18	4.07E−19	4	2
NO: 47
SEQ ID	0.745	0.722	0.829	4.98E−18	2.69E−16	1.92E−17	5	1
NO: 16
SEQ ID	0.701	0.664	0.838	5.22E−17	2.82E−15	1.88E−16	5	2
NO: 34
SEQ ID	0.747	0.728	0.819	9.31E−17	5.03E−15	3.14E−16	4	2
NO: 42
SEQ ID	0.695	0.655	0.844	1.61E−15	8.69E−14	5.11E−15	4	3
NO: 13
SEQ ID	0.73	0.729	0.731	2.04E−15	1.10E−13	6.11E−15	4	4
NO: 39
SEQ ID	0.731	0.72	0.769	3.58E−15	1.93E−13	1.02E−14	4	1
NO: 43
SEQ ID	0.691	0.66	0.807	4.12E−15	2.23E−13	1.11E−14	5	4
NO: 29
SEQ ID	0.723	0.7	0.812	8.23E−15	4.45E−13	2.12E−14	8	7
NO: 22
SEQ ID	0.69	0.625	0.935	1.09E−14	5.89E−13	2.68E−14	4	4
NO: 30
SEQ ID	0.688	0.67	0.756	1.90E−14	1.03E−12	4.46E−14	4	4
NO: 11
SEQ ID	0.69	0.674	0.749	8.91E−14	4.81E−12	2.00E−13	9	4
NO: 10
SEQ ID	0.709	0.702	0.735	1.01E−13	5.47E−12	2.19E−13	5	5
NO: 8
SEQ ID	0.727	0.718	0.762	7.74E−13	4.18E−11	1.61E−12	4	4
NO: 48
SEQ ID	0.631	0.602	0.738	7.90E−12	4.27E−10	1.58E−11	5	2
NO: 50
SEQ ID	0.631	0.586	0.803	2.75E−11	1.49E−09	5.31E−11	3	2
NO: 33
SEQ ID	0.606	0.56	0.778	1.94E−10	1.05E−08	3.62E−10	5	3
NO: 24
SEQ ID	0.678	0.687	0.646	3.57E−10	1.93E−08	6.42E−10	3	2
NO: 26
SEQ ID	0.642	0.623	0.713	2.19E−09	1.18E−07	3.81E−09	5	2
NO: 54
SEQ ID	0.665	0.653	0.712	2.52E−09	1.36E−07	4.25E−09	5	1
NO: 38
SEQ ID	0.661	0.643	0.728	7.27E−09	3.93E−07	1.19E−08	5	1
NO: 25
SEQ ID	0.636	0.618	0.706	1.59E−08	8.58E−07	2.52E−08	3	1
NO: 32
SEQ ID	0.664	0.635	0.774	4.69E−08	2.53E−06	7.24E−08	5	0
NO: 5
SEQ ID	0.648	0.622	0.744	5.74E−08	3.10E−06	8.62E−08	3	1
NO: 23
SEQ ID	0.636	0.599	0.774	1.17E−07	6.32E−06	1.71E−07	5	2
NO: 17
SEQ ID	0.64	0.638	0.647	1.33E−07	7.17E−06	1.89E−07	5	1
NO: 1
SEQ ID	0.601	0.571	0.715	1.58E−07	8.55E−06	2.19E−07	3	1
NO: 14
SEQ ID	0.69	0.705	0.635	3.78E−07	2.04E−05	5.11E−07	4	2
NO: 52
SEQ ID	0.642	0.619	0.728	5.19E−07	2.80E−05	6.83E−07	5	1
NO: 9
SEQ ID	0.602	0.567	0.734	1.23E−06	6.64E−05	1.58E−06	4	1
NO: 19
SEQ ID	0.611	0.582	0.722	3.21E−06	1.73E−04	4.03E−06	5	1
NO: 40
SEQ ID	0.623	0.641	0.553	7.05E−05	3.81E−03	8.65E−05	4	0
NO: 35
SEQ ID	0.594	0.569	0.69	1.02E−04	5.50E−03	1.22E−04	4	1
NO: 2
SEQ ID	0.596	0.567	0.704	1.21E−04	6.52E−03	1.42E−04	7	2
NO: 28
SEQ ID	0.583	0.584	0.579	4.02E−04	2.17E−02	4.61E−04	4	1
NO: 36
SEQ ID	0.564	0.538	0.662	7.11E−04	3.84E−02	8.00E−04	4	1
NO: 20
SEQ ID	0.619	0.636	0.554	5.71E−03	3.08E−01	6.29E−03	3	0
NO: 37
SEQ ID	0.425	0.33	0.781	9.30E−02	1.00E+00	1.00E−01	5	0
NO: 55
SEQ ID	0.533	0.511	0.613	1.09E−01	1.00E+00	1.16E−01	5	0
NO: 15
SEQ ID	0.488	0.454	0.615	1.43E−01	1.00E+00	1.48E−01	2	0
NO: 44
SEQ ID	0.528	0.521	0.556	1.53E−01	1.00E+00	1.55E−01	4	0
NO: 21
SEQ ID	0.525	0.521	0.54	1.95E−01	1.00E+00	1.95E−01	4	0
NO: 45

TABLE 14
Sample overview
Sample					Menopausal
No.	main class	subclass	sex	age	status
1	benign breast	Normal Breast	f	45
2	benign breast	Normal Breast	f	45
3	benign breast	Normal Breast	f	17
4	benign breast	Normal Breast	f	20
5	benign breast	Normal Breast	f	19
6	benign breast	Normal Breast	f	33
7	benign breast	Normal Breast	f	36
8	benign breast	Normal Breast	f	37
9	benign breast	Normal Breast	f	57
10	benign breast	Normal Breast	f	50
11	benign breast	Normal Breast	f	53
12	benign breast	Normal Breast	f	77
13	other cancer	ovarian cancer	f	83
14	other cancer	ovarian cancer	f	30
15	other cancer	ovarian cancer	f	53
16	other cancer	ovarian cancer	f	56
17	other cancer	ovarian cancer	f	47
18	other cancer	ovarian cancer	f	63
19	other cancer	ovarian cancer	f	55
20	other cancer	ovarian cancer	f	58
21	other cancer	ovarian cancer	f	49
22	other cancer	ovarian cancer	f	52
23	other cancer	endometrial cancer	f	53
24	other cancer	endometrial cancer	f	46
25	other cancer	endometrial cancer	f	64
26	other cancer	endometrial cancer	f	51
27	other cancer	endometrial cancer	f	80
28	other cancer	endometrial cancer	f	68
29	other cancer	endometrial cancer	f	70
30	other cancer	endometrial cancer	f	77
31	other cancer	endometrial cancer	f	92
32	other cancer	endometrial cancer	f	27
33	other cancer	endometrial cancer	f	52
34	other cancer	endometrial cancer	f	61
35	other cancer	ovarian cancer	f	52
36	other cancer	ovarian cancer	f	65
37	other cancer	ovarian cancer	f	na
38	other cancer	ovarian cancer	f	54
39	other cancer	ovarian cancer	f	52
40	other cancer	ovarian cancer	f	68
41	other cancer	endometrial cancer	f	74
42	other cancer	endometrial cancer	f	30
43	other cancer	endometrial cancer	f	44
44	other cancer	endometrial cancer	f	58
45	benign breast	Normal Breast	f	78
46	benign breast	Normal Breast	f	37
47	benign breast	Normal Breast	f	48
48	benign breast	Normal Breast	f	37
49	benign breast	Normal Breast	f	36
50	benign breast	Normal Breast	f	43
51	benign breast	Normal Breast	f	41
52	benign breast	Normal Breast	f	48
53	benign breast	Normal Breast	f	35
54	benign breast	Normal Breast	f	41	pre
55	benign breast	Normal Breast	f	48
56	benign breast	Normal Breast	f	39
57	benign breast	Normal Breast	f	69
58	benign breast	Normal Breast	f	52
59	benign breast	Normal Breast	f	41
60	benign breast	Normal Breast	f	43
61	benign breast	Normal Breast	f	36
62	benign breast	Normal Breast	f	36
63	other cancer	lung cancer	f	—
64	other cancer	lung cancer	f	—
65	other cancer	lung cancer	f	—
66	other cancer	lung cancer	f	—
67	other cancer	lung cancer	f	78
68	other cancer	lung cancer	f	60
69	other cancer	lung cancer	f	54
70	other cancer	lung cancer	f	—
71	other cancer	lung cancer	f	67	post
72	other cancer	lung cancer	f	56	post
73	other cancer	lung cancer	f	51	pre
74	other cancer	lung cancer	f	76	post
75	other cancer	lung cancer	f	41
76	other cancer	lung cancer	f	66	post
77	lymphocytes	lymphocytes	f	60
78	lymphocytes	lymphocytes	f	57
79	lymphocytes	lymphocytes	f	61
80	lymphocytes	lymphocytes	f	61
81	lymphocytes	lymphocytes	f	49
82	lymphocytes	lymphocytes	f	48
83	lymphocytes	lymphocytes	f	42
84	lymphocytes	lymphocytes	f	44
85	lymphocytes	lymphocytes	f	47
86	lymphocytes	lymphocytes	f	47
87	lymphocytes	lymphocytes	f	49
88	lymphocytes	lymphocytes	f	55
89	lymphocytes	lymphocytes	f	55
90	lymphocytes	lymphocytes	f	55
91	lymphocytes	lymphocytes	m	49
92	lymphocytes	lymphocytes	f	65
93	lymphocytes	lymphocytes	f	82
94	lymphocytes	lymphocytes	f	64
95	lymphocytes	lymphocytes	f	74
96	lymphocytes	lymphocytes	f	37
97	lymphocytes	lymphocytes	f	37
98	lymphocytes	lymphocytes	f	42
99	lymphocytes	lymphocytes	f	28
100	lymphocytes	lymphocytes	f	58
101	lymphocytes	lymphocytes	f	67
102	lymphocytes	lymphocytes	f	38
103	other cancer	lung cancer	f	55
104	other cancer	lung cancer	f	56
105	other cancer	lung cancer	f	68
106	other cancer	lung cancer	f	80
107	lymphocytes	lymphocytes	m	NA
108	lymphocytes	lymphocytes	m	NA
109	lymphocytes	lymphocytes	m	NA
110	lymphocytes	lymphocytes	m	NA
111	lymphocytes	lymphocytes	m	NA
112	lymphocytes	lymphocytes	m	NA
113	lymphocytes	lymphocytes	m	NA
114	lymphocytes	lymphocytes	m	NA
115	brca	IDC	f	69	post
116	brca	IDC	f	69	post
117	brca	IDC	f	33	pre
118	brca	IDC	f	54	pre
119	brca	IDC	f	86	post
120	brca	IDC	f	62	post
121	brca	IDC	f	30	pre
122	brca	IDC	f	33	pre
123	brca	IDC	f	78	post
124	brca	IDC	f	34	pre
125	brca	IDC	f	46	pre
126	brca	IDC	f	61	post
127	brca	IDC	f	44	pre
128	brca	IDC	f	68	post
129	brca	IDC	f	57	post
130	brca	IDC	f	70	post
131	brca	IDC	f	42	pre
132	brca	IDC	f	37	pre
133	brca	IDC	f	45	pre
134	brca	IDC	f	47	pre
135	brca	IDC	f	35	pre
136	brca	IDC	f	49	pre
137	brca	IDC	f	40	post
138	brca	IDC	f	75	post
139	brca	IDC	f	76	post
140	brca	IDC	f	69	post
141	brca	IDC	f	46	pre
142	brca	IDC	f	50	pre
143	brca	IDC	f	44	pre
144	brca	IDC	f	47	pre
145	brca	ILC	f	47	pre
146	brca	IDC	f	56	post
147	brca	IDC	f	40	pre
148	brca	IDC	f	38	pre
149	brca	ILC	f	50	pre
150	brca	IDC	f	42	pre
151	brca	ILC	f	55	pre
152	brca	IDC	f	62	post
153	brca	IDC	f	63	post
154	brca	IDC	f	38	pre
155	brca	IDC	f	32	pre
156	brca	IDC	f	59	post
157	brca	IDC	f	53	post
158	brca	IDC	f	38	pre
159	brca	IDC	f	43	pre
160	brca	IDC	f	46	pre
161	brca	IDC	f	47	pre
162	brca	IDC	f	52	pre
163	brca	IDC	f	55	post
164	brca	IDC	f	68	post
165	brca	IDC	f	68	post
166	brca	IDC	f	63	post
167	brca	IDC	f	49	post
168	brca	IDC	f	47	pre
169	brca	IDC	f	50	pre
170	brca	IDC	f	66	post
171	brca	ILC	f	48	pre
172	brca	IDC	f	56	post
173	brca	IDC	f	53	post
174	brca	IDC	f	33	pre
175	brca	IDC	f	48	pre
176	brca	ILC	f	40	pre
177	brca	ILC	f	44	pre
178	brca	IDC	f	79	post
179	brca	IDC	f	78	post
180	brca	IDC	f	30	pre
181	brca	IDC	f	44	pre
182	brca	IDC	f	45	pre
183	brca	ILC	f	47	pre
184	brca	ILC	f	51	pre
185	brca	IDC	f	65	post
186	brca	IDC	f	70	post
187	brca	IDC	f	51	pre
188	brca	IDC	f	67	post
189	brca	IDC	f	44	pre
190	brca	IDC	f	64	post
191	brca	IDC	f	72	post
192	brca	ILC	f	42	pre
193	brca	IDC	f	41	pre
194	brca	ILC	f	37	pre
195	brca	IDC	f	65	post
196	brca	IDC	f	67	post
197	brca	IDC	f	62	post
198	brca	IDC	f	51	pre
199	brca	IDC	f	55	post
200	brca	IDC	f	53	post
201	brca	IDC	f	74	post
202	brca	ILC	f	45	pre
203	brca	ILC	f	46	pre
204	brca	IDC	f	85	post
205	brca	IDC	f	72	post
206	brca	IDC	f	48	pre
207	brca	IDC	f	62	post
208	brca	IDC	f	52	post
209	brca	IDC	f	45	pre
210	brca	IDC	f	35	pre
211	brca	IDC	f	71	post
212	brca	IDC	f	61	post
213	brca	IDC	f	49	pre
214	brca	IDC	f	24	pre
215	brca	IDC	f	48	pre
216	brca	IDC	f	51	post
217	brca	IDC	f	61	post
218	brca	IDC	f	55	post
219	brca	IDC	f	87	post
220	brca	IDC	f	51	post
221	brca	IDC	f	43	pre
222	brca	IDC	f	65	post
223	brca	IDC	f	59	post
224	brca	IDC	f	53	post
225	brca	IDC	f	51	pre
226	brca	IDC	f	31	pre
227	brca	IDC	f	54	post
228	brca	IDC	f	60	post
229	brca	ILC	f	49	pre
230	brca	IDC	f	46	pre
231	brca	IDC	f	74	post
232	brca	IDC	f	47	pre
233	brca	IDC	f	46	pre
234	brca	IDC	f	44	pre
235	brca	ILC	f	48	pre
236	brca	IDC	f	51	post
237	brca	ILC	f	35	pre
238	brca	IDC	f	32	pre
239	brca	IDC	f	40	pre
240	brca	IDC	f	43	pre
241	brca	IDC	f	60	post
242	brca	IDC	f	76	post
243	brca	IDC	f	48	pre
244	brca	IDC	f	48	pre
245	brca	IDC	f	33	pre
246	brca	IDC	f	58	post
247	brca	IDC	f	62	post
248	brca	IDC	f	46	post
249	brca	IDC	f	63	post
250	brca	IDC	f	64	post
251	brca	IDC	f	46	pre
252	brca	IDC	f	47	pre
253	brca	ILC	f	44	pre
254	brca	IDC	f	38	pre
255	brca	ILC	f	38	pre
256	brca	IDC	f	48	pre
257	brca	IDC	f	50	pre
258	brca	IDC	f	66	post
259	brca	IDC	f	33	pre
260	brca	IDC	f	59	post
261	brca	IDC	f	35	pre
262	brca	IDC	f	59	post
263	brca	IDC	f	65	post
264	brca	IDC	f	56	post
265	brca	IDC	f	52	post
266	brca	IDC	f	47	pre
267	brca	IDC	f	75	post
268	brca	IDC	f	29	pre
269	brca	IDC	f	70	post
270	brca	IDC	f	79	post
271	brca	IDC	f	63	post
272	brca	ILC	f	37	pre
273	brca	IDC	f	69	post
274	brca	IDC	f	57	post
275	brca	IDC	f	72	post
276	brca	IDC	f	79	post
277	brca	IDC	f	53	post
278	brca	IDC	f	52	pre
279	brca	IDC	f	48	pre
280	brca	ILC	f	44	pre
281	brca	IDC	f	50	pre
282	brca	IDC	f	61	post
283	brca	IDC	f	57	post
284	brca	IDC	f	64	post
285	brca	IDC	f	43	pre
286	brca	ILC	f	46	pre
287	brca	IDC	f	62	post
288	brca	IDC	f	32	pre
289	brca	IDC	f	40	pre
290	brca	IDC	f	65	post
291	brca	IDC	f	47	pre
292	brca	IDC	f	45	pre
293	brca	IDC	f	51	pre
294	brca	IDC	f	62	post
295	brca	IDC	f	72	post
296	brca	IDC	f	52	post
297	brca	IDC	f	52	post
298	brca	IDC	f	46	pre
299	brca	IDC	f	61	post
300	brca	IDC	f	51	pre
301	brca	IDC	f	48	pre
302	brca	IDC	f	47	pre
303	brca	IDC	f	44	pre
304	brca	IDC	f	52	pre
305	brca	IDC	f	55	post
306	brca	IDC	f	42	pre
307	brca	IDC	f	49	pre
308	brca	IDC	f	52	post
309	brca	IDC	f	69	post
310	brca	IDC	f	64	post
311	brca	IDC	f	40	pre
312	brca	IDC	f	45	pre
313	brca	IDC	f	66	post
314	brca	IDC	f	64	post
315	brca	IDC	f	53	post
316	brca	ILC	f	51	pre
317	brca	IDC	f	54	post
318	brca	IDC	f	52	pre
319	brca	IDC	f	45	pre
320	brca	ILC	f	54	pre
321	brca	IDC	f	52	pre
322	brca	IDC	f	47	pre
323	brca	ILC	f	41	pre
324	brca	IDC	f	56	post
325	brca	IDC	f	72	post
326	brca	ILC	f	41	pre
327	brca	IDC	f	54	pre
328	brca	IDC	f	36	pre
329	brca	IDC	f	44	pre
330	brca	IDC	f	71	post
331	brca	IDC	f	38	pre
332	brca	IDC	f	27	pre
333	brca	IDC	f	42	pre
334	brca	IDC	f	51	pre
335	brca	DCIS	f	49
336	brca	DCIS	f	96
337	brca	DCIS	f	39
338	benign breast	fibroadenoma	f	36
339	benign breast	fibroadenoma	f	42
340	benign breast	fibroadenoma	f	24
341	benign breast	fibroadenoma	f	27
342	benign breast	fibroadenoma	f	42
343	benign breast	fibroadenoma	f	50
344	benign breast	fibroadenoma	f	43
345	benign breast	fibroadenoma	f	43
346	benign breast	fibroadenoma	f	33
347	benign breast	fibrocystic changes	f	54
348	benign breast	fibrocystic changes	f	61
349	benign breast	fibrocystic disease	f	35
350	benign breast	fibrocystic changes	f	44
351	benign breast	fibrocystic disease	f	45
352	benign breast	Breast Benign Disease	f	45
353	brca	BRCA1	f	44
354	brca	BRCA1	f	31
355	brca	BRCA1	f	39
356	brca	BRCA1	f	32
357	brca	BRCA1	f	44
358	brca	BRCA1	f	35
359	brca	BRCA1	f	32
360	brca	BRCA1	f	32
361	brca	BRCA1	f	29
362	brca	BRCA1	f	47
363	brca	BRCA1	f	49
364	brca	BRCA1	f	37
365	brca	BRCA1	f	32
366	brca	BRCA1	f	50
367	brca	BRCA1	f	35
368	brca	BRCA1	f	56
369	brca	BRCA1	f	49
370	brca	BRCA1	f	44
371	brca	BRCA1	f	45
372	brca	BRCA1	f	37
373	brca	BRCA1	f	37
374	brca	BRCA1	f	29
375	brca	BRCA1	f	41
376	brca	DCIS	f	59
377	brca	IDC	f	61
378	brca	DCIS	f	46
379	brca	DCIS	f	38
380	brca	DCIS	f	45
381	brca	DCIS	f	46
382	benign breast	Normal Breast	f	44
383	brca	DCIS	f	58
384	brca	DCIS	f	52
385	brca	DCIS	f	60
386	brca	DCIS	f	46
387	brca	DCIS	f	60
388	brca	DCIS	f	59
389	brca	DCIS	f	60
390	brca	DCIS	f	62
391	brca	DCIS	f	39
392	brca	DCIS	f	50
393	brca	DCIS	f	62
394	brca	IDC	f	84
395	benign breast	Normal Breast	f	55
396	brca	DCIS	f	41
397	brca	IDC	f	32
398	brca	IDC	f	49
399	brca	DCIS	f	43
400	brca	DCIS	f	48
401	brca	DCIS	f	45
402	brca	IDC	f	33
403	benign breast	Normal Breast	f	71
404	benign breast	Normal Breast	f	40
405	benign breast	Normal Breast	f	40
406	brca	IDC	f	42
407	brca	DCIS	f	—
408	benign breast	Normal Breast	f	—
409	brca	IDC	f	58
410	brca	IDC	f	70
411	brca	DCIS	f	43
412	brca	DCIS	f	83
413	brca	DCIS	f	74
414	brca	DCIS	f	28
415	benign breast	fibroadenoma	f	38
416	benign breast	fibroadenoma	f	39
417	benign breast	fibroadenoma	f	39
418	benign breast	fibroadenoma	f	38
419	benign breast	fibroadenoma	f	51
420	benign breast	fibroadenoma	f	58
421	benign breast	fibroadenoma	f	50
422	benign breast	fibroadenoma	f	58
423	benign breast	fibroadenoma	f	39
424	benign breast	fibroadenoma	f	41
425	benign breast	fibroadenoma	f	15
426	benign breast	fibroadenoma	f	42
427	benign breast	adenosis	f	14
428	benign breast	fibroadenoma	f	26
429	benign breast	Normal Breast	f	31
430	benign breast	fibroadenoma	f	—
431	benign breast	Normal Breast	f	30
432	benign breast	fibroadenoma	f	46
433	benign breast	fibroadenoma	f	53
434	benign breast	fibroadenoma	f	43
435	benign breast	fibroadenoma	f	20
436	benign breast	fibroadenoma	f	44
437	benign breast	Normal Breast	f	45
438	benign breast	fibroadenoma	f	27
439	benign breast	fibroadenoma	f	63
440	benign breast	fibroadenoma	f	44
441	benign breast	fibroadenoma	f	40
442	benign breast	fibroadenoma	f	45
443	benign breast	fibroadenoma	f	41
444	benign breast	fibroadenoma	f	41
445	benign breast	Normal Breast	f	41
446	benign breast	fibroadenoma	f	35
447	benign breast	fibroadenoma	f	33
448	benign breast	fibroadenoma	f	—
449	benign breast	fibroadenoma	f	24
450	benign breast	fibroadenoma	f	—
451	lymphocytes	lymphocytes	f	77
452	lymphocytes	lymphocytes	m	50
453	lymphocytes	lymphocytes	f	74
454	other cancer	colorectal cancer	f	0
455	other cancer	colorectal cancer	f	0
456	lymphocytes	lymphocytes	f	53
457	other cancer	colorectal cancer	f	0
458	lymphocytes	lymphocytes	f	72
459	other cancer	colorectal cancer	f	0
460	other cancer	colorectal cancer	f	0
461	lymphocytes	lymphocytes	f	71
462	lymphocytes	lymphocytes	f	69
463	lymphocytes	lymphocytes	f	53
464	other cancer	colorectal cancer	f	0
465	lymphocytes	lymphocytes	f	51
466	other cancer	colorectal cancer	f	0
467	lymphocytes	lymphocytes	f	50
468	other cancer	colorectal cancer	f	53
469	other cancer	colorectal cancer	f	46
470	other cancer	colorectal cancer	f	62
471	other cancer	colorectal cancer	f	78
472	other cancer	colorectal cancer	f	55
473	other cancer	colorectal cancer	f	53
474	other cancer	colorectal cancer	f	60
475	other cancer	colorectal cancer	f	84
476	other cancer	colorectal cancer	f	69
477	other cancer	colorectal cancer	f	66
478	other cancer	colorectal cancer	f	NA
479	other cancer	colorectal cancer	f	45
480	other cancer	colorectal cancer	f	75
481	other cancer	lung cancer	f	69
482	other cancer	colorectal cancer	f	73
483	other cancer	colorectal cancer	f	73
484	other cancer	colorectal cancer	f	72
485	other cancer	colorectal cancer	m	72
486	other cancer	liver cancer	f	66
487	other cancer	colorectal cancer	m	88
488	other cancer	colorectal cancer	f	65
489	other cancer	colorectal cancer	f	54
490	other cancer	colorectal cancer	m	76
491	other cancer	liver cancer	f	NA
492	other cancer	stomach cancer	f	82
493	other cancer	stomach cancer	f	85
494	other cancer	stomach cancer	f	60
495	other cancer	stomach cancer	f	55
496	other cancer	stomach cancer	f	56
497	other cancer	stomach cancer	f	63
498	other cancer	cancer esophagus	f	57
499	other cancer	cancer esophagus	f	45
500	other cancer	cancer esophagus	f	71

TABLE 15
Sample grading
Sample No.	T	N	M	grade	ER
1
2
3
4
5
6
7
8
9
10
11
12
13
14
15
16
17
18
19
20
21
22
23
24
25
26
27
28
29
30
31
32
33
34
35
36
37
38
39
40
41
42
43
44
45
46
47
48
49
50
51
52
53
54
55
56
57
58
59
60
61
62
63
64
65
66
67
68
69
70
71
72
73
74
75
76
77
78
79
80
81
82
83
84
85
86
87
88
89
90
91
92
93
94
95
96
97
98
99
100
101
102
103
104
105
106
107
108
109
110
111
112
113
114
115	T1	N0	M0	poor	pos
116	T1	N1	M0	poor	pos
117	T1	N1	M0		neg
118	T1	N1	M0		pos
119	T1	N1	M0	poor	neg
120	T1	N0	M0	poor	pos
121	T1	N0	M0	poor	neg
122	T1	N1	M0	poor	neg
123	T1	N1	M0	poor	neg
124	T1	N1	M0	poor	pos
125	T1	N0	M0	poor	pos
126	T1	N1	M0	poor	neg
127	T1	N1	M0	poor	pos
128	T1	N0	M0	poor	neg
129	T1	N0	M0	poor	neg
130	T1	N1	M0		pos
131	T1	N0	M0		pos
132	T1	N1	M0	mod	neg
133	T1	N1	M0	poor	pos
134	T1	N0	M0	mod	pos
135	T1	N0	M0	poor	pos
136	T1	N1	M0	poor	neg
137	T1	N1	M0		pos
138	T1	N1	M0	mod	pos
139	T1	N1	M0	mod	neg
140	T1	N0	M0		pos
141	T1	N0	M0		pos
142	T1	N0	M0		neg
143	T1	N0	M0		pos
144	T1	N0	M0		pos
145	T1	N2	M0	poor	pos
146	T1	N0	M0	mod	pos
147	T1	N0	M0	poor	pos
148	T1	N1	M0	poor	neg
149	T1	N0	M0	mod	pos
150	T1	N1	M0		neg
151	T1	N1	M0	poor	pos
152	T1	N1	M0	poor	neg
153	T1	N1	M0	poor	pos
154	T1	N0	M0	poor	pos
155	T1	N0	M0		neg
156	T1	N0	M0	poor	neg
157	T1	N0	M0		neg
158	T1	N0	M0	poor	neg
159	T1	N1	M0		neg
160	T1	N0	M0	poor	pos
161	T1	N1	M0	poor	neg
162	T1	N1	M0		pos
163	T1	N0	M0		pos
164	T1	N0	M0	poor	pos
165	T1	N1	M0	poor	pos
166	T1	N1	M0	poor	pos
167	T1	N0	M0	poor	neg
168	T1	N0	M0	poor	pos
169	T1	N0	M0	poor	neg
170	T1	N1	M0	poor	neg
171	T1	N0	M0	poor	pos
172	T1	N0	M0	poor	pos
173	T1	N1	M0		pos
174	T1	N0	M0	poor	pos
175	T1	N0	M0		neg
176	T1	N0	M0		pos
177	T1	N0	M0		pos
178	T1	N0	M0	mod	pos
179	T1	N0	M0	poor	neg
180	T1	N0	M0	poor	neg
181	T1	N0	M0	poor	neg
182	T1	N2	M0		pos
183	T1	N0	M0	poor	pos
184	T1	N0	M0		pos
185	T1	N0	M0		pos
186	T1	N0	M0		pos
187	T1	N1	M0		pos
188	T1	N2	M0	poor	pos
189	T1	N0	M0		pos
190	T1	N0	M0	poor	pos
191	T1	N0	M0		neg
192	T1	N1	M0	poor	pos
193	T1	N2	M0	poor	pos
194	T1	N1	M0		pos
195	T1	N0	M0	poor	neg
196	T1	N1	M0		pos
197	T1	N1	M0		pos
198	T1	N1	M0	good	neg
199	T1	N1	M0		neg
200	T1	N0	M0	poor	neg
201	T1	N0	M0		neg
202	T1	N1	M0		pos
203	T1	N0	M0	mod	pos
204	T1	N0	M0		pos
205	T1	N0	M0		pos
206	T1	N0	M0		neg
207	T1	N1	M0		neg
208	T1	N1	M0		pos
209	T1	N1	M0	poor	pos
210	T1	N1	M0	poor	neg
211	T1	N1	M0	poor	neg
212	T1	N1	M0	poor	pos
213	T1	N1	M0	poor	neg
214	T1	N1	M0	poor	pos
215	T1	N1	M0	poor	neg
216	T1	N2	M0	poor	neg
217	T1	N1	M0	mod	pos
218	T1	N1	M0	poor	neg
219	T1	N1	M0		pos
220	T1	N0	M0	poor	neg
221	T1	N0	M0	mod	pos
222	T1	N0	M0	poor	neg
223	T1	N0	M0	mod	pos
224	T1	N0	M0	poor	neg
225	T1	N0	M0		neg
226	T1	N0	M0	poor	neg
227	T1	N1	M0	poor	pos
228	T1	N0	M0	poor	neg
229	T1	N0	M0		pos
230	T1	N1	M0	poor	pos
231	T1	N1	M0	poor	neg
232	T1	N0	M0	poor	neg
233	T1	N2	M0	poor	pos
234	T1	N1	M0		pos
235	T1	N0	M0	poor	pos
236	T1	N1	M0		pos
237	T1	N0	M0		pos
238	T1	N2	M0	mod	pos
239	T1	N0	M0		pos
240	T1	N0	M0		neg
241	T1	N0	M0	poor	pos
242	T1	N1	M0		pos
243	T1	N0	M0		pos
244	T1	N1	M0	poor	pos
245	T1	N0	M0	poor	pos
246	T1	N2	M0	poor	pos
247	T1	N1	M0		pos
248	T1	N0	M0	poor	neg
249	T1	N0	M0	poor	neg
250	T1	N1	M0	mod	neg
251	T1	N1	M0	poor	pos
252	T1	N1	M0	poor	neg
253	T1	N0	M0	poor	pos
254	T1	N1	M0	poor	neg
255	T1	N1	M0		pos
256	T1	N0	M0	mod	pos
257	T1	N1	M0		pos
258	T1	N1	M0	poor	pos
259	T1	N1	M0	mod	pos
260	T1	N0	M0	poor	pos
261	T1	N0	M0		pos
262	T1	N0	M0	poor	neg
263	T1	N0	M0	poor	pos
264	T1	N1	M0		neg
265	T1	N0	M0	poor	neg
266	T1	N1	M0	poor	pos
267	T1	N0	M0		neg
268	T1	N1	M0	poor	pos
269	T1	N1	M0	poor	pos
270	T1	N0	M0	mod	pos
271	T1	N1	M0	poor	pos
272	T1	N0	M0	poor	pos
273	T1	N1	M0	mod	neg
274	T1	N1	M0	poor	neg
275	T1	N1	M0	poor	pos
276	T1	N1	M0	mod	pos
277	T1	N0	M0		pos
278	T1	N0	M0	good	neg
279	T1	N0	M0	poor	neg
280	T1	N0	M0		pos
281	T1	N0	M0	mod	pos
282	T1	N0	M0	mod	pos
283	T1	N0	M0	poor	neg
284	T1	N0	M0	poor	neg
285	T1	N0	M0	poor	neg
286	T1	N0	M0	poor	pos
287	T1	N0	M0		pos
288	T1	N0	M0	poor	neg
289	T1	N1	M0	poor	pos
290	T1	N1	M0	poor	neg
291	T1	N1	M0	poor	neg
292	T1	N1	M0	poor	neg
293	T1	N1	M0	poor	neg
294	T1	N2	M0	poor	neg
295	T1	N1	M0	poor	pos
296	T1	N1	M0	mod	neg
297	T1	N0	M0		neg
298	T1	N1	M0		neg
299	T1	N0	M0		neg
300	T1	N0	M0	poor	neg
301	T1	N1	M0		pos
302	T1	N2	M0	poor	neg
303	T1	N0	M0	mod	pos
304	T1	N1	M0	poor	neg
305	T1	N1	M0	poor	pos
306	T1	N1	M0		neg
307	T1	N0	M0	mod	pos
308	T1	N0	M0	poor	neg
309	T1	N1	M0	poor	neg
310	T1	N1	M0	poor	neg
311	T1	N1	M0		neg
312	T1	N1	M0		neg
313	T1	N2	M0	poor	neg
314	T1	N0	M0		pos
315	T1	N0	M0	mod	neg
316	T1	N1	M0	poor	pos
317	T1	N1	M0	poor	neg
318	T1	N0	M0	mod	pos
319	T1	N0	M0	poor	pos
320	T1	N0	M0		pos
321	T1	N0	M0	mod	neg
322	T1	N0	M0	poor	neg
323	T1	N1	M0		pos
324	T1	N1	M0	poor	neg
325	T1	N0	M0	good	pos
326	T1	N0	M0		pos
327	T1	N0	M0	poor	neg
328	T1	N0	M0	poor	neg
329	T1	N1	M0		pos
330	T1	N0	M0	mod	pos
331	T1	N1	M0	mod	pos
332	T1	N1	M0	poor	neg
333	T1	N0	M0		neg
334	T1	N0	M0	mod	neg
335	Tis	N0	Mx		pos
336	Tis	N0	Mx
337	Tis	N0	Mx
338
339
340
341
342
343
344
345
346
347
348
349
350
351
352
353	T1	N0	M0	poor
354				poor
355
356	T1	N0	M0	poor
357	T1	N0	M0	2e prim, unknown
358	T1	N0	M0	poor
359	T1	N0	M0	unknown
360	T1	N0	M0
361	T1	N0	M0	poor
362	T1	N0	M0
363	T1	N0	M0	LR
364	T1	N0	M0	poor
365	T1	N0	M0	poor
366	T1	N0	M0	poor
367	T1	N0	M0
368	T1	N0	M0
369	T1	N0	M0
370	T1	N0	M0	missing
371	T1	N0	M0	poor
372	T1	N0	M0	poor
373	T1	N0	M0	mod
374	T1	N0	M0	poor
375	T1	N0	M0
376
377
378
379
380
381
382
383				poor
384				poor
385
386
387
388
389				poor
390
391
392
393
394
395
396
397
398
399
400
401
402
403
404
405
406				LR, poor
407
408
409
410
411
412
413
414				poor
415
416
417
418
419
420
421
422
423
424
425
426
427
428
429
430
431
432
433
434
435
436
437
438
439
440
441
442
443
444
445
446
447
448
449
450
451
452
453
454
455
456
457
458
459
460
461
462
463
464
465
466
467
468
469
470
471
472
473
474
475
476
477
478
479
480
481
482
483
484
485
486
487
488
489
490
491
492
493
494
495
496
497
498
499
500

TABLE 16
Breast cancer vs. all other controls
No:	Gene	Oligo:
1	SCGB3A1	TAGTGTTCGACGTTGT
	(SEQ ID NO: 115)	(SEQ ID NO: 1475)
2	SCGB3A1	TAGTGTTTGATGTTGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 1476)
3	SASH1	TAGATTCGAGGTGCGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1477)
4	SASH1	TAGATTTGAGGTGTGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1478)
5	SASH1	TAGATTCGAGGTGCGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1477)
6	SASH1	TAGATTTGAGGTGTGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1478)
7	SASH1	ATTCGGTATTCGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1479)
8	SASH1	ATTTGGTATTTGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1480)
9	SASH1	ATTCGGTATTCGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1479)
10	SASH1	ATTTGGTATTTGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1480)
11	SASH1	AGTCGGAATCGGAGTT
	(SEQ ID NO: 102)	(SEQ ID NO: 1481)
12	SASH1	GTTGGAATTGGAGTTTA
	(SEQ ID NO: 102)	(SEQ ID NO: 1482)
13	ARH1/NOEY2	TGTTATCGTTAACGATT
	(SEQ ID NO: 97)	(SEQ ID NO: 1483)
14	ARH1/NOEY2	AGGTGTTATTGTTAATGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1484)
15	ARH1/NOEY2	TAAAACGTTCGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1485)
16	ARH1/NOEY2	TTTAAAATGTTTGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1486)
17	ARH1/NOEY2	TGTATTCGTCGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1487)
18	ARH1/NOEY2	AATGTATTTGTTGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1488)
19	ARH1/NOEY2	TTAGACGGAGTTCGGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1489)
20	ARH1/NOEY2	TAGATGGAGTTTGGAGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1490)
21	ARH1/NOEY2	TAGACGTAGGCGTATT
	(SEQ ID NO: 97)	(SEQ ID NO: 1491)
22	ARH1/NOEY2	GGGTAGATGTAGGTGT
	(SEQ ID NO: 97)	(SEQ ID NO: 1492)
23	CCND2	TTAGGGTCGATCGTGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1493)
24	CCND2	TAGGGTTGATTGTGTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1494)
25	CCND2	TTATCGTAGTCGGTTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1495)
26	CCND2	GATTTTATTGTAGTTGGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1496)
27	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1497)
28	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1498)
29	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1497)
30	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1498)
31	CCND2	AAGGATCGAGCGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1499)
32	CCND2	AAGGATTGAGTGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1500)
33	CCND2	AAGGATCGAGCGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1499)
34	CCND2	AAGGATTGAGTGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1500)
35	CDKN1A	ATTAGGGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1501)
36	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1502)
37	CDKN1A	ATTAGGGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1501)
38	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1502)
39	CDKN2A	GGCGTTGTTTAACGTAT
	(SEQ ID NO: 57)	(SEQ ID NO: 1503)
40	CDKN2A	GGGTGTTGTTTAATGTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1504)
41	CDKN2A	AATAGTTACGGTCGGA
	(SEQ ID NO: 57)	(SEQ ID NO: 1505)
42	CDKN2A	AGTTATGGTTGGAGGT
	(SEQ ID NO: 57)	(SEQ ID NO: 1506)
43	CDKN2A	GTCGGAGGTCGATTTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1507)
44	CDKN2A	GGTTGGAGGTTGATTTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1508)
45	DAPK1	TTTCGGAGATTCGGTT
	(SEQ ID NO: 98)	(SEQ ID NO: 1509)
46	DAPK1	TTTGGAGATTTGGTTTT
	(SEQ ID NO: 98)	(SEQ ID NO: 1510)
47	DAPK1	TTTTAGCGTCGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1511)
48	DAPK1	TTTTAGTGTTGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1512)
49	DAPK1	TTTTAGCGTCGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1511)
50	DAPK1	TTTTAGTGTTGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1512)
51	EYA4	GGTATAAAATCGTAAATTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1513)
52	EYA4	GGGTATAAAATTGTAAATTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1514)
53	EYA4	TATGTAGTCGCGTAGT
	(SEQ ID NO: 58)	(SEQ ID NO: 1515)
54	EYA4	TTTATGTAGTTGTGTAGT
	(SEQ ID NO: 58)	(SEQ ID NO: 1516)
55	EYA4	GTTTAGATACGAAATGTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1517)
56	EYA4	GTTTAGATATGAAATGTTAT
	(SEQ ID NO: 58)	(SEQ ID NO: 1518)
57	EYA4	AGTTTTGACGTCGTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1519)
58	EYA4	TTGATGTTGTTTTGGAA
	(SEQ ID NO: 58)	(SEQ ID NO: 1520)
59	FHIT	GTTACGTTAGCGGGTT
	(SEQ ID NO: 76)	(SEQ ID NO: 1521)
60	FHIT	GGTTATGTTAGTGGGT
	(SEQ ID NO: 76)	(SEQ ID NO: 1522)
61	FHIT	TTCGGGGACGTTATAG
	(SEQ ID NO: 76)	(SEQ ID NO: 1523)
62	FHIT	GGTTTGGGGATGTTAT
	(SEQ ID NO: 76)	(SEQ ID NO: 1524)
63	GSTP1	GGCGATTTCGGGGATT
	(SEQ ID NO: 59)	(SEQ ID NO: 1525)
64	GSTP1	GGTGATTTTGGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1526)
65	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1527)
66	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1528)
67	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1527)
68	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1528)
69	GSTP1	AGTTCGCGGGATTTTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1529)
70	GSTP1	GGAGTTTGTGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1530)
71	GSTP1	AGTTTTCGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1531)
72	GSTP1	TAGTTTTTGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1532)
73	HIC1	TATCGAAGTTTTCGGG
	(SEQ ID NO: 85)	(SEQ ID NO: 1533)
74	HIC1	TATTGAAGTTTTTGGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1534)
75	HIC1	TAGCGGTTATTTCGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1535)
76	HIC1	TTTAGTGGTTATTTTGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1536)
77	HIC1	TACGTTTTTCGTAGCGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1537)
78	HIC1	ATTATGTTTTTTGTAGTGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1538)
79	HIC1	TTCGGTTTTGTCGTATA
	(SEQ ID NO: 85)	(SEQ ID NO: 1539)
80	HIC1	TTTGGTTTTGTTGTATAG
	(SEQ ID NO: 85)	(SEQ ID NO: 1540)
81	MLH1	AGGCGGCGATAGATTA
	(SEQ ID NO: 89)	(SEQ ID NO: 1541)
82	MLH1	ATGAGGTGGTGATAGA
	(SEQ ID NO: 89)	(SEQ ID NO: 1542)
83	PGR	TTTCGAGGTCGGATTT
	(SEQ ID NO: 83)	(SEQ ID NO: 1543)
84	PGR	TTTGAGGTTGGATTTTT
	(SEQ ID NO: 83)	(SEQ ID NO: 1544)
85	PGR	GTGTCGTTTAGTCGTA
	(SEQ ID NO: 83)	(SEQ ID NO: 1545)
86	PGR	GTTGTTTAGTTGTAGGT
	(SEQ ID NO: 83)	(SEQ ID NO: 1546)
87	PGR	TTTTTTCGACGAAAAGA
	(SEQ ID NO: 83)	(SEQ ID NO: 1547)
88	PGR	AGGATTTTTTTGATGAAA
	(SEQ ID NO: 83)	(SEQ ID NO: 1548)
89	SERPINB5	TTATTAACGTGTTTGAGA
	(SEQ ID NO: 68)	(SEQ ID NO: 1549)
90	SERPINB5	TTATTAATGTGTTTGAGAA
	(SEQ ID NO: 68)	(SEQ ID NO: 1550)
91	SERPINS5	ATTGTCGTACGTATGT
	(SEQ ID NO: 68)	(SEQ ID NO: 1551)
92	SERPINB5	AGAGGATTGTTGTATGTA
	(SEQ ID NO: 68)	(SEQ ID NO: 1552)
93	SERPINB5	TTTTTTGTTCGAATATGT
	(SEQ ID NO: 68)	(SEQ ID NO: 1553)
94	SERPINE5	TTTGTTTGAATATGTTGG
	(SEQ ID NO: 68)	(SEQ ID NO: 1554)
95	RARB	ATGTCGAGAACGCGAG
	(SEQ ID NO: 88)	(SEQ ID NO: 1555)
96	RARB	GGATGTTGAGAATGTGA
	(SEQ ID NO: 88)	(SEQ ID NO: 1556)
97	RARB	AGCGATTCGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1557)
98	RARB	AGTGATTTGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1558)
99	RARB	AGCGATTCGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1557)
100	RARB	AGTGATTTGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1558)
101	RARB	TAGGATTCGGAACGTA
	(SEQ ID NO: 88)	(SEQ ID NO: 1559)
102	RARB	GGTAGGATTTGGAATGT
	(SEQ ID NO: 88)	(SEQ ID NO: 1560)
103	SFN	TAGTACGGTGTCGTAT
	(SEQ ID NO: 69)	(SEQ ID NO: 1561)
104	SFN	GTTTAGTATGGTGTTGT
	(SEQ ID NO: 69)	(SEQ ID NO: 1562)
105	SFN	TACGTATTTCGGGTTT
	(SEQ ID NO: 69)	(SEQ ID NO: 1563)
106	SFN	TATTTATGTATTTTGGGTT
	(SEQ ID NO: 69)	(SEQ ID NO: 1564)
107	SFN	TTCGTTTTTCGTAGGAG
	(SEQ ID NO: 69)	(SEQ ID NO: 1565)
108	SFN	TTTGTTTTTTGTAGGAGA
	(SEQ ID NO: 69)	(SEQ ID NO: 1566)
109	TGFBR2	ATGGGGCGGACGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1567)
110	TGFBR2	ATGGGGTGGATGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1568)
111	TGFBR2	ATGGGGCGGACGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1567)
112	TGFBR2	ATGGGGTGGATGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1568)
113	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1569)
114	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1570)
115	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1569)
116	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1570)
117	TIMP3	TTATTAACGGAGGAAGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1571)
118	TIMP3	TATTAATGGAGGAAGGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1572)
119	TIMP3	TTCGTTATGTGTACGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1573)
120	TIMP3	TTTGTTATGTGTATGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1574)
121	TIMP3	TTCGTTATGTGTACGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1573)
122	TIMP3	TTTGTTATGTGTATGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1574)
123	TIMP3	GAGTATTTCGAGTTTGT
	(SEQ ID NO: 103)	(SEQ ID NO: 1575)
124	TIMP3	AGTATTTTGAGTTTGTATT
	(SEQ ID NO: 103)	(SEQ ID NO: 1576)
125	TIMP3	TAAGCGTTAATCGAGT
	(SEQ ID NO: 103)	(SEQ ID NO: 1577)
126	TIMP3	TAGGTAAGTGTTAATTGA
	(SEQ ID NO: 103)	(SEQ ID NO: 1578)
127	TP73	TAGGATTCGCGTTTTT
	(SEQ ID NO: 86)	(SEQ ID NO: 1579)
128	TP73	GGTAGGATTTGTGTTTT
	(SEQ ID NO: 86)	(SEQ ID NO: 1580)
129	TP73	TTTCGGAGTTGCGAGT
	(SEQ ID NO: 86)	(SEQ ID NO: 1581)
130	TP73	TAGTTTTGGAGTTGTGA
	(SEQ ID NO: 86)	(SEQ ID NO: 1582)
131	CDH13	TAAAACGAGGGAGCGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1583)
132	CDH13	AAAATGAGGGAGTGTT
	(SEQ ID NO: 70)	(SEQ ID NO: 1584)
133	CDH13	TAGTCGCGTGTATGAA
	(SEQ ID NO: 70)	(SEQ ID NO: 1585)
134	CDH13	TGTAGTTGTGTGTATGA
	(SEQ ID NO: 70)	(SEQ ID NO: 1586)
135	CDH13	ATGAAAACGTCGTCGG
	(SEQ ID NO: 70)	(SEQ ID NO: 1587)
136	CDH13	AATGAAAATGTTGTTGG
	(SEQ ID NO: 70)	(SEQ ID NO: 1588)
137	CDH13	TAGTCGAGAATTTCGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1589)
138	CD513	TGTAGTTGAGAATTTTGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1590)
139	TMS1/ASC	TTCGTTTCGGAGTCGA
	(SEQ ID NO: 84)	(SEQ ID NO: 1591)
140	TMS1/ASC	TTTGTTTTGGAGTTGAT
	(SEQ ID NO: 84)	(SEQ ID NO: 1592)
141	APAF1	GTGTCGTAGCGGTATT
	(SEQ ID NO: 82)	(SEQ ID NO: 1593)
142	APAF1	GGTGTTGTAGTGGTAT
	(SEQ ID NO: 82)	(SEQ ID NO: 1594)
143	APAF1	AGTAGCGTCGGGTTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1595)
144	APAF1	GAGTAGTGTTGGGTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1596)
145	SYK	GAAGTTATCGCGTTGG
	(SEQ ID NO: 60)	(SEQ ID NO: 1597)
146	SYK	AGAAGTTATTGTGTTGG
	(SEQ ID NO: 60)	(SEQ ID NO: 1598)
147	SYK	GATCGATGCGGTTTAT
	(SEQ ID NO: 60)	(SEQ ID NO: 1599)
148	SYK	GGGATTGATGTGGTTT
	(SEQ ID NO: 60)	(SEQ ID NO: 1600)
149	SYK	GGCGTTTTAGTCGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1601)
150	SYK	GGTGTTTTAGTTGATTTT
	(SEQ ID NO: 60)	(SEQ ID NO: 1602)
151	SYK	TTATTCGGTCGGGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1603)
152	SYK	TTTATTTGGTTGGGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1604)
153	FABP3	GATGGGCGTATTAGTT
	(SEQ ID NO: 77)	(SEQ ID NO: 1605)
154	FABP3	GGGATGGGTGTATTAG
	(SEQ ID NO: 77)	(SEQ ID NO: 1606)
155	FABP3	GTGATGCGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1607)
156	FABP3	GTGATGTGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1608)
157	FABP3	GTGATGCGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1607)
158	FABP3	GTGATGTGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1608)
159	FABP3	TAAAGCGGTAGTTCGG
	(SEQ ID NO: 77)	(SEQ ID NO: 1609)
160	FABP3	AAGTGGTAGTTTGGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1610)
161	FABP3	TATTGGCGTTGACGTA
	(SEQ ID NO: 77)	(SEQ ID NO: 1611)
162	FABP3	TGGTGTTGATGTAGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1612)
163	RASSF1A	TACGGGTATTTTCGCGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1613)
164	RASSF1A	ATATGGGTATTTTTGTGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1614)
165	RASSF1A	AGAGCGCGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1615)
166	RASSF1A	GAGAGTGTGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1616)
167	RASSF1A	AGTAAATCGGATTAGGA
	(SEQ ID NO: 90)	(SEQ ID NO: 1617)
168	RASSF1A	AGTAAATTGGATTAGGAG
	(SEQ ID NO: 90)	(SEQ ID NO: 1618)
169	TWIST	AGTAAAGGCGTTGCGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1619)
170	TWIST	AGTAAAGGTGTTGTGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1620)
171	TWIST	AGTAAAGGCGTTGCGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1619)
172	TWIST	AGTAAAGGTGTTGTGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1620)
173	TWIST	TATTTTTCGAGGCGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1621)
174	TWIST	TTTTGAGGTGTAGTTTT
	(SEQ ID NO: 100)	(SEQ ID NO: 1622)
175	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1623)
176	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1624)
177	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1623)
178	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1624)
179	TWIST	TAGGTCGGGACGTAAA
	(SEQ ID NO: 100)	(SEQ ID NO: 1625)
180	TWIST	AGTAGGTTGGGATGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1626)
181	ESR2	GAGTATTTTCGAATCGA
	(SEQ ID NO: 91)	(SEQ ID NO: 1627)
182	ESR2	GGAGTATTTTTGAATTGA
	(SEQ ID NO: 91)	(SEQ ID NO: 1628)
183	ESR2	ATAAGCGATTTAACGAT
	(SEQ ID NO: 91)	(SEQ ID NO: 1629)
184	ESR2	AAGTGATTTAATGATAAGT
	(SEQ ID NO: 91)	(SEQ ID NO: 1630)
185	ESR2	TTTACGTGATCGAGTT
	(SEQ ID NO: 91)	(SEQ ID NO: 1631)
186	ESR2	AGTTTATGTGATTGAGTT
	(SEQ ID NO: 91)	(SEQ ID NO: 1632)
187	PLAU	TATTTGTCGCGTTGAT
	(SEQ ID NO: 62)	(SEQ ID NO: 1633)
188	PLAU	ATTTGTTGTGTTGATGA
	(SEQ ID NO: 62)	(SEQ ID NO: 1634)
189	PLAU	TGTAATTCGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1635)
190	PLAU	TTGTAATTTGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1636)
191	PLAU	TTGGAGATCGCGTTTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1637)
192	PLAU	TTGGAGATTGTGTTTTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1638)
193	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1639)
194	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1640)
195	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1639)
196	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1640)
197	STAT1	GTTATTTTCGAGAGTTG
	(SEQ ID NO: 109)	(SEQ ID NO: 1641)
198	STAT1	GTTATTTTTGAGAGTTGT
	(SEQ ID NO: 109)	(SEQ ID NO: 1642)
199	BRCA1	AGTTTCGAGAGACGTT
	(SEQ ID NO: 66)	(SEQ ID NO: 1643)
200	BRCA1	AGAGTTTTGAGAGATGT
	(SEQ ID NO: 66)	(SEQ ID NO: 1644)
201	BRCA1	TTTCGTGGTAACGGAA
	(SEQ ID NO: 66)	(SEQ ID NO: 1645)
202	BRCA1	TTTGTGGTAATGGAAAA
	(SEQ ID NO: 66)	(SEQ ID NO: 1646)
203	BRCA1	AAAGCGCGGGAATTAT
	(SEQ ID NO: 66)	(SEQ ID NO: 1647)
204	BRCA1	GGAAAAGTGTGGGAAT
	(SEQ ID NO: 66)	(SEQ ID NO: 1648)
205	LOT1	ATGGGTACGTTTAAGG
	(SEQ ID NO: 95)	(SEQ ID NO: 1649)
206	LOT1	TGGGTATGTTTAAGGG
	(SEQ ID NO: 95)	(SEQ ID NO: 1650)
207	LOT1	AAATTAGTTACGTTATTTAA
	(SEQ ID NO: 95)	(SEQ ID NO: 1651)
208	LOT1	TGAAATTAGTTATGTTATTTA
	(SEQ ID NO: 95)	(SEQ ID NO: 1652)
209	LOT1	ATGTCGGTTATTACGT
	(SEQ ID NO: 95)	(SEQ ID NO: 1653)
210	LOT1	TGTTGGTTATTATGTAGA
	(SEQ ID NO: 95)	(SEQ ID NO: 1654)
211	PRSS8	AGTTGGCGGAGTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1655)
212	PRSS8	AGTTGGTGGAGTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1656)
213	PRSS8	AGTTGGCGGAGTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1655)
214	PRSS8	AGTTGGTGGAGTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1656)
215	PRSS8	TTGGTGATTCGTTTATAT
	(SEQ ID NO: 72)	(SEQ ID NO: 1657)
216	PRSS8	GTTGGTGATTTGTTTATA
	(SEQ ID NO: 72)	(SEQ ID NO: 1658)
217	PRSS8	TGTTCGTTTCGGATAT
	(SEQ ID NO: 72)	(SEQ ID NO: 1659)
218	PRSS8	TTTGTTTTGGATATTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1660)
219	TPM1	TTGATTCGCGTTCGTA
	(SEQ ID NO: 110)	(SEQ ID NO: 1661)
220	TPM1	TGATTTGTGTTTGTAGA
	(SEQ ID NO: 110)	(SEQ ID NO: 1662)
221	SLC19A1	GTCGTGCGGTTTTTAA
	(SEQ ID NO: 116)	(SEQ ID NO: 1663)
222	SLC19A1	GGTTGTGTGGTTTTTAA
	(SEQ ID NO: 116)	(SEQ ID NO: 1664)
223	SLC19A1	TTAGGAAGGCGGTTTA
	(SEQ ID NO: 116)	(SEQ ID NO: 1665)
224	SLC19A1	TTTTATGAAGGTGGTTT
	(SEQ ID NO: 116)	(SEQ ID NO: 1666)
225	GJB2	GGATTTCGTCGGTATT
	(SEQ ID NO: 111)	(SEQ ID NO: 1667)
226	GJB2	GGGGATTTTGTTGGTA
	(SEQ ID NO: 111)	(SEQ ID NO: 1668)
227	GJB2	GAATTTCGTTTACGGT
	(SEQ ID NO: 111)	(SEQ ID NO: 1669)
228	GJB2	TTGAATTTTGTTTATGGT
	(SEQ ID NO: 111)	(SEQ ID NO: 1670)
229	HS3ST2	GAATCGGAGAGGCGAG
	(SEQ ID NO: 113)	(SEQ ID NO: 1671)
230	HS3ST2	AATTGGAGAGGTGAGG
	(SEQ ID NO: 113)	(SEQ ID NO: 1672)
231	HS3ST2	GGGTAATCGTTTGGTA
	(SEQ ID NO: 113)	(SEQ ID NO: 1673)
232	HS3ST2	GGGTAATTGTTTGGTAT
	(SEQ ID NO: 113)	(SEQ ID NO: 1674)
233	PRDM2	TGTAGAGACGACGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1675)
234	PRDM2	ATTGTAGAGATGATGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1676)
235	PRDM2	AGAGCGCGGTAGTAGT
	(SEQ ID NO: 114)	(SEQ ID NO: 1677)
236	PRDM2	TGAGAGTGTGGTAGTA
	(SEQ ID NO: 114)	(SEQ ID NO: 1678)
237	PRDM2	TGTTCGCGATGTTTTA
	(SEQ ID NO: 114)	(SEQ ID NO: 1679)
238	PRDM2	TGTTTGTGATGTTTTAGT
	(SEQ ID NO: 114)	(SEQ ID NO: 1680)
239	PRDM2	AGTATATAAACGTAGATTTT
	(SEQ ID NO: 114)	(SEQ ID NO: 1681)
240	PRDM2	AAGTATATAAATGTAGATTTT
	(SEQ ID NO: 114)	(SEQ ID NO: 1682)
241	ALX4	AAGTCGATCGTTTTGT
	(SEQ ID NO: 64)	(SEQ ID NO: 1683)
242	ALM	TGGAAGTTGATTGTTTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1684)
243	ALX4	TATTGCGAGGATTCGG
	(SEQ ID NO: 64)	(SEQ ID NO: 1685)
244	ALX4	ATTGTGAGGATTTGGT
	(SEQ ID NO: 64)	(SEQ ID NO: 1686)
245	ALX4	TTCGTAGCGTAGGGTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1687)
246	ALX4	TTTGTAGTGTAGGGTTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1688)
247	S100A7	TATAGTCGGGGTGATA
	(SEQ ID NO: 96)	(SEQ ID NO: 1689)
248	S100A7	TTTATAGTTGGGGTGAT
	(SEQ ID NO: 96)	(SEQ ID NO: 1690)
249	S100A7	AGTCGGGCGTTAGTAA
	(SEQ ID NO: 96)	(SEQ ID NO: 1691)
250	S100A7	GAGTTGGGTGTTAGTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1692)
251	S100A7	GGATGGCGGAAGTTTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1693)
252	S100A7	GGATGGTGGAAGTTTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1694)
253	$100A7	GGATGGCGGAAGTTTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1693)
254	S100A7	GGATGGTGGAAGTTTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1694)
255	APC	GATTCGTATTTCGTAGT
	(SEQ ID NO: 65)	(SEQ ID NO: 1695)
256	APC	GATTCGTATTTCGTAGT
	(SEQ ID NO: 65)	(SEQ ID NO: 1695)
257	APC	AGCGTTTTGGTTCGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1696)
258	APC	AGTGTTTTGGTTTGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1697)
259	APC	AGCGTTTTGGTTCGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1696)
260	APC	AGTGTTTTGGTTTGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1697)
261	APC	TTAATCGGCGGGTTTT
	(SEQ ID NO: 65)	(SEQ ID NO: 1698)
262	APC	AGTTAATTGGTGGGTT
	(SEQ ID NO: 65)	(SEQ ID NO: 1699)
263	APC	ATTTTCGAGTTCGGTA
	(SEQ ID NO: 65)	(SEQ ID NO: 1700)
264	APC	TTTTTGAGTTTGGTAGT
	(SEQ ID NO: 65)	(SEQ ID NO: 1701)
265	BRCA2	ATTCGTTTTAGAGGCGTA
	(SEQ ID NO: 56)	(SEQ ID NO: 1702)
266	BRCA2	ATTTGTTTTAGAGGTGTA
	(SEQ ID NO: 56)	(SEQ ID NO: 1703)
267	BRCA2	ATTCGTTTTAGAGGCGTA
	(SEQ ID NO: 56)	(SEQ ID NO: 1702)
268	BRCA2	ATTTGTTTTAGAGGTGTA
	(SEQ ID NO: 56)	(SEQ ID NO: 1703)
269	SEQ ID NO: 2	TAGGTATACGAAAGAGTA
	(SEQ ID NO: 2)	(SEQ ID NO: 1704)
270	SEQ ID NO: 2	TTAGGTATATGAAAGAGTA
	(SEQ ID NO: 2)	(SEQ ID NO: 1705)
271	SEQ ID NO: 2	TTGATTGGCGGACGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1706)
272	SEQ ID NO: 2	TTGATTGGTGGATGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1707)
273	SEQ ID NO: 2	TTGATTGGCGGACGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1706)
274	SEQ ID NO: 2	TTGATTGGTGGATGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1707)
275	IGFBP7	TAGTCGCGGAATGTTA
	(SEQ ID NO: 94)	(SEQ ID NO: 1708)
276	IGFBP7	TTGGTAGTTGGGAAT
	(SEQ ID NO: 94)	(SEQ ID NO: 1709)
277	IGFBP7	ATTTTTTCGCGGGTAT
	(SEQ ID NO: 94)	(SEQ ID NO: 1710)
278	IGFBP7	TTTTTGTGGGTATTTTAG
	(SEQ ID NO: 94)	(SEQ ID NO: 1711)
279	IGFBP7	GGTATATTCGACGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1712)
280	IGFBP7	GGGTATATTTGATGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1713)
281	IGFBP7	GGTACGAGCGTTTTTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1710)
282	IGFBP7	TGGGTATGAGTGTTTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1715)
283	IGFBP7	AAAGCGTATTTAATTCGT
	(SEQ ID NO: 94)	(SEQ ID NO: 1716)
284	IGFBP7	AGTGTATTTAATTTGTGTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1717)
285	SOD2	GTCGTTTAGTCGGTTTA
	(SEQ ID NO: 105)	(SEQ ID NO: 1718)
286	SOD2	GTTGTTTAGTTGGTTTAT
	(SEQ ID NO: 105)	(SEQ ID NO: 1719)
287	SOD2	TATTAGGCGGTTGCGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1720)
288	SOD2	TATTAGGTGGTTGTGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1721)
289	SOD2	TATTAGGCGGTTGCGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1720)
290	SOD2	TATTAGGTGGTTGTGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1721)
291	SOD2	TACGGTTCGAAGGTTT
	(SEQ ID NO: 105)	(SEQ ID NO: 1722)
292	SOD2	AGTTGGTATGGTTTGA
	(SEQ ID NO: 105)	(SEQ ID NO: 1723)
293	NME1	AATTCGAGATTAGTTCGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1724)
294	NME1	AATTTGAGATTAGTTTGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1725)
295	NME1	AATTCGAGATTAGTTCGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1724)
296	NME1	AATTTGAGATTAGTTTGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1725)
297	THES1	TAAAGGGGCGTTCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1726)
298	THBS1	AAGGGGTGTTTGTATT
	(SEQ ID NO: 81)	(SEQ ID NO: 1727)
299	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1728)
300	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1729)
301	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1728)
302	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1729)
303	THBS1	TTGTGCGTTCGGAGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1730)
304	THBS1	TGTGTTTGGAGTAGAG
	(SEQ ID NO: 81)	(SEQ ID NO: 1731)
305	ESR1	AAATCGGCGGGTTATT
	(SEQ ID NO: 75)	(SEQ ID NO: 1732)
306	ESR1	AGAAATTGGTGGGTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1733)
307	ESR1	AGTTGCGGACGGTTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1734)
308	ESR1	AGTTGTGGATGGTTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1735)
309	ESR1	AGTTGCGGACGGTTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1734)
310	ESR1	AGTTGTGGATGGTTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1735)
311	IL6	TTCGGTTATACGTAGG
	(SEQ ID NO: 99)	(SEQ ID NO: 1736)
312	IL6	TTTTGGTTATATGTAGGG
	(SEQ ID NO: 99)	(SEQ ID NO: 1737)
313	IL6	AGTTTAGTCGGTTTCGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1738)
314	IL6	AGTTTAGTTGGTTTTGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1739)
315	IL6	AGTTTAGTCGGTTTCGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1738)
316	IL6	AGTTTAGTTGGTTTTGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1739)
317	CASP8	TGTATTCGAGGCGGTA
	(SEQ ID NO: 71)	(SEQ ID NO: 1740)
318	CASP8	TTGTATTTGAGGTGGT
	(SEQ ID NO: 71)	(SEQ ID NO: 1741)
319	CASP8	ATTTTTTAAACGGGTTTA
	(SEQ ID NO: 71)	(SEQ ID NO: 1742)
320	CASP8	TTTTAAATGGGTTTATAGG
	(SEQ ID NO: 71)	(SEQ ID NO: 1743)
321	CASP8	ATCGTAGTTTTCCAGT
	(SEQ ID NO: 71)	(SEQ ID NO: 1744)
322	CASP8	ATTGTAGTTTTTGAGTTT
	(SEQ ID NO: 71)	(SEQ ID NO: 1745)
323	HOXA5	TTCGAGTTCGGTTGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1746)
324	HOXA5	GTTTGAGTTTGGTTGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1747)
325	HOXA5	TAGTTTTCGGTCGGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1748)
326	HOXA5	TAGTTTTTGGTTGGAAG
	(SEQ ID NO: 78)	(SEQ ID NO: 1749)
327	HOXA5	TAATTCGATTTCGGTTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1750)
328	HOXA5	TTTAATTTGATTTTGGTTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1751)
329	HOXA5	ATCGGTAGTTGACGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1752)
330	HOXA5	ATTGGTAGTTGATGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1753)
331	HOXA5	ATCGGTAGTTGACGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1752)
332	HOXA5	ATTGGTAGTTGATGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1753)
333	RARA	TTCGGGATGTACGTTT
	(SEQ ID NO: 108)	(SEQ ID NO: 1754)
334	RARA	TTTGGGTGTATGTTTT
	(SEQ ID NO: 108)	(SEQ ID NO: 1755)
335	RARA	GAATTAGTATCGGTTTTT
	(SEQ ID NO: 108)	(SEQ ID NO: 1756)
336	RARA	ATTAGTATTGGTTTTTGG
	(SEQ ID NO: 108)	(SEQ ID NO: 1757)
337	SNCG	TGCGGTAGTATTCGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1758)
338	SNCG	TGTGGTAGTATTTGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1759)
339	SNCG	TGCGGTAGTATTCGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1758)
340	SNCG	TGTGGTAGTATTTGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1759)
341	GPC3	AATAGTCGCGTTTAGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1760)
342	GPC3	TAGTTGTGTTTAGGGAT
	(SEQ ID NO: 118)	(SEQ ID NO: 1761)
343	GPC3	TTTAACGTAGTTTTGATCGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1762)
344	GPC3	TTTAATGTAGTTTTGATGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1763)
345	GPC3	TTTAACGTAGTTTTGATCGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1762)
346	GPC3	TTTAATGTAGTTTTGATTGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1763)
347	CLDN7	TTACGTTAAGTCGGGT
	(SEQ ID NO: 87)	(SEQ ID NO: 1764)
348	CLDN7	AGTTATGTTAAGTTGGG
	(SEQ ID NO: 87)	(SEQ ID NO: 1765)
349	CLDN7	TAGCGTTTTAGGCGTA
	(SEQ ID NO: 87)	(SEQ ID NO: 1766)
350	CLDN7	TAGTGTTTTAGGTGTATT
	(SEQ ID NO: 87)	(SEQ ID NO: 1767)
351	CLDN7	TTAGGGGCGTTTCGTA
	(SEQ ID NO: 87)	(SEQ ID NO: 1768)
352	CLDN7	TTAGGGGTGTTTTGTAG
	(SEQ ID NO: 87)	(SEQ ID NO: 1769)
353	CLDN7	TAGAATTCGGCGGGGA
	(SEQ ID NO: 87)	(SEQ ID NO: 1770)
354	CLDN7	TAGAATTTGGTGGGGA
	(SEQ ID NO: 87)	(SEQ ID NO: 1771)
355	CLDN7	TAGAATTCGGCGGGGA
	(SEQ ID NO: 87)	(SEQ ID NO: 1770)
356	CLDN7	TAGAATTTGGTGGGGA
	(SEQ ID NO: 87)	(SEQ ID NO: 1771)
357	SLIT2	TTCGATAGTTAACGATG
	(SEQ ID NO: 112)	(SEQ ID NO: 1772)
358	SLIT2	TTTGATAGTTAATGATGGT
	(SEQ ID NO: 112)	(SEQ ID NO: 1773)
359	SLIT2	ATTTCGTCGTAGTTTG
	(SEQ ID NO: 112)	(SEQ ID NO: 1774)
360	SLIT2	TTTTGTTGTAGTTTGGA
	(SEQ ID NO: 112)	(SEQ ID NO: 1775)
361	SLIT2	TAGCGGGTTCGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1776)
362	SLIT2	TTAGTGGGTTTGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1777)
363	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1778)
364	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1779)
365	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1778)
366	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1779)
367	IGSF4	AGGTAGATCGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1780)
368	IGSF4	AGGTAGATTGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1781)
369	IGSF4	AGGTAGATCGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1780)
370	IGSF4	AGGTAGATTGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1781)
371	IGSF4	TAGTCGTAGAGTCGGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1782)
372	IGSF4	GTTGTAGAGTTGGGTT
	(SEQ ID NO: 74)	(SEQ ID NO: 1783)
373	IGSF4	TAGGTTTTCGGATTGA
	(SEQ ID NO: 74)	(SEQ ID NO: 1784)
374	IGSF4	GTAGGTTTTTGGATTGA
	(SEQ ID NO: 74)	(SEQ ID NO: 1785)
375	MCT1	ATTTTACGTAGGCGTT
	(SEQ ID NO: 101)	(SEQ ID NO: 1786)
376	MCT1	GATTTTATGTAGGTGTTT
	(SEQ ID NO: 101)	(SEQ ID NO: 1787)
377	MCT1	AGTTAGTCGCGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1788)
378	MCT1	AGAGTTAGTTGTGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1789)
379	MCT1	TATACGAGGAAGGTCGG
	(SEQ ID NO: 101)	(SEQ ID NO: 1790)
380	MCT1	TATATGAGGAAGGTTGG
	(SEQ ID NO: 101)	(SEQ ID NO: 1791)
381	MCT1	TATACGAGGAAGGTCGG
	(SEQ ID NO: 101)	(SEQ ID NO: 1790)
382	MCT1	TATATGAGGAAGGTTGG
	(SEQ ID NO: 101)	(SEQ ID NO: 1791)
383	SEQ ID NO: 6	AAGTTTATCGGCGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1792)
384	SEQ ID NO: 6	AGAAGTTTATTGGTGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1793)
385	SEQ ID NO: 6	ATTTCGGAATTTAAGCGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1794)
386	SEQ ID NO: 6	TTTTGGAATTTAAGTGTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1795)
387	SEQ ID NO: 6	TAATTTCGGACGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1796)
388	SEQ ID NO: 6	TTTTGGATGTGGAGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1797)
389	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1798)
390	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1799)
391	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1798)
392	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1799)
393	SEQ ID NO: 6	TTTCGGTTTTCGTTAAT
	(SEQ ID NO: 6)	(SEQ ID NO: 1800)
394	SEQ ID NO: 6	TTTGGTTTTTGTTAATTTAG
	(SEQ ID NO: 6)	(SEQ ID NO: 1801)
395	SEQ ID NO: 6	TGTGCGAAGTTAACGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1802)
396	SEQ ID NO: 6	TTGTGTGAAGTTAATGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1803)
397	SEQ ID NO: 8	ATAAAGCGGGGTTTTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1804)
398	SEQ ID NO: 8	GGATATAGTGGGGTTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1805)
399	SEQ ID NO: 8	AGGAGGCGAGAAATTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1806)
400	SEQ ID NO: 8	GAGGAGGTGAGAAATT
	(SEQ ID NO: 8)	(SEQ ID NO: 1807)
401	SEQ ID NO: 8	AGAAATTTCGGGGTAG
	(SEQ ID NO: 8)	(SEQ ID NO: 1808)
402	SEQ ID NO: 8	GAAATTTTGGGGTAGTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1809)
403	SEQ ID NO: 8	GGTAGTATCGTTTATAGA
	(SEQ ID NO: 8)	(SEQ ID NO: 1810)
404	SEQ ID NO: 8	GGGGTAGTATTGTTTATA
	(SEQ ID NO: 8)	(SEQ ID NO: 1811)
405	PROSTAGLANDIN E2	AGTGTATCGTTTTTCGG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1812)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
406	PROSTAGLANDIN E2	TAGTGTATTGTTTTTTGG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1813)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
407	PROSTAGLANDIN E2	TGCGTATCGTTAGTTA
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1814)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
408	PROSTAGLANDIN E2	AGGTTGTGTATTGTTAG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1815)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
409	PROSTAGLANDIN E2	ATTATTTCGGCGGTGA
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1816)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
410	PROSTAGLANDIN E2	GATTATTTTGGTGGTGA
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1817)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
411	PROSTAGLANDIN E2	TAAGTCGCGTAAGGAG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1818)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
412	PROSTAGLANDIN E2	AAGTTGTGTAAGGAGTA
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1819)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
413	PROSTAGLANDIN E2	GTATCGCGAGTTTGGA
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1820)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
414	PROSTAGLANDIN E2	GTATTGTGAGTTTGGAG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1821)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
415	SEQ ID NO: 51	GTCGGGGTCGATTCGA
	(SEQ ID NO: 51)	(SEQ ID NO: 1822)
416	SEQ ID NO: 51	GTTGGGGTTGATTTGAT
	(SEQ ID NO: 51)	(SEQ ID NO: 1823)
417	SEQ ID NO: 51	AGGATTCGTTTGCGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1824)
418	SEQ ID NO: 51	AAGGATTTGTTTGTGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1825)
419	MGC34831	ATTAGCGTTTGGCGTT
	(SEQ ID NO: 52)	(SEQ ID NO: 1826)
420	MGC34831	AATTAGTGTTTGGTGTT
	(SEQ ID NO: 52)	(SEQ ID NO: 1827)
421	MGC34831	GTTTAGCGACGGTCGT
	(SEQ ID NO: 52)	(SEQ ID NO: 1828)
422	MGC34831	TGTTTAGTGATGGTTGT
	(SEQ ID NO: 52)	(SEQ ID NO: 1829)
423	SEQ ID NO: 54	TGTGTAGCGGCGATTA
	(SEQ ID NO: 54)	(SEQ ID NO: 1830)
424	SEQ ID NO: 54	GTGTGTAGTGGTGATT
	(SEQ ID NO: 54)	(SEQ ID NO: 1831)
425	SEQ ID NO: 54	ATTAGCGTTTGGTCGG
	(SEQ ID NO: 54)	(SEQ ID NO: 1832)
426	SEQ ID NO: 54	ATTAGTGTTTGGTTGGG
	(SEQ ID NO: 54)	(SEQ ID NO: 1833)
427	PDLIM1	TAGGTCGCGTAGTCGT
	(SEQ ID NO: 55)	(SEQ ID NO: 1834)
428	PDLIM1	TTAGGTTGTGTAGTTGT
	(SEQ ID NO: 55)	(SEQ ID NO: 1835)
429	SEQ ID NO: 15	AATCGTGCGGTTGATA
	(SEQ ID NO: 15)	(SEQ ID NO: 1836)
430	SEQ ID NO: 15	TGTAGAATTGTGTGGT
	(SEQ ID NO: 15)	(SEQ ID NO: 1837)
431	SEQ ID NO: 15	TTGCGTAGAAAATTCGAG
	(SEQ ID NO: 15)	(SEQ ID NO: 1838)
432	SEQ ID NO: 15	TTGTGTAGAAAATTTGAG
	(SEQ ID NO: 15)	(SEQ ID NO: 1839)
433	SEQ ID NO: 15	TTGCGTAGAAAATTCGAG
	(SEQ ID NO: 15)	(SEQ ID NO: 1838)
434	SEQ ID NO: 15	TTGTGTAGAAAATTTGAG
	(SEQ ID NO: 15)	(SEQ ID NO: 1839)
435	SEQ ID NO: 15	AAAATTCGAGGTCGGG
	(SEQ ID NO: 15)	(SEQ ID NO: 1840)
436	SEQ ID NO: 15	AAAATTTGAGGTTGGG
	(SEQ ID NO: 15)	(SEQ ID NO: 1841)
437	SEQ ID NO: 15	AAAATTCGAGGTCGGG
	(SEQ ID NO: 15)	(SEQ ID NO: 1840)
438	SEQ ID NO: 15	AAAATTTGAGGTTGGG
	(SEQ ID NO: 15)	(SEQ ID NO: 1841)
439	DKK3	ATTCGTTTTAGTTCGAG
	(SEQ ID NO: 24)	(SEQ ID NO: 1842)
440	DKK3	ATTTGTTTTAGTTTGAGT
	(SEQ ID NO: 24)	(SEQ ID NO: 1843)
441	DKK3	TTCGATCGTTTTAGGA
	(SEQ ID NO: 24)	(SEQ ID NO: 1844)
442	DKK3	AGTTTTGATTGTTTTAGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1845)
443	DKK3	ATTCGTTCGGAGACGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1846)
444	DKK3	TTTGTTTGGAGATGGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1847)
445	DKK3	GAAAAGACGCGATTTT
	(SEQ ID NO: 24)	(SEQ ID NO: 1848)
446	DKK3	GAAAAGATGTGATTTTATT
	(SEQ ID NO: 24)	(SEQ ID NO: 1849)
447	SEQ ID NO: 28	TATCGACGTTTTTGGT
	(SEQ ID NO: 28)	(SEQ ID NO: 1850)
448	SEQ ID NO: 28	TATTGATGTTTTTGGTTT
	(SEQ ID NO: 28)	(SEQ ID NO: 1851)
449	SEQ ID NO: 29	TTGATGCGGAGTTCGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1852)
450	SEQ ID NO: 29	TTGATGTGGAGTTTGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1853)
451	SEQ ID NO: 29	TTGATGCGGAGTTCGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1852)
452	SEQ ID NO: 29	TTGATGTGGAGTTTGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1853)
453	SEQ ID NO: 29	TAGGAACGGTAGGCGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1854)
454	SEQ ID NO: 29	TAGGAATGGTAGGTGG
	(SEQ ID NO: 29)	(SEQ ID NO: 2855)
455	SEQ ID NO: 29	TAGGAACGGTAGGCGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1854)
456	SEQ ID NO: 29	TAGGAATGGTAGGTGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1855)
457	SEQ ID NO: 29	GTCGGAGGCGTTTGAG
	(SEQ ID NO: 29)	(SEQ ID NO: 1856)
458	SEQ ID NO: 29	GTTGGAGGTGTTTGAGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1857)
459	ARL7	TAGATTTCGTAGTTTTTTA
	(SEQ ID NO: 30)	(SEQ ID NO: 1858)
460	ARL7	TAGATTTTGTAGTTTTTTAA
	(SEQ ID NO: 30)	(SEQ ID NO: 1859)
461	ARL7	TGGGTACGTTTACGGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1860)
462	ARL7	TGGGTATGTTTATGGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1861)
463	ARL7	GAAGAAATCGTTTTTGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1862)
464	ARL7	GAAGAAATTGTTTTTGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1863)
465	ARL7	TAGTAGGATCGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1864)
466	ARL7	ATAGTAGGATTGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1865)
467	SEQ ID NO: 31	AACGTTGCGTTGGGTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1866)
468	SEQ ID NO: 31	AATGTTGTGTTGGGTAA
	(SEQ ID NO: 31)	(SEQ ID NO: 1867)
469	SEQ ID NO: 31	TAGCGTTTCGTGGTTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1868)
470	SEQ ID NO: 31	GTAGTGTTTTGTGGTTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1869)
471	THH	TTCGGAAGAAAAGCGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1870)
472	THH	TTTGGAAGAAAAGTGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1871)
473	THH	TTCGGAAGAAAAGCGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1870)
474	THH	TTTGGAAGAAAAGTGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1871)
475	THH	GTTCGTTGGCGTAAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1872)
476	THH	GGTTTGTTGGTGTAAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1873)
477	THH	TATTCGGAAGTGATCGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1874)
478	THH	TATTTGGAAGTGATTGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1875)
479	THH	TATTCGGAAGTGATCGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1874)
480	THH	TATTTGGAAGTGATTGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1875)
481	SENP3	TATTCGGATCGGGTTT
	(SEQ ID NO: 39)	(SEQ ID NO: 1876)
482	SENP3	TTTATTTGGATTGGGTT
	(SEQ ID NO: 39)	(SEQ ID NO: 1877)
483	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1878)
484	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1879)
485	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1878)
486	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1879)
487	SENP3	AGGACGTTTTTGATCGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1880)
488	SENP3	AGGATGTTTTTGATTGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1881)
489	SENP3	AGGACGTTTTTGATCGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1680)
490	SENP3	AGGATGTTTTTGATTGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1881)
491	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1882)
492	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1883)
493	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1882)
494	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1883)
495	SEQ ID NO: 42	GAGTCGGGTTGCGATG
	(SEQ ID NO: 42)	(SEQ ID NO: 1884)
496	SEQ ID NO: 42	GGAGTTGGGTTGTGAT
	(SEQ ID NO: 42)	(SEQ ID NO: 1885)
497	SEQ ID NO: 42	ATGGGTTGCGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1886)
498	SEQ ID NO: 42	ATGGGTTGTGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1887)
499	SEQ ID NO: 42	ATGGGTTGCGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1886)
500	SEQ ID NO: 42	ATGGGTTGTGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1887)
501	(SEQ ID NO: 117)	TAGCGGTTTTTTAGCGTA
		(SEQ ID NO: 1888)
502	(SEQ ID NO: 117)	AGTGGTTTTTTAGTGTAT
		(SEQ ID NO: 1889)
503	(SEQ ID NO: 117)	AGATGCGCGGGTAGAT
		(SEQ ID NO: 1890)
504	(SEQ ID NO: 117)	AGATGTGTGGGTAGAT
		(SEQ ID NO: 1891)
505	(SEQ ID NO: 117)	AGATGCGCGGGTAGAT
		(SEQ ID NO: 1890)
506	(SEQ ID NO: 117)	AGATGTGTGGGTAGAT
		(SEQ ID NO: 1891)
507	(SEQ ID NO: 117)	AGATAGTTCGTATTCGT
		(SEQ ID NO: 1892)
508	(SEQ ID NO: 117)	GTAGATAGTTTGTATTTGT
		(SEQ ID NO: 1893)
509	(SEQ ID NO: 117)	TTTGTTCGTAACGTTT
		(SEQ ID NO: 1894)
510	(SEQ ID NO: 117)	TGTTTGTAATGTTTAGAG
		(SEQ ID NO: 1895)
511	O60279	AGTAAACGAATAAGAAGT
	(SEQ ID NO: 47)	(SEQ ID NO: 1896)
512	O60279	AAGTAAATGAATAAGAAGT
	(SEQ ID NO: 47)	(SEQ ID NO: 1897)
513	O60279	TACGTTTTTTCGGATTA
	(SEQ ID NO: 47)	(SEQ ID NO: 1898)
514	O60279	TATGTTTTTTTGGATTAAG
	(SEQ ID NO: 47)	(SEQ ID NO: 1899)
515	O60279	TAATTATCGGCGGTGT
	(SEQ ID NO: 47)	(SEQ ID NO: 1900)
516	O60279	ATTATTGGTGGTGTTTT
	(SEQ ID NO: 47)	(SEQ ID NO: 1901)
517	O60279	GGACGGCGGAAAATTA
	(SEQ ID NO: 47)	(SEQ ID NO: 1902)
518	O60279	AGGGATGGTGGAAAAT
	(SEQ ID NO: 47)	(SEQ ID NO: 1903)
519	SEQ ID NO: 48	TATTTGGCGATTGGGA
	(SEQ ID NO: 48)	(SEQ ID NO: 1904)
520	SEQ ID NO: 48	TGGTGATTTGGAGATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1905)
521	SEQ ID NO: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1906)
522	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1907)
523	SEQ ID N0: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1906)
524	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1907)
525	SEQ ID NO: 48	AACGAATTTTTCGATATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1908)
526	SEQ ID NO: 48	TTTAATGAATTTTTTGATATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1909)
527	SEQ ID NO: 48	AAAATCGTATGCGTGT
	(SEQ ID NO: 48)	(SEQ ID NO: 1910)
528	SEQ ID NO: 48	GAAAATTGTATGTGTGTG
	(SEQ ID NO: 48)	(SEQ ID NO: 1911)
529	SEQ ID NO: 9	GTTTCGCGTTTAGGGA
	(SEQ ID NO: 9)	(SEQ ID NO: 1912)
530	SEQ ID NO: 9	GTTTTGTGTTTAGGGAT
	(SEQ ID NO: 9)	(SEQ ID NO: 1913)
531	SEQ ID NO: 9	AGTGTTCGTCGTAGTT
	(SEQ ID NO: 9)	(SEQ ID NO: 1914)
532	SEQ ID NO: 9	TGAGTGTTTGTTGTAGT
	(SEQ ID NO: 9)	(SEQ ID NO: 1915)
533	SEQ ID NO: 4	TTTTGTTCGCGTTGAA
	(SEQ ID NO: 4)	(SEQ ID NO: 1916)
534	SEQ ID NO: 4	TTGTTTGTGTTGAAGTA
	(SEQ ID NO: 4)	(SEQ ID NO: 1917)
535	SEQ ID NO: 4	GGGTCGCGAGGTAGTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1918)
536	SEQ ID NO: 4	TGGGTTGTGAGGTAGT
	(SEQ ID NO: 4)	(SEQ ID NO: 1919)
537	SEQ ID NO: 4	TTTGTGCGACGTTATT
	(SEQ ID NO: 4)	(SEQ ID NO: 1920)
538	SEQ ID NO: 4	GGTTTGTGTGATGTTAT
	(SEQ ID NO: 4)	(SEQ ID NO: 1921)
539	SEQ ID NO: 4	ATGGCGGTTTCGATTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1922)
540	SEQ ID NO: 4	GATGGTGGTTTTGATTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1923)
541	SEQ ID NO: 5	AATGAGCGAGAAAGTA
	(SEQ ID NO: 5)	(SEQ ID NO: 1924)
542	SEQ ID NO: 5	AGAATGAGTGAGAAAGT
	(SEQ ID NO: 5)	(SEQ ID NO: 1925)
543	SEQ ID NO: 5	ATTAAACGGGATGGTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1926)
544	SEQ ID NO: 5	AATATTAAATGGGATGGT
	(SEQ ID NO: 5)	(SEQ ID NO: 1927)
545	SEQ ID NO: 5	GAGTTGCGAGGATTTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1928)
546	SEQ ID NO: 5	GGAGTTGTGAGGATTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1929)
547	SEQ ID NO: 5	GGGAATCGTTGATTTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1930)
548	SEQ ID NO: 5	AGGGGAATTGTTGATT
	(SEQ ID NO: 5)	(SEQ ID NO: 1931)
549	SEQ ID NO: 7	TAGTCGTCGTGTAGGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1932)
550	SEQ ID NO: 7	TAGGTAGTTGTTGTGTA
	(SEQ ID NO: 7)	(SEQ ID NO: 1933)
551	SEQ ID NO: 7	TATAGGTACGCGATGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1934)
552	SEQ ID NO: 7	AGGTATGTGATGAGGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1935)
553	SEQ ID NO: 7	TATGGTTACGTACGAG
	(SEQ ID NO: 7)	(SEQ ID NO: 1936)
554	SEQ ID NO: 7	ATGGTTATGTATGAGTTT
	(SEQ ID NO: 7)	(SEQ ID NO: 1937)
555	SEQ ID NO: 7	ATGATTTGCGTTACGT
	(SEQ ID NO: 7)	(SEQ ID NO: 1938)
556	SEQ ID NO: 7	ATGATTTGTGTTATGTTT
	(SEQ ID NO: 7)	(SEQ ID NO: 1939)
557	SEQ ID NO: 7	TAACGTTGTGGTTCGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1940)
558	SEQ ID NO: 7	TAATGTTGTGGTTTGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1941)
559	SEQ ID NO: 7	TAACGTTGTGGTTCGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1940)
560	SEQ ID NO: 7	TAATGTTGTGGTTTGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1941)
561	SEQ ID NO: 1	GGTCGGCGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1942)
562	SEQ ID NO: 1	GGTTGGTGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1943)
563	SEQ ID NO: 1	GGTCGGCGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1942)
564	SEQ ID NO: 1	GGTTGGTGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1943)
565	SEQ ID NO: 1	GATTCGAACGGATTTT
	(SEQ ID NO: 1)	(SEQ ID NO: 1944)
566	SEQ ID NO: 1	GGGATTTGAATGGATTT
	(SEQ ID NO: 1)	(SEQ ID NO: 1945)
567	SEQ ID NO: 1	TGGGTCGGGATTCGAA
	(SEQ ID NO: 1)	(SEQ ID NO: 1946)
568	SEQ ID NO: 1	TGGGTTGGGATTTGAA
	(SEQ ID NO: 1)	(SEQ ID NO: 1947)
569	SEQ ID NO: 1	TGGGTCGGGATTCGAA
	(SEQ ID NO: 1)	(SEQ ID NO: 1946)
570	SEQ ID NO: 1	TGGGTTGGGATTTGAA
	(SEQ ID NO: 1)	(SEQ ID NO: 1947)
571	SEQ ID NO: 1	GTCGGAAGTTTCGGGA
	(SEQ ID NO: 1)	(SEQ ID NO: 1948)
572	SEQ ID NO: 1	GTTGGAAGTTTTGGGAT
	(SEQ ID NO: 1)	(SEQ ID NO: 1949)
573	SEQ ID NO: 1	TGGATATCGTAGGGTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1950)
574	SEQ ID NO: 1	TGGATATTGTAGGGTAG
	(SEQ ID NO: 1)	(SEQ ID NO: 1951)
575	PROSTAGLANDIN E2	AGGTAATCGAGGCGGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1952)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
576	PROSTAGLANDIN E2	AGGTAATTGAGGTGGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1953)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
577	PROSTAGLANDIN E2	AGGTAATCGAGGCGGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1952)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
578	PROSTAGLANDIN E2	AGGTAATTGAGGTGGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1953)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
579	PROSTAGLANDIN E2	GGCGTCGAAAGTCGTT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1954)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
580	PROSTAGLANDIN E2	GGTGTTGAAAGTTGTTG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1955)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
581	PROSTAGLANDIN E2	TAATCGTTTGTTTACGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1956)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
582	PROSTAGLANDIN E2	AATTGTTTGTTTATGTAGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1957)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
583	ORPHAN NUCLEAR	TTACGGAGGCGTTTTA
	RECEPTOR NR5A2	(SEQ ID NO: 1958)
	(ALPHA-1-FETO-
	PROTEIN TRANSCRIPT-
	ION FACTOR) (HEPATO-
	CYTIC TRANSCRIPTION
	FACTOR) (B1-BINDING
	FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
584	ORPHAN NUCLEAR	TTTTATGGAGGTGTTTT
	RECEPTOR NR5A2	(SEQ ID NO: 1959)
	(ALPHA-1-FETO-
	PROTEIN TRANSCRIPT-
	ION FACTOR) (HEPATO-
	CYTIC TRANSCRIPTION
	FACTOR) (B1-BINDING
	FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
585	ORPHAN NUCLEAR	AGGCGAATTTATCGGG
	RECEPTOR NR5A2	(SEQ ID NO: 1960)
	(ALPHA-1-FETO-
	PROTEIN TRANSCRIPT-
	ION FACTOR) (HEPATO-
	CYTIC TRANSCRIPTION
	FACTOR) (B1-BINDING
	FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
586	ORPHAN NUCLEAR	GGTGAATTTATTGGGG
	RECEPTOR NR5A2	(SEQ ID NO: 1961)
	(ALPHA-1-FETO-
	PROTEIN TRANSCRIPT-
	ION FACTOR) (HEPATO-
	CYTIC TRANSCRIPTION
	FACTOR) (B1-BINDING
	FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
587	ORPHAN NUCLEAR	TAGTCGAAGTAGGCGT
	RECEPTOR NR5A2	(SEQ ID NO: 1962)
	(ALPHA-1-FETO-
	PROTEIN TRANSCRIPT-
	ION FACTOR) (HEPATO-
	CYTIC TRANSCRIPTION
	FACTOR) (B1-BINDING
	FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
588	ORPHAN NUCLEAR	TAGTTGAAGTAGGTGTT
	RECEPTOR NR5A2	(SEQ ID NO: 1963)
	(ALPHA-1-FETO-
	PROTEIN TRANSCRIPT-
	ION FACTOR) (HEPATO-
	CYTIC TRANSCRIPTION
	FACTOR) (B1-BINDING
	FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
589	ORPHAN NUCLEAR	TTTTCGACGAAGTTTT
	RECEPTOR NR5A2	(SEQ ID NO: 1964)
	(ALPHA-1-FETO-
	PROTEIN TRANSCRIPT-
	ION FACTOR) (HEPATO-
	CYTIC TRANSCRIPTION
	FACTOR) (B1-BINDING
	FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
590	ORPHAN NUCLEAR	TTTTGATGAAGTTTTGTT
	RECEPTOR NR5A2	(SEQ ID NO: 1965)
	(ALPHA-1-FETO-
	PROTEIN TRANSCRIPT-
	ION FACTOR) (HEPATO-
	CYTIC TRANSCRIPTION
	FACTOR) (B1-BINDING
	FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
591	LIM DOMAIN KINASE 1	TGTAGTCGGGAGGTTA
	(EC 2.7.1.37)	(SEQ ID NO: 1966)
	(LIMK-1)
	(SEQ ID NO: 12)
592	LIM DOMAIN KINASE 1	TGTAGTTGGGAGGTTA
	(EC 2.7.1.37)	(SEQ ID NO: 1967)
	(LIMK-1)
	(SEQ ID NO: 12)
593	LIM DOMAIN KINASE 1	TGTAGTCGGGAGGTTA
	(EC 2.7.1.37)	(SEQ ID NO: 1966)
	(LIMK-1)
	(SEQ ID NO: 12)
594	LIM DOMAIN KINASE 1	TGTAGTTGGGAGGTTA
	(EC 2.7.1.37)	(SEQ ID NO: 1967)
	(LIMK-1)
	(SEQ ID NO: 12)
595	LIM DOMAIN KINASE 1	GGATTATCGCGGGGGT
	(EC 2.7.1.37)	(SEQ ID NO: 1968)
	(LIMK-1)
	(SEQ ID NO: 12)
596	LIM DOMAIN KINASE 1	GGATTATTGTGGGGGT
	(EC 2.7.1.37)	(SEQ ID NO: 1969)
	(LIMK-1)
	(SEQ ID NO: 12)
597	LIM DOMAIN KINASE 1	GGATTATCGCGGGGGT
	(EC 2.7.1.37)	(SEQ ID NO: 1968)
	(LIMK-1)
	(SEQ ID NO: 12)
598	LIM DOMAIN KINASE 1	GGATTATTGTGGGGGT
	(EC 2.7.1.37)	(SEQ ID NO: 1969)
	(LIMK-1)
	(SEQ ID NO: 12)
599	LIM DOMAIN KINASE 1	GTCGGTAGTTTATCGGAT
	(EC 2.7.1.37)	(SEQ ID NO: 1970)
	(LIMK-1)
	(SEQ ID NO: 12)
600	LIM DOMAIN KINASE 1	GTTGGTAGTTTATTGGAT
	(EC 2.7.1.37)	(SEQ ID NO: 1971)
	(LIMK-1)
	(SEQ ID NO: 12)
601	LIM DOMAIN KINASE 1	GTCGGTAGTTTATCGGAT
	(EC 2.7.1.37)	(SEQ ID NO: 1970)
	(LIMK-1)
	(SEQ ID NO: 12)
602	LIM DOMAIN KINASE 1	GTTGGTAGTTTATTGGAT
	(EC 2.7.1.37)	(SEQ ID NO: 1971)
	(LIMK-1)
	(SEQ ID NO: 12)
603	LIM DOMAIN KINASE 1	TAGGAGACGTTACGTT
	(EC 2.7.1.37)	(SEQ ID NO: 1972)
	(LIMK-1)
	(SEQ ID NO: 12)
604	LIM DOMAIN KINASE 1	AGATGTTATGTTAGGGT
	(EC 2.7.1.37)	(SEQ ID NO: 1973)
	(LIMK-1)
	(SEQ ID NO: 12)
605	BCL11B	TAGGTTTCGATTCGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1974)
606	BCL11B	TTAGGTTTTGATTTGTTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1975)
607	BCL11B	AAGTCGTCGGAGTTAG
	(SEQ ID NO: 50)	(SEQ ID NO: 1976)
608	BCL11B	GTGAAGTTGTTGGAGT
	(SEQ ID NO: 50)	(SEQ ID NO: 1977)
609	BCL11B	TTGAGGCGTTACGGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1978)
610	BCL11B	TTGAGGTGTTATGGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1979)
611	BCL11B	TTGAGGCGTTACGGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1978)
612	BCL11B	TTGAGGTGTTATGGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1979)
613	MSF	GTTTCGAAATTGGCGT
	(SEQ ID NO: 13)	(SEQ ID NO: 1980)
614	MSF	TTTGAAATTGGTGTGG
	(SEQ ID NO: 13)	(SEQ ID NO: 1981)
615	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1982)
616	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1983)
617	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1992)
618	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1983)
619	MSF	TTACGGTTCGATTTTG
	(SEQ ID NO: 13)	(SEQ ID NO: 1984)
620	MSF	TATGGTTTGATTTTGGG
	(SEQ ID NO: 13)	(SEQ ID NO: 1985)
621	SEQ ID NO: 14	TAAGGCGTTTTCGATA
	(SEQ ID NO: 14)	(SEQ ID NO: 1986)
622	SEQ ID NO: 14	GTAAGGTGTTTTTGATAT
	(SEQ ID NO: 14)	(SEQ ID NO: 1987)
623	SEQ ID NO: 14	TGGGTGTACGCGTGAA
	(SEQ ID NO: 14)	(SEQ ID NO: 1988)
624	SEQ ID NO: 14	TGTATGTGTGAAGGGG
	(SEQ ID NO: 14)	(SEQ ID NO: 1989)
625	SEQ ID NO: 16	ATCGTTGGTCGGATTT
	(SEQ ID NO: 16)	(SEQ ID NO: 1990)
626	SEQ ID NO: 16	TAGGATTGTTGGTTGGA
	(SEQ ID NO: 16)	(SEQ ID NO: 1991)
627	SEQ ID NO: 16	AGGAGTTTTCGTGTCGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1992)
628	SEQ ID NO: 16	AGGAGTTTTTGTGTTGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1993)
629	SEQ ID NO: 16	AGGAGTTTTCGTGTCGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1992)
630	SEQ ID NO: 16	AGGAGTTTTTGTGTTGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1993)
631	SEQ ID NO: 16	TTACGGATAGGGCGAT
	(SEQ ID NO: 16)	(SEQ ID NO: 1994)
632	SEQ ID NO: 16	TATGGATAGGGTGATTT
	(SEQ ID NO: 16)	(SEQ ID NO: 1995)
633	SEQ ID NO: 16	AGGCGTTGTCGGTGAT
	(SEQ ID NO: 16)	(SEQ ID NO: 1996)
634	SEQ ID NO: 16	AGGTGTTGTTGGTGATA
	(SEQ ID NO: 16)	(SEQ ID NO: 1997)
635	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1998)
636	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1999)
637	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1998)
638	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1999)
639	SEQ ID NO: 17	ATTTAGTCGTGCGTTT
	(SEQ ID NO: 17)	(SEQ ID NO: 2000)
640	SEQ ID NO: 17	TGATTTAGTTGTGTGTT
	(SEQ ID NO: 17)	(SEQ ID NO: 2001)
641	SEQ ID NO: 18	TTTACGCGGGGTTTTA
	(SEQ ID NO: 18)	(SEQ ID NO: 2002)
642	SEQ ID NO: 18	TTTATGTGGGGTTTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2003)
643	SEQ ID NO: 18	TTACGTCGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2004)
644	SEQ ID NO: 18	TTTTATGTTGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2005)
645	SEQ ID NO: 18	TATTTGGACGTCGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2006)
646	SEQ ID NO: 18	TATTTGGATGTTGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2007)
647	SEQ ID NO: 18	TATTTGGACGTCGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2006)
648	SEQ ID NO: 18	TATTTGGATGTTGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2007)
649	SEQ ID NO: 18	GAGGCGTATTAGGTCGG
	(SEQ ID NO: 18)	(SEQ ID NO: 2008)
650	SEQ ID NO: 18	AGGTGTATTAGGTTGGG
	(SEQ ID NO: 18)	(SEQ ID NO: 2009)
651	SEQ ID NO: 18	AAAGCGGAGTCGTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2010)
652	SEQ ID NO: 18	AGTGGAGTTGTTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2011)
653	SEQ ID NO: 19	AGGTTTTCGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2012)
654	SEQ ID NO: 19	TAGGTTTTTGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2013)
655	SEQ ID NO: 19	TGAGATTGGTTTTTTAAA
	(SEQ ID NO: 19)	(SEQ ID NO: 2014)
656	SEQ ID NO: 19	GGTGAGATTTGTTTTTTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2015)
657	PRDM6	AGTTTTAAGCGTTTGGT
	(SEQ ID NO: 20)	(SEQ ID NO: 2016)
658	PRDM6	AGTTTTAAGTGTTTGGT
	(SEQ ID NO: 20)	(SEQ ID NO: 2017)
659	PRDM6	AGTTTTAAGCGTTTGGT
	(SEQ ID NO: 20)	(SEQ ID NO: 2016)
660	PRDM6	AGTTTTAAGTGTTTGGT
	(SEQ ID NO: 20)	(SEQ ID NO: 2017)
661	PRDM6	GAAGTTCGGATTTCGG
	(SEQ ID NO: 20)	(SEQ ID NO: 2018)
662	PRDM6	GGAAGTTTGGATTTTGG
	(SEQ ID NO: 20)	(SEQ ID NO: 2019)
663	PRDM6	TTGTCGGGTTACGGGA
	(SEQ ID NO: 20)	(SEQ ID NO: 2020)
664	PRDM6	GTTGGGTTATGGGAGA
	(SEQ ID NO: 20)	(SEQ ID NO: 2021)
665	PRDM6	TTCGTAGAATTGTCGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2022)
666	PRDM6	TTTGTAGAATTGTTGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2023)
667	PRDM6	TTCGTAGAATTGTCGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2022)
668	PRDM6	TTTGTAGAATTGTTGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2023)
669	RAP2B	GGTCGGGTAATCGTTA
	(SEQ ID NO: 21)	(SEQ ID NO: 2024)
670	RAP2B	GTTGGGTAATTGTTAGA
	(SEQ ID NO: 21)	(SEQ ID NO: 2025)
671	RAP2B	AGGAAGCGTTTTCGTT
	(SEQ ID NO: 21)	(SEQ ID NO: 2026)
672	RAP2B	AGAGGAAGTGTTTTTGT
	(SEQ ID NO: 21)	(SEQ ID NO: 2027)
673	NR2E1	AATGTAGCGGCGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2028)
674	NR2E1	TAAATGTAGTGGTGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2029)
675	NR2E1	GTCGTTATCGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2030)
676	NR2E1	GTTGTTATTGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2031)
677	NR2E1	GTCGTTATGGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2030)
678	NR2E1	GTTGTTATTCGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2031)
679	NR2E1	GACGTAAGTTTCGGGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2032)
680	NR2E1	GGATGTAAGTTTTGGG
	(SEQ ID NO: 22)	(SEQ ID NO: 2033)
681	NR2E1	TTTTTAGTCGGGAGAA
	(SEQ ID NO: 22)	(SEQ ID NO: 2034)
682	NR2E1	TTTTTAGTTGTGAGAAGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2035)
683	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2036)
684	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2037)
685	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2036)
686	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2037)
687	NR2E1	AGGCGAGTCGGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2038)
688	NR2E1	AGGTGAGTTGGAGTTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2039)
689	NR2E1	TAAGTCGAGCGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2040)
690	NR2E1	TAGTAAGTTGAGTGAGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2041)
691	NR2E1	AGGGACGCGAAAATTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2042)
692	NR2E1	GGAGGGATGTGAAAAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2043)
693	PCDH7	ATCGTAGTCGGTTTTA
	(SEQ ID NO: 23)	(SEQ ID NO: 2044)
694	PCDE7	GATTATTGTAGTTGGTTT
	(SEQ ID NO: 23)	(SEQ ID NO: 2045)
695	RTTN	TAGTGGCGCGGTAGTT
	(SEQ ID NO: 25)	(SEQ ID NO: 2046)
696	RTTN	TAGTGGTGTGGTAGTTT
	(SEQ ID NO: 25)	(SEQ ID NO: 2047)
697	RTTN	TAGGACGTGTTTTCGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2048)
698	RTTN	AGGATGTGTTTTTGGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2049)
699	SNAP25	TATTTCGAGTTAGAGTTACGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2050)
700	SNAP25	TATTTTGAGTTAGAGTTATGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2051)
701	SNAP25	TATTTCGAGTTAGAGTTACGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2050)
702	SNAP25	TATTTTGAGTTAGAGTTATGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2051)
703	SNAP25	ATACGGAATATCGTATTT
	(SEQ ID NO: 33)	(SEQ ID NO: 2052)
704	SNAP25	GTGTATATATGGAATATTGT
	(SEQ ID NO: 33)	(SEQ ID NO: 2053)
705	SEQ ID NO: 26	TTAAGTATCGAGGCGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2054)
706	SEQ ID NO: 26	TTTTAAGTATTGAGGTGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2055)
707	SEQ ID NO: 26	AATTTTGGTCGTTTAGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2056)
708	SEQ ID NO: 26	AAATTTTGGTTGTTTAGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2057)
709	SEQ ID NO: 26	TTCGTATTGACGTTAAT
	(SEQ ID NO: 26)	(SEQ ID NO: 2058)
710	SEQ ID NO: 26	TTTGTATTGATGTTAATAGA
	(SEQ ID NO: 26)	(SEQ ID NO: 2059)
711	GIRK2	AGTTGTTCGTAGGCGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2060)
712	GIRK2	AGTTGTTTGTAGGTGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2061)
713	GIRK2	AGTTGTTCGTAGGCGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2060)
714	GIRK2	AGTTGTTTGTAGGTGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2061)
715	GIRK2	TTATTTCGTTCGTAGTT
	(SEQ ID NO: 27)	(SEQ ID NO: 2062)
716	GIRK2	TTTGTTTGTAGTTAGGTA
	(SEQ ID NO: 27)	(SEQ ID NO: 2063)
717	GIRK2	TTAGTCGAAAGGCGAG
	(SEQ ID NO: 27)	(SEQ ID NO: 2064)
718	GIRK2	TAGTTGAAAGGTGAGG
	(SEQ ID NO: 27)	(SEQ ID NO: 2065)
719	SEQ ID NO: 28	ATTAGGCGAGTTTCGT
	(SEQ ID NO: 28)	(SEQ ID NO: 2066)
720	SEQ ID NO: 28	TTAGGTGAGTTTTGTTT
	(SEQ ID NO: 28)	(SEQ ID NO: 2067)
721	SEQ ID NO: 31	TTTACGTAGGGCGATT
	(SEQ ID NO: 31)	(SEQ ID NO: 2068)
722	SEQ ID NO: 31	ATTTTTATGTAGGGTGAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2069)
723	SEQ ID NO: 31	GATACGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2070)
724	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2071)
725	SEQ ID NO: 31	GATACGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2070)
726	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2071)
727	SEQ ID NO: 31	TTCGGGCGTTTTATAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2072)
728	SEQ ID NO: 31	GGTTTGGGTGTTTTATA
	(SEQ ID NO: 31)	(SEQ ID NO: 2073)
729	HOXB13	GTCGTTATTATTTCGAGG
	(SEQ ID NO: 34)	(SEQ ID NO: 2074)
730	HOXB13	GTTGTTATTATTTTGAGGA
	(SEQ ID NO: 34)	(SEQ ID NO: 2075)
731	HOXB13	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2076)
732	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2077)
733	HOXB13	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2076)
734	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2077)
735	HOXB13	TTGGTCGCGTAGTAAA
	(SEQ ID NO: 34)	(SEQ ID NO: 2078)
736	HOXB13	TGGTTGTGTAGTAAAGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2079)
737	(SEQ ID NO: 35)	GGAGGTGCGAATTTAA
		(SEQ ID NO: 2080)
738	(SEQ ID NO: 35)	GGGAGGTGTGAATTTA
		(SEQ ID NO: 2081)
739	(SEQ ID NO: 35)	AAATAGTCGTTTGGGA
		(SEQ ID NO: 2082)
740	(SEQ ID NO: 35)	AAATAGTTGTTTGGGAG
		(SEQ ID NO: 2083)
741	(SEQ ID NO: 35)	AGAAAATATACGAGATTTAT
		(SEQ ID NO: 2084)
742	(SEQ ID NO: 35)	AGAAAATATATGAGATTTATT
		(SEQ ID NO: 2085)
743	(SEQ ID NO: 35)	TAAAGACGGGAAGAGA
		(SEQ ID NO: 2086)
744	(SEQ ID NO: 35)	ATAAAGATGGGAAGAGA
		(SEQ ID NO: 2087)
745	MGC10561	TTTTTTACGTTAAGGGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2088)
746	MGC10561	TTTTTATGTTAAGGGGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2089)
747	MGC10561	TTTGTTTTTCGAGTAGA
	(SEQ ID NO: 37)	(SEQ ID NO: 2090)
748	MGC10561	TGTTTTTTGAGTAGAGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2091)
749	LMX1A	GTCGGGTTTTTCGGAA
	(SEQ ID NO: 38)	(SEQ ID NO: 2092)
750	LMX1A	GTTGGGTTTTTTGGAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2093)
751	LMX1A	GTCGAGATTTTATCGAAA
	(SEQ ID NO: 38)	(SEQ ID NO: 2094)
752	LMX1A	GTTGAGATTTTATTGAAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2095)
753	LMX1A	AGTATTCGGGCGGGTA
	(SEQ ID NO: 38)	(SEQ ID NO: 2096)
754	LMX1A	GTAGTATTTGGGTGGG
	(SEQ ID NO: 38)	(SEQ ID NO: 2097)
755	LMX1A	AACGAAATTACGTGTAT
	(SEQ ID NO: 38)	(SEQ ID NO: 2098)
756	LMX1A	TGAAATGAAATTATGTGTA
	(SEQ ID NO: 38)	(SEQ ID NO: 2099)
757	GS1	TGCGAGTTAGCGGTTA
	(SEQ ID NO: 40)	(SEQ ID NO: 2100)
758	GS1	TTGTGAGTTAGTGGTT
	(SEQ ID NO: 40)	(SEQ ID NO: 2101)
759	GS1	AGTTTCGAGGTTTTCGG
	(SEQ ID NO: 40)	(SEQ ID NO:2102)
760	GS1	AAGTTTTGAGGTTTTTGG
	(SEQ ID NO: 40)	(SEQ ID NO: 2103)
761	TITF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2104)
762	TITF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2105)
763	TITF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2104)
764	TITF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2105)
765	TITF1	GGTTCGTTTAAGTTCGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2106)
766	TITF1	GGTTTGTTTAAGTTTGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2107)
767	TITF1	GGTTCGTTTAAGTTCGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2106)
768	TITF1	GGTTTGTTTAAGTTTGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2107)
769	TITF1	TTAGGTCGCGTTTGTA
	(SEQ ID NO: 41)	(SEQ ID NO: 2108)
770	TITF1	AGGTTGTGTTTGTAGA
	(SEQ ID NO: 41)	(SEQ ID NO: 2109)
771	TITF1	TATTTCGTTTTCGTAATT
	(SEQ ID NO: 41)	(SEQ ID NO: 2110)
772	TITF1	TTTGTTTTTGTAATTAGATT
	(SEQ ID NO: 41)	(SEQ ID NO: 2111)
773	DDX51	AGATTTTCGGCGAGAT
	(SEQ ID NO: 43)	(SEQ ID NO: 2112)
774	DDX51	ATTTTTGGTGAGATAGG
	(SEQ ID NO: 43)	(SEQ ID NO: 2113)
775	DDX51	TACGTGTGGTTTTCGGTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2114)
776	DDX51	TATGTGTGGTTTTTGGTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2115)
777	DDX51	TACGTGTGGTTTTCGGTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2114)
778	DDX51	TATGTGTGGTTTTTGGTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2115)
779	DDX51	AACGTGCGGGGTTTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2116)
780	DDX51	TGAATGTGTGGGGTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2117)
781	SEQ ID NO: 45	AGCGAACGTTTATTTT
	(SEQ ID NO: 45)	(SEQ ID NO: 2118)
782	SEQ ID NO: 45	TAGGAGAGTGAATGTTT
	(SEQ ID NO: 45)	(SEQ ID NO: 2119)
783	SEQ ID NO: 46	GAGTCGGGTTATCGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2120)
784	SEQ ID NO: 46	GGAGTTGGGTTATTGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2121)
785	SEQ ID NO: 46	TTACGGATGTTTCGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2122)
786	SEQ ID NO: 46	TTTATGGATGTTTTGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2123)
787	SEQ ID NO: 46	TGACGTATTTTCGGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2124)
788	SEQ ID NO: 46	GGTGATGTATTTTTGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2125)
789	SEQ ID NO: 46	ATAGTCGGAATCGTTG
	(SEQ ID NO: 46)	(SEQ ID NO: 2126)
790	SEQ ID NO: 46	TAGTTGGAATTGTTGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2127)
791	SEQ ID NO: 2	ATTGGGTTTCGCGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2128)
792	SEQ ID NO: 2	ATTGGGTTTTGTGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2129)
793	SEQ ID NO: 2	ATTGGGTTTCGCGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2128)
794	SEQ ID NO: 2	ATTGGGTTTTGTGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2129)
795	SEQ ID NO: 2	TAGTAGTCGGCGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2130)
796	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2131)
797	SEQ ID NO: 2	TAGTAGTCGGCGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2130)
798	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2131)
799	SEQ ID NO: 2	TTGATTGGCGGACGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1706)
800	SEQ ID NO: 2	TTGATTGGTGGATGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1707)
801	SEQ ID NO: 2	TTGATTGGCGGACGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1706)
802	SEQ ID NO: 2	TTGATTGGTGGATGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1707)
803	SEQ ID NO: 3	TTGCGTTAATTCGGTA
	(SEQ ID NO: 3)	(SEQ ID NO: 2132)
804	SEQ ID NO: 3	AATTTGTGTTAATTTGGT
	(SEQ ID NO: 3)	(SEQ ID NO: 2133)
805	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2134)
806	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2135)
807	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2134)
808	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2135)
809	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2136)
810	SEQ ID NO: 3	GGTTGAAGAGTTGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2137)
811	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2136)
812	SEQ ID NO: 3	GGTTGAAGAGTTGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2137)
813	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2138)
814	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2139)
815	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2138)
816	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2139)

TABLE 17
Breast cancer vs. other cancer
No:	Gene	Oligo:
1	SCGB3A1	GGCGTAGAAGGCGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2140)
2	SCGB3A1	GGTGTAGAAGGTGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2141)
3	SCGB3A1	GGCGTAGAAGGCGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2140)
4	SCGB3A1	GGTGTAGAAGGTGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2141)
5	SCGB3A1	TAGTGTTCGACGTTGT
	(SEQ ID NO: 115)	(SEQ ID NO: 1475)
6	SCGB3A1	TAGTGTTTGATGTTGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 1476)
7	ARH1/NOEY2	TAAAACGTTCGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1485)
8	ARH1/NOEY2	TTTAAAATGTTTGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1486)
9	ARH1/NOEY2	TGTATTCGTCGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1487)
10	ARH1/NOEY2	AATGTATTTGTTGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1488)
11	ARH1/NOEY2	TTAGACGGAGTTCGGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1489)
12	ARH1/NOEY2	TAGATGGAGTTTGGAGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1490)
13	ARH1/NOEY2	TAGACGTAGGCGTATT
	(SEQ ID NO: 97)	(SEQ ID NO: 1491)
14	ARH1/NOEY2	GGGTAGATGTAGGTGT
	(SEQ ID NO: 97)	(SEQ ID NO: 1492)
15	CCND2	TTAGGGTCGATCGTGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1493)
16	CCND2	TAGGGTTGATTGTGTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1494)
17	CCND2	TTATCGTAGTCGGTTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1495)
18	CCND2	GATTTTATTGTAGTTGGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1496)
19	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1497)
20	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1498)
21	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1497)
22	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1498)
23	CCND2	AAGGATCGAGCGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1499)
24	CCND2	AAGGATTGAGTGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1500)
25	CCND2	AAGGATCGAGCGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1499)
26	CCND2	AAGGATTGAGTGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1500)
27	CDKN1A	ATTAGGGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1501)
28	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1502)
29	CDKN1A	ATTAGGGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1501)
30	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1502)
31	CDKN2A	GGCGTTGTTTAACGTAT
	(SEQ ID NO: 57)	(SEQ ID NO: 1503)
32	CDKN2A	GGGTGTTGTTTAATGTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1504)
33	DAPK1	TTTCGGAGATTCGGTT
	(SEQ ID NO: 98)	(SEQ ID NO: 1509)
34	DAPK1	TTTGGAGATTTGGTTTT
	(SEQ ID NO: 98)	(SEQ ID NO: 1510)
35	DAPK1	TTTTAGCGTCGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1511)
36	DAPK1	TTTTAGTGTTGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1512)
37	DAPK1	TTTTAGCGTCGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1511)
38	DAPK1	TTTTAGTGTTGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1512)
39	EYA4	GGTATAAAATCGTAAATTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1513)
40	EYA4	GGGTATAAAATTGTAAATTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1514)
41	EYA4	TATGTAGTCGCGTAGT
	(SEQ ID NO: 58)	(SEQ ID NO: 1515)
42	EYA4	TTTATGTAGTTGTGTAGT
	(SEQ ID NO: 58)	(SEQ ID NO: 1516)
43	EYA4	GTTTAGATACGAAATGTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1517)
44	EYA4	GTTTAGATATGAAATGTTAT
	(SEQ ID NO: 58)	(SEQ ID NO: 1518)
45	EYA4	AGTTTTGACGTCGTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1519)
46	EYA4	TTGATGTTGTTTTGGAA
	(SEQ ID NO: 58)	(SEQ ID NO: 1520)
47	FHIT	GTTACGTTAGCGGGTT
	(SEQ ID NO: 76)	(SEQ ID NO: 1521)
48	FHIT	GGTTATGTTAGTGGGT
	(SEQ ID NO: 76)	(SEQ ID NO: 1522)
49	GSTP1	GGCGATTTCGGGGATT
	(SEQ ID NO: 59)	(SEQ ID NO: 1525)
50	GSTP1	GGTGATTTTGGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1526)
51	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1527)
52	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1528)
53	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1527)
54	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1528)
55	GSTP1	AGTTCGCGGGATTTTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1529)
56	GSTP1	GGAGTTTGTGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1530)
57	GSTP1	AGTTTTCGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1531)
58	GSTP1	TAGTTTTTGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1532)
59	HIC1	TATCGAAGTTTTCGGG
	(SEQ ID NO: 85)	(SEQ ID NO: 1533)
60	HIC1	TATTGAAGTTTTTGGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1534)
61	HIC1	TAGCGGTTATTTCGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1535)
62	HIC1	TTTAGTGGTTATTTTGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1536)
63	HIC1	TACGTTTTTCGTAGCGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1537)
64	HIC1	ATTATGTTTTTTGTAGTGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1538)
65	HIC1	TTCGGTTTTGTCGTATA
	(SEQ ID NO: 85)	(SEQ ID NO: 1539)
66	HIC1	TTTGGTTTTGTTGTATAG
	(SEQ ID NO: 85)	(SEQ ID NO: 1540)
67	SERPINB5	ATTGTCGTACGTATGT
	(SEQ ID NO: 68)	(SEQ ID NO: 1551)
68	SERPINB5	AGAGGATTGTTGTATGTA
	(SEQ ID NO: 68)	(SEQ ID NO: 1552)
69	SERPINB5	TTTTTTGTTCGAATATGT
	(SEQ ID NO: 68)	(SEQ ID NO: 1553)
70	SERPINB5	TTTGTTTGAATATGTTGG
	(SEQ ID NO: 68)	(SEQ ID NO: 1554)
71	TERT	TATAACGAACGTCGTT
	(SEQ ID NO: 92)	(SEQ ID NO: 2142)
72	TERT	AGGTATAATGAATGTTGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2143)
73	TGFBR2	AAGACGGTTAGGTCGG
	(SEQ ID NO: 93)	(SEQ ID NO: 2144)
74	TGFBR2	AAGATGGTTAGGTTGG
	(SEQ ID NO: 93)	(SEQ ID NO: 2145)
75	TGFBR2	AAGACGGTTAGGTCGG
	(SEQ ID NO: 93)	(SEQ ID NO: 2144)
76	TGFBR2	AAGATGGTTAGGTTGG
	(SEQ ID NO: 93)	(SEQ ID NO: 2145)
77	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1569)
78	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1570)
79	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1569)
80	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1570)
81	TIMP3	TTATTAACGGAGGAAGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1571)
82	TIMP3	TATTAATGGAGGAAGGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1572)
83	TIMP3	TTCGTTATGTGTACGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1573)
84	TIMP3	TTTGTTATGTGTATGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1574)
85	TIMP3	TTCGTTATGTGTACGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1573)
86	TIMP3	TTTGTTATGTGTATGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1574)
87	TIMP3	GAGTATTTCGAGTTTGT
	(SEQ ID NO: 103)	(SEQ ID NO: 1575)
88	TIMP3	AGTATTTTGAGTTTGTATT
	(SEQ ID NO: 103)	(SEQ ID NO: 1576)
89	TIMP3	TAAGCGTTAATCGAGT
	(SEQ ID NO: 103)	(SEQ ID NO: 1577)
90	TIMP3	TAGGTAAGTGTTAATTGA
	(SEQ ID NO: 103)	(SEQ ID NO: 1578)
91	TP73	TAGGATTCGCGTTTTT
	(SEQ ID NO: 86)	(SEQ ID NO: 1579)
92	TP73	GGTAGGATTTGTGTTTT
	(SEQ ID NO: 86)	(SEQ ID NO: 1580)
93	CDH13	TAGTCGCGTGTATGAA
	(SEQ ID NO: 70)	(SEQ ID NO: 1585)
94	CDH13	TGTAGTTGTGTGTATGA
	(SEQ ID NO: 70)	(SEQ ID NO: 1586)
95	TMS1/ASC	TTCGTTTCGGAGTCGA
	(SEQ ID NO: 84)	(SEQ ID NO: 1591)
96	TMS1/ASC	TTTGTTTTGGAGTTGAT
	(SEQ ID NO: 84)	(SEQ ID NO: 1592)
97	APAF1	GTGTCGTAGCGGTATT
	(SEQ ID NO: 82)	(SEQ ID NO: 1593)
98	APAF1	GGTGTTGTAGTGGTAT
	(SEQ ID NO: 82)	(SEQ ID NO: 1594)
99	APAF1	AGTAGCGTCGGGTTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1595)
100	APAF1	GAGTAGTGTTGGGTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1596)
101	SYK	GAAGTTATCGCGTTGG
	(SEQ ID NO: 60)	(SEQ ID NO: 1597)
102	SYK	AGAAGTTATTGTGTTGG
	(SEQ ID NO: 60)	(SEQ ID NO: 1598)
103	SYK	GATCGATGCGGTTTAT
	(SEQ ID NO: 60)	(SEQ ID NO: 1599)
104	SYK	GGGATTGATGTGGTTT
	(SEQ ID NO: 60)	(SEQ ID NO: 1600)
105	SYK	TTATTCGGTCGGGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1603)
106	SYK	TTTATTTGGTTGGGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1604)
107	FAEP3	TAAAGCGGTAGTTCGG
	(SEQ ID NO: 77)	(SEQ ID NO: 1609)
108	FABP3	AAGTGGTAGTTTGGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1610)
109	FABP3	TATTGGCGTTGACGTA
	(SEQ ID NO: 77)	(SEQ ID NO: 1611)
110	FABP3	TGGTGTTGATGTAGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1612)
111	RASSF1A	TACGGGTATTTTCGCGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1613)
112	RASSF1A	ATATGGGTATTTTTGTGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1614)
113	RASSF1A	AGAGCGCGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1615)
114	RASSF1A	GAGAGTGTGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1616)
115	RASSF1A	AGTAAATCGGATTAGGA
	(SEQ ID NO: 90)	(SEQ ID NO: 1617)
116	RASSF1A	AGTAAATTGGATTAGGAG
	(SEQ ID NO: 90)	(SEQ ID NO: 1618)
117	TWIST	AGTAAAGGCGTTGCGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1619)
118	TWIST	AGTAAAGGTGTTGTGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1620)
119	TWIST	AGTAAAGGCGTTGCGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1619)
120	TWIST	AGTAAAGGTGTTGTGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1620)
121	TWIST	TATTTTTCGAGGCGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1621)
122	TWIST	TTTTGAGGTGTAGTTTT
	(SEQ ID NO: 100)	(SEQ ID NO: 1622)
123	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1623)
124	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1624)
125	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1623)
126	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1624)
127	TWIST	TAGGTCGGGACGTAAA
	(SEQ ID NO: 100)	(SEQ ID NO: 1625)
128	TWIST	AGTAGGTTGGGATGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1626)
129	ESR2	ATAAGCGATTTAACGAT
	(SEQ ID NO: 91)	(SEQ ID NO: 1629)
130	ESR2	AAGTGATTTAATGATAAGT
	(SEQ ID NO: 91)	(SEQ ID NO: 1630)
131	PLAU	TATTTGTCGCGTTGAT
	(SEQ ID NO: 62)	(SEQ ID NO: 1633)
132	PLAU	ATTTGTTGTGTTGATGA
	(SEQ ID NO: 62)	(SEQ ID NO: 1634)
133	PLAU	TGTAATTCGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1635)
134	PLAU	TTGTAATTTGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1636)
135	PLAU	TTGGAGATCGCGTTTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1637)
136	PLAU	TTGGAGATTGTGTTTTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1638)
137	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1639)
138	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1640)
139	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1639)
140	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1640)
141	STAT1	GTTATTTTCGAGAGTTG
	(SEQ ID NO: 109)	(SEQ ID NO: 1641)
142	STAT1	GTTATTTTTGAGAGTTGT
	(SEQ ID NO: 109)	(SEQ ID NO: 1642)
143	LOT1	ATGGGTACGTTTAAGG
	(SEQ ID NO: 95)	(SEQ ID NO: 1649)
144	LOT1	TGGGTATGTTTAAGGG
	(SEQ ID NO: 95)	(SEQ ID NO: 1650)
145	GJB2	GGATTTCGTCGGTATT
	(SEQ ID NO: 111)	(SEQ ID NO: 1667)
146	GJB2	GGGGATTTTGTTGGTA
	(SEQ ID NO: 111)	(SEQ ID NO: 1668)
147	PRDM2	TGTAGAGACGACGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1675)
148	PRDM2	ATTGTAGAGATGATGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1676)
149	PRDM2	AGAGCGGGGTAGTAGT
	(SEQ ID NO: 114)	(SEQ ID NO: 1677)
150	PRDM2	TGAGAGTGTGGTAGTA
	(SEQ ID NO: 114)	(SEQ ID NO: 1678)
151	PRDM2	TGTTCGCGATGTTTTA
	(SEQ ID NO: 114)	(SEQ ID NO: 1679)
152	PRDM2	TGTTTGTGATGTTTTAGT
	(SEQ ID NO: 114)	(SEQ ID NO: 1680)
153	ALX4	AAGTCGATCGTTTTGT
	(SEQ ID NO: 64)	(SEQ ID NO: 1683)
154	ALX4	TGGAAGTTGATTGTTTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1684)
155	ALX4	ATATCGTTCGGGGGAA
	(SEQ ID NO: 64)	(SEQ ID NO: 2146)
156	ALX4	ATATCGTTCGGGGGAA
	(SEQ ID NO: 64)	(SEQ ID NO: 2146)
157	ALX4	TATTGCGAGGATTCGG
	(SEQ ID NO: 64)	(SEQ ID NO: 1685)
158	ALX4	ATTGTGAGGATTTGGT
	(SEQ ID NO: 64)	(SEQ ID NO: 1686)
159	ALX4	TTCGTAGCGTAGGGTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1667)
160	ALX4	TTTGTAGTGTAGGGTTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1688)
161	IGFBP7	ATTTTTTCGCGGGTAT
	(SEQ ID NO: 94)	(SEQ ID NO: 1710)
162	IGFBP7	TTTTTGTGGGTATTTTAG
	(SEQ ID NO: 94)	(SEQ ID NO: 1711)
163	IGFBP7	GGTATATTCGACGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1712)
164	IGFBP7	GGGTATATTTGATGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1713)
165	IGEBP7	GGTACGAGCGTTTTTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1714)
166	IGFBP7	TGGGTATGAGTGTTTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1715)
167	IGEBP7	AAAGCGTATTTAATTCGT
	(SEQ ID NO: 94)	(SEQ ID NO: 1716)
168	IGEBP7	AGTGTATTTAATTTGTGTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1717)
169	NME1	AGTCGAGATTGCGTTA
	(SEQ ID NO: 107)	(SEQ ID NO: 2147)
170	NME1	AGTTGAGATTGTGTTAG
	(SEQ ID NO: 107)	(SEQ ID NO: 2148)
171	NME1	ATCGTTTGAATTCGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2149)
172	NME1	ATTGTTTGAATTTGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2150)
173	NME1	ATCGTTTGAATTCGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2149)
174	NME1	ATTGTTTGAATTTGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2150)
175	NME1	AATTCGAGATTAGTTCGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1724)
176	NME1	AATTTGAGATTAGTTTGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1725)
177	NME1	AATTCGAGATTAGTTCGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1724)
178	NME1	AATTTGAGATTAGTTTGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1725)
179	NME1	TTTTAGTACGTTGGAAA
	(SEQ ID NO: 107)	(SEQ ID NO: 2151)
180	NME1	TTAGTATGTTGGAAAGTA
	(SEQ ID NO: 107)	(SEQ ID NO: 2152)
181	THBS1	TAAAGGGGCGTTCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1726)
182	THBS1	AAGGGGTGTTTGTATT
	(SEQ ID NO: 81)	(SEQ ID NO: 1727)
183	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1728)
184	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1729)
185	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1728)
186	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1729)
187	THBS1	TTGTGCGTTCGGAGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1730)
188	THBS1	TGTGTTTGGAGTAGAG
	(SEQ ID NO: 81)	(SEQ ID NO: 1731)
189	IL6	TTCGGTTATACGTAGG
	(SEQ ID NO: 99)	(SEQ ID NO: 1736)
190	IL6	TTTTGGTTATATGTAGGG
	(SEQ ID NO: 99)	(SEQ ID NO: 1737)
191	IL6	AGTTTAGTCGGTTTCGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1738)
192	IL6	AGTTTAGTTGGTTTTGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1739)
193	IL6	AGTTTAGTCGGTTTCGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1738)
194	IL6	AGTTTAGTTGGTTTTGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1739)
195	HOXA5	TAGTTTTCGGTCGGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1748)
196	HOXA5	TAGTTTTTGGTTGGAAG
	(SEQ ID NO: 78)	(SEQ ID NO: 1749)
197	HOXA5	ATCGGTAGTTGACGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1752)
198	HOXA5	ATTGGTAGTTGATGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1753)
199	HOXA5	ATGGGTAGTTGACGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1752)
200	HOXA5	ATTGGTAGTTGATGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1753)
201	GPC3	AATAGTCGCGTTTAGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1760)
202	GPC3	TAGTTGTGTTTAGGGAT
	(SEQ ID NO: 118)	(SEQ ID NO: 1761)
203	CLDN7	TTACGTTAAGTCGGGT
	(SEQ ID NO: 87)	(SEQ ID NO: 1764)
204	CLDN7	AGTTATGTTAAGTTGGG
	(SEQ ID NO: 87)	(SEQ ID NO: 1765)
205	SLIT2	ATTTCGTCGTAGTTTG
	(SEQ ID NO: 122)	(SEQ ID NO: 1774)
206	SLIT2	TTTTGTTGTAGTTTGGA
	(SEQ ID NO: 112)	(SEQ ID NO: 1775)
207	SLIT2	TAGCGGGTTCGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1776)
208	SLIT2	TTAGTGGGTTTGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1777)
209	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1778)
210	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1779)
211	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1778)
212	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1779)
213	IGSF4	AGGTAGATCGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1780)
214	IGSF4	AGGTAGATTGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1781)
215	IGSF4	AGGTAGATCGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1780)
216	IGSF4	AGGTAGATTGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1781)
217	IGSF4	TAGTCGTAGAGTCGGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1782)
218	IGSF4	GTTGTAGAGTTGGGTT
	(SEQ ID NO: 74)	(SEQ ID NO: 1783)
219	MCT1	AGTTAGTCGCGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1788)
220	MCT1	AGAGTTAGTTGTGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1789)
221	SEQ ID NO: 6	AAGTTTATCGGCGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1792)
222	SEQ ID NO: 6	AGAAGTTTATTGGTGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1793)
223	SEQ ID NO: 6	ATTTCGGAATTTAAGCGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1794)
224	SEQ ID NO: 6	TTTTGGAATTTAAGTGTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1795)
225	SEQ ID NO: 6	TAATTTCGGACGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1796)
226	SEQ ID NO: 6	TTTTGGATGTGGAGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1797)
227	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1798)
228	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1799)
229	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1798)
230	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1799)
231	SEQ ID NO: 6	TTTCGGTTTTCGTTAAT
	(SEQ ID NO: 6)	(SEQ ID NO: 1800)
232	SEQ ID NO: 6	TTTGGTTTTTGTTAATTTAG
	(SEQ ID NO: 6)	(SEQ ID NO: 1801)
233	SEQ ID NO: 8	ATAGGGCGGGATTTTA
	(SEQ ID NO: 8)	(SEQ ID NO: 2153)
234	SEQ ID NO: 8	GATAGGGTGGGATTTT
	(SEQ ID NO: 8)	(SEQ ID NO: 2154)
235	SEQ ID NO: 8	ATAAAGCGGGGTTTTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1804)
236	SEQ ID NO: 8	GGATAAAGTGGGGTTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1805)
237	SEQ ID NO: 8	AGGAGGCGAGAAATTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1806)
238	SEQ ID NO: 8	GAGGAGGTGAGAAATT
	(SEQ ID NO: 8)	(SEQ ID NO: 1807)
239	SEQ ID NO: 8	AGAAATTTCGGGGTAG
	(SEQ ID NO: 8)	(SEQ ID NO: 1808)
240	SEQ ID N0: 8	GAAATTTTGGGGTAGTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1809)
241	SEQ ID NO: 8	GGTAGTATCGTTTATAGA
	(SEQ ID NO: 8)	(SEQ ID NO: 1810)
242	SEQ ID NO: 8	GGGGTAGTATTGTTTATA
	(SEQ ID NO: 8)	(SEQ ID NO: 1811)
243	PROSTAGLANDIN E2	AGTGTATCGTTTTTCGG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1812)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
244	PROSTAGLANDIN E2	TAGTGTATTGTTTTTTGG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1813)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
245	PROSTAGLANDIN E2	TGCGTATCGTTAGTTA
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1814)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
246	PROSTAGLANDIN E2	AGGTTGTGTATTGTTAG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1815)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
247	PROSTAGLANDIN E2	ATTATTTCGGCGGTGA
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1816)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
248	PROSTAGLANDIN E2	GATTATTTTGGTGGTGA
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1817)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
249	PROSTAGLANDIN E2	TAAGTCGCGTAAGGAG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1818)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
250	PROSTAGLANDIN E2	AAGTTGTGTAAGGAGTA
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1819)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
251	MGC34831	GTCGGACGGATTTATA
	(SEQ ID NO: 52)	(SEQ ID NO: 2177)
252	MGC34831	TGGTTGGATGGATTTAT
	(SEQ ID NO: 52)	(SEQ ID NO: 2178)
253	SEQ ID NO:54	TGTGTAGCGGCGATTA
	(SEQ ID NO: 54)	(SEQ ID NO: 1830)
254	SEQ ID NO:54	GTGTGTAGTGGTGATT
	(SEQ ID NO: 54)	(SEQ ID NO: 1831)
255	ARL7	TAGATTTCGTAGTTTTTTA
	(SEQ ID NO: 30)	(SEQ ID NO: 1858)
256	ARL7	TAGATTTTGTAGTTTTTTAA
	(SEQ ID NO: 30)	(SEQ ID NO: 1859)
257	ARL7	TGGGTACGTTTACGGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1860)
258	ARL7	TGGGTATGTTTATGGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1861)
259	ARL7	GAAGAAATCGTTTTTGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1862)
260	ARL7	GAAGAAATTGTTTTTGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1863)
261	ARL7	TAGTAGGATCGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1864)
262	ARL7	ATAGTAGGATTGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1865)
263	THH	TTCGGAAGAAAAGCGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1870)
264	THH	TTTGGAAGAAAAGTGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1871)
265	THH	TTCGGAAGAAAAGCGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1870)
266	THH	TTTGGAAGAAAAGTGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1871)
267	THH	TATTCGGAAGTGATCGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1874)
268	THH	TATTTGGAAGTGATTGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1875)
269	THH	TATTCGGAAGTGATCGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1874)
270	THH	TATTTGGAAGTGATTGG
	(SEQ ID NO: 32)	(SEQ ID NO: 1875)
271	SENP3	TATTCGGATCGGGTTT
	(SEQ ID NO: 39)	(SEQ ID NO: 1876)
272	SENP3	TTTATTTGGATTGGGTT
	(SEQ ID NO: 39)	(SEQ ID NO: 1877)
273	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1878)
274	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1879)
275	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1878)
276	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1879)
277	SENP3	AGGACGTTTTTGATCGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1880)
278	SENP3	AGGATGTTTTTGATTGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1881)
279	SENP3	AGGACGTTTTTGATCGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1880)
280	SENP3	AGGATGTTTTTGATTGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1881)
281	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1882)
282	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1883)
283	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1882)
284	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1883)
285	SEQ ID NO: 42	AGGTCGAATAAAGCGT
	(SEQ ID NO: 42)	(SEQ ID NO: 2179)
286	SEQ ID NO: 42	GAGGTTGAATAAAGTGT
	(SEQ ID NO: 42)	(SEQ ID NO: 2180)
287	O60279	TAATTATCGGCGGTGT
	(SEQ ID NO: 47)	(SEQ ID NO: 1900)
288	O60279	ATTATTGGTGGTGTTTT
	(SEQ ID NO: 47)	(SEQ ID NO: 1901)
289	SEQ ID NO: 48	TATTTGGCGATTCGGA
	(SEQ ID NO: 48)	(SEQ ID NO: 1904)
290	SEQ ID NO: 48	TGGTGATTTGGAGATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1905)
291	SEQ ID NO: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1906)
292	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1907)
293	SEQ ID NO: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1906)
294	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1907)
295	SEQ ID NO: 48	AACGAATTTTTCGATATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1908)
296	SEQ ID NO: 48	TTTAATGAATTTTTTGATATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1909)
297	SEQ ID NO: 4	TTTTGTTCGCGTTGAA
	(SEQ ID NO: 4)	(SEQ ID NO: 1916)
298	SEQ ID NO: 4	TTGTTTGTGTTGAAGTA
	(SEQ ID NO: 4)	(SEQ ID NO: 1917)
299	SEQ ID NO: 5	AATGAGCGAGAAAGTA
	(SEQ ID NO: 5)	(SEQ ID NO: 1924)
300	SEQ ID NO: 5	AGAATGAGTGAGAAAGT
	(SEQ ID NO: 5)	(SEQ ID NO: 1925)
301	SEQ ID NO: 5	ATTAAACGGGATGGTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1926)
302	SEQ ID NO: 5	AATATTAAATGGGATGGT
	(SEQ ID NO: 5)	(SEQ ID NO: 1927)
303	SEQ ID NO: 5	GAGTTGCGAGGATTTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1928)
304	SEQ ID NO: 5	GGAGTTGTGAGGATTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1929)
305	SEQ ID NO: 5	TATGAGGTCGTATTGG
	(SEQ ID NO: 5)	(SEQ ID NO: 2163)
306	SEQ ID NO: 5	TATGAGGTTGTATTGGT
	(SEQ ID NO: 5)	(SEQ ID NO: 2164)
307	SEQ ID NO: 5	GGGAATCGTTGATTTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1930)
308	SEQ ID NO: 5	AGGGGAATTGTTGATT
	(SEQ ID NO: 5)	(SEQ ID NO: 1931)
309	SEQ ID NO: 1	GGTCGGCGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1942)
310	SEQ ID NO: 1	GGTTGGTGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1943)
311	SEQ ID NO: 1	GGTCGGCGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1942)
312	SEQ ID NO: 1	GGTTGGTGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1943)
313	SEQ ID NO: 1	GTCGGAAGTTTCGGGA
	(SEQ ID NO: 1)	(SEQ ID NO: 1948)
314	SEQ ID NO: 1	GTTGGAAGTTTTGGGAT
	(SEQ ID NO: 1)	(SEQ ID NO: 1949)
315	PROSTAGLANDIN E2	AGGTAATCGAGGCGGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1952)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
316	PROSTAGLANDIN E2	AGGTAATTGAGGTGGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1953)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
317	PROSTAGLANDIN E2	AGGTAATCGAGGCGGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1952)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
318	PROSTAGLANDIN E2	AGGTAATTGAGGTGGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1953)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
319	PROSTAGLANDIN E2	GGCGTCGAAAGTCGTT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1954)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
320	PROSTAGLANDIN E2	GGTGTTGAAAGTTGTTG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1955)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
321	PROSTAGLANDIN E2	TAATCGTTTGTTTACGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1956)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
322	PROSTAGLANDIN E2	AATTGTTTGTTTATGTAGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1957)
	TYPE (PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
323	LIM DOMAIN KINASE 1	TGTAGTCGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1966)
	(SEQ ID NO: 12)
324	LIM DOMAIN KINASE 1	TGTAGTTGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1967)
	(SEQ ID NO: 12)
325	LIM DOMAIN KINASE 1	TGTAGTCGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1966)
	(SEQ ID NO: 12)
326	LIM DOMAIN KINASE 1	TGTAGTTGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1967)
	(SEQ ID NO: 12)
327	LIM DOMAIN KINASE 1	GGATTATCGCGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1968)
	(SEQ ID NO: 12)
328	LIM DOMAIN KINASE 1	GGATTATTGTGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1969)
	(SEQ ID NO: 12)
329	LIM DOMAIN KINASE 1	GGATTATCGCGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1968)
	(SEQ ID NO: 12)
330	LIM DOMAIN KINASE 1	GGATTATTGTGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1969)
	(SEQ ID NO: 12)
331	LIM DOMAIN KINASE 1	GTCGGTAGTTTATCGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1970)
	(SEQ ID NO: 12)
332	LIM DOMAIN KINASE 1	GTTGGTAGTTTATTGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1971)
	(SEQ ID NO: 12)
333	LIM DOMAIN KINASE 1	GTCGGTAGTTTATCGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1970)
	(SEQ ID NO: 12)
334	LIM DOMAIN KINASE 1	GTTGGTAGTTTATTGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1971)
	(SEQ ID NO: 12)
335	MSF	GTTTCGAAATTGGCGT
	(SEQ ID NO: 13)	(SEQ ID NO: 1980)
336	MSF	TTTGAAATTGGTGTGG
	(SEQ ID NO: 13)	(SEQ ID NO: 1981)
337	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1982)
338	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1983)
339	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1982)
340	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1983)
341	MSF	TTACGGTTCGATTTTG
	(SEQ ID NO: 13)	(SEQ ID NO: 1984)
342	MSF	TATGGTTTGATTTTGGG
	(SEQ ID NO: 13)	(SEQ ID NO: 1985)
343	SEQ ID NO: 16	TTACGGATAGGGCGAT
	(SEQ ID NO: 16)	(SEQ ID NO: 1994)
344	SEQ ID NO: 16	TATGGATAGGGTGATTT
	(SEQ ID NO: 16)	(SEQ ID NO: 1995)
345	SEQ ID NO: 16	AGGCGTTGTCGGTGAT
	(SEQ ID NO: 16)	(SEQ ID NO: 1996)
346	SEQ ID NO: 16	AGGTGTTGTTGGTGATA
	(SEQ ID NO: 16)	(SEQ ID NO: 1997)
347	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1998)
348	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1999)
349	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1998)
350	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1999)
351	SEQ ID NO: 18	TTACGTCGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2004)
352	SEQ ID NO: 18	TTTTATGTTGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2005)
353	SEQ ID NO: 18	AAAGCGGAGTCGTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2010)
354	SEQ ID NO: 18	AGTGGAGTTGTTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2011)
355	SEQ ID NO: 19	AGGTTTTCGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2012)
356	SEQ ID NO: 19	TAGGTTTTTGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2013)
357	SEQ ID NO: 19	TGAGATTCGTTTTTTAAA
	(SEQ ID NO: 19)	(SEQ ID NO: 2014)
358	SEQ ID NO: 19	GGTGAGATTTGTTTTTTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2015)
359	PRDM6	TTGTCGGGTTACGGGA
	(SEQ ID NO: 20)	(SEQ ID NO: 2020)
360	PRDM6	GTTGGGTTATGGGAGA
	(SEQ ID NO: 20)	(SEQ ID NO: 2021)
361	NR2E1	AATGTAGGGGCGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2028)
362	NR2E1	TAAATGTAGTGGTGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2029)
363	NR2E1	GTCGTTATCGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2030)
364	NR2E1	GTTGTTATTGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2031)
365	NR2E1	GTCGTTATCGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2030)
366	NR2E1	GTTGTTATTGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2031)
367	NR2E1	GACGTAAGTTTCGGGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2032)
368	NR2E1	GGATGTAAGTTTTGGG
	(SEQ ID NO: 22)	(SEQ ID NO: 2033)
369	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2036)
370	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2037)
371	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2036)
372	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2037)
373	NR2E1	AGGCGAGTCGGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2038)
374	NR2E1	AGGTGAGTTGGAGTTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2039)
375	NR2E1	TAAGTCGAGCGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2040)
376	NR2E1	TAGTAAGTTGAGTGAGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2041)
377	NR2E1	AGGGACGCGAAAATTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2042)
378	NR2E1	GGAGGGATGTGAAAAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2043)
379	PCDH7	ATCGTAGTCGGTTTTA
	(SEQ ID NO: 23)	(SEQ ID NO: 2044)
380	PCDH7	GATTATTGTAGTTGGTTT
	(SEQ ID NO: 23)	(SEQ ID NO: 2045)
381	RTTN	TAGTGGCGCGGTAGTT
	(SEQ ID NO: 25)	(SEQ ID NO: 2046)
382	RTTN	TAGTGGTGTGGTAGTTT
	(SEQ ID NO: 25)	(SEQ ID NO: 2047)
383	RTTN	TAGGACGTGTTTTCGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2048)
384	RTTN	AGGATGTGTTTTTGGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2049)
385	SNAP25	GTTATTATTCGGTACGT
	(SEQ ID NO: 33)	(SEQ ID NO: 2169)
386	SNAP25	AGTTATTATTTGGTATGTAT
	(SEQ ID NO: 33)	(SEQ ID NO: 2170)
387	SEQ ID NO: 26	TTAAGTATCGAGGCGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2054)
388	SEQ ID NO: 26	TTTTAAGTATTGAGGTGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2055)
389	SEQ ID NO: 26	AATTTTGGTCGTTTAGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2056)
390	SEQ ID NO: 26	AAATTTTGGTTGTTTAGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2057)
391	SEQ ID NO: 26	TTCGTATTGACGTTAAT
	(SEQ ID NO: 26)	(SEQ ID NO: 2058)
392	SEQ ID NO: 26	TTTGTATTGATGTTAATAGA
	(SEQ ID NO: 26)	(SEQ ID NO: 2059)
393	SEQ ID NO: 28	ATTAGGCGAGTTTCGT
	(SEQ ID NO: 28)	(SEQ ID NO: 2066)
394	SEQ ID NO: 28	TTAGGTGAGTTTTGTTT
	(SEQ ID NO: 28)	(SEQ ID NO: 2067)
395	SEQ ID NO: 31	TTTACGTAGGGCGATT
	(SEQ ID NO: 31)	(SEQ ID NO: 2068)
396	SEQ ID NO: 31	ATTTTTATGTAGGGTGAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2069)
397	SEQ ID NO: 31	GATACGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2070)
398	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2071)
399	SEQ ID NO: 31	GATACGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2070)
400	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2071)
401	SEQ ID NO: 31	TTCGGGCGTTTTATAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2072)
402	SEQ ID NO: 31	GGTTTGGGTGTTTTATA
	(SEQ ID NO: 31)	(SEQ ID NO: 2073)
403	HOXB13	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2076)
404	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2077)
405	HOXB13	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2076)
406	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2077)
407	(SEQ ID NO: 35)	GGAGGTGCGAATTTAA
		(SEQ ID NO: 2080)
408	(SEQ ID NO: 35)	GGGAGGTGTGAATTTA
		(SEQ ID NO: 2081)
409	(SEQ ID NO: 35)	AAATAGTCGTTTGGGA
		(SEQ ID NO: 2082)
410	(SEQ ID NO: 35)	AAATAGTTGTTTGGGAG
		(SEQ ID NO: 2083)
411	(SEQ ID NO: 35)	AGAAAATATACGAGATTTAT
		(SEQ ID NO: 2084)
412	(SEQ ID NO: 35)	AGAAAATATATGAGATTTATT
		(SEQ ID NO: 2085)
413	(SEQ ID NO: 35)	TAAAGACGGGAAGAGA
		(SEQ ID NO: 2086)
414	(SEQ ID NO: 35)	ATAAAGATGGGAAGAGA
		(SEQ ID NO: 2087)
415	MGC10561	TTTTTTACGTTAAGGGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2088)
416	MGC10561	TTTTTATGTTAAGGGGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2089)
417	LMX1A	GTCGGGTTTTTCGGAA
	(SEQ ID NO: 38)	(SEQ ID NO: 2092)
418	LMX1A	GTTGGGTTTTTTGGAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2093)
419	LMX1A	GTCGAGATTTTATCGAAA
	(SEQ ID NO: 38)	(SEQ ID NO: 2094)
420	LMX1A	GTTGAGATTTTATTGAAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2095)
421	LMX1A	AGTATTCGGGCGGGTA
	(SEQ ID NO: 38)	(SEQ ID NO: 2096)
422	LMX1A	GTAGTATTTGGGTGGG
	(SEQ ID NO: 38)	(SEQ ID NO: 2097)
423	LMX1A	AACGAAATTACGTGTAT
	(SEQ ID NO: 38)	(SEQ ID NO: 2098)
424	LMX1A	TGAAATGAAATTATGTGTA
	(SEQ ID NO: 38)	(SEQ ID NO: 2099)
425	TITF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2104)
426	TITF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2105)
427	TITF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2104)
428	TITF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2105)
429	TITF1	TTAGGTCGCGTTTGTA
	(SEQ ID NO: 41)	(SEQ ID NO: 2108)
430	TITF1	AGGTTGTGTTTGTAGA
	(SEQ ID NO: 41)	(SEQ ID NO: 2109)
431	DDXF1	AACGTGCGGGGTTTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2116)
432	DDXF1	TGAATGTGTGGGGTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2117)
433	SEQ ID NO: 45	AGCGAACGTTTATTTT
	(SEQ ID NO: 45)	(SEQ ID NO: 2118)
434	SEQ ID NO: 45	TAGGAGAGTGAATGTTT
	(SEQ ID NO: 45)	(SEQ ID NO: 2119)
435	SEQ ID NO: 2	TAGTAGTCGGCGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2130)
436	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2131)
437	SEQ ID NO: 2	TAGTAGTCGGGGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2130)
438	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2131)
439	SEQ ID NO: 3	TTGCGTTAATTCGGTA
	(SEQ ID NO: 3)	(SEQ ID NO: 2132)
440	SEQ ID NO: 3	AATTTGTGTTAATTTGGT
	(SEQ ID NO: 3)	(SEQ ID NO: 2133)
441	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2134)
442	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2135)
443	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2134)
444	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2135)
445	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2136)
446	SEQ ID NO: 3	GGTTGAAGAGTTGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2137)
447	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2136)
448	SEQ ID NO: 3	GGTTGAAGAGTTGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2137)
449	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2138)
450	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2139)
451	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2138)
452	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2139)

TABLE 18
Breast cancer vs. lymphocytes
No:	Gene	Oligo:
1	SCGB3A1	TATTGGCGTCGAGGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2181)
2	SCGB3A1	TATTGGTGTTGAGGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2182)
3	SCGB3A1	TATTGGCGTCGAGGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2181)
4	SCGB3A1	TATTGGTGTTGAGGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2182)
5	SCGB3A1	GGCGTAGAAGGCGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2140)
6	SCGB3A1	GGTGTAGAAGGTGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2141)
7	SCGB3A1	GGCGTAGAAGGCGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2140)
8	SCGB3A1	GGTGTAGAAGGTGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2141)
9	SCGB3A1	TAGTGTTCGACGTTGT
	(SEQ ID NO: 115)	(SEQ ID NO: 1475)
10	SCGB3A1	TAGTGTTTGATGTTGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 1476)
11	SASH1	TAGATTCGAGGTGCGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1477)
12	SASH1	TAGATTTGAGGTGTGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1478)
13	SASH1	TAGATTCGAGGTGCGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1477)
14	SASH1	TAGATTTGAGGTGTGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1478)
15	SASH1	ATTCGGTATTCGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1479)
16	SASH1	ATTTGGTATTTGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1480)
17	SASH1	ATTCGGTATTCGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1479)
18	SASH1	ATTTGGTATTTGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1480)
19	ARH1/NOEY2	TAAAACGTTCGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1485)
20	ARH1/NOEY2	TTTAAAATGTTTGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1486)
21	ARH1/NOEY2	TGTATTCGTCGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1487)
22	ARH1/NOEY2	AATGTATTTGTTGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1488)
23	ARH1/NOEY2	TTAGACGGAGTTCGGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1489)
24	ARH1/NOEY2	TAGATGGAGTTTGGAGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1490)
25	ARH1/NOEY2	TAGACGTAGGCGTATT
	(SEQ ID NO: 97)	(SEQ ID NO: 1491)
26	ARH1/NOEY2	GGGTAGATGTAGGTGT
	(SEQ ID NO: 97)	(SEQ ID NO: 1492)
27	CCND2	TTAGGGTCGATCGTGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1493)
28	CCND2	TAGGGTTGATTGTGTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1494)
29	CCND2	TTATCGTAGTCGGTTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1495)
30	CCND2	GATTTTATTGTAGTTGGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1496)
31	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1497)
32	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1498)
33	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1497)
34	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1498)
35	CDKN1A	ATTAGGGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1501)
36	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1502)
37	CDKN1A	ATTAGGGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1501)
38	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1502)
39	CDKN2A	GGCGTTGTTTAACGTAT
	(SEQ ID NO: 57)	(SEQ ID NO: 1503)
40	CDKN2A	GGGTGTTGTTTAATGTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1504)
41	CDKN2A	AATAGTTACGGTCGGA
	(SEQ ID NO: 57)	(SEQ ID NO: 1505)
42	CDKN2A	AGTTATGGTTGGAGGT
	(SEQ ID NO: 57)	(SEQ ID NO: 1506)
43	CDKN2A	GTCGGAGGTCGATTTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1507)
44	CDKN2A	GGTTGGAGGTTGATTTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1508)
45	DAPK1	TTTCGGAGATTCGGTT
	(SEQ ID NO: 98)	(SEQ ID NO: 1509)
46	DAPK1	TTTGGAGATTTGGTTTT
	(SEQ ID NO: 98)	(SEQ ID NO: 1510)
47	DAPK1	TTTTAGCGTCGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1511)
48	DAPK1	TTTTAGTGTTGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1512)
49	DAPK1	TTTTAGCGTCGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1511)
50	DAPK1	TTTTAGTGTTGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1512)
51	EYA4	GGTATAAAATCGTAAATTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1513)
52	EYA4	GGGTATAAAATTGTAAATTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1514)
53	EYA4	TATGTAGTCGCGTAGT
	(SEQ ID NO: 58)	(SEQ ID NO: 1515)
54	EYA4	TTTATGTAGTTGTGTAGT
	(SEQ ID NO: 58)	(SEQ ID NO: 1516)
55	EYA4	GTTTAGATACGAAATGTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1517)
56	EYA4	GTTTAGATATGAAATGTTAT
	(SEQ ID NO: 58)	(SEQ ID NO: 1518)
57	EYA4	AGTTTTGACGTCGTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1519)
58	EYA4	TTGATGTTGTTTTGGAA
	(SEQ ID NO: 58)	(SEQ ID NO: 1520)
59	FHIT	TTTAAGTATCGATTTTAGT
	(SEQ ID NO: 76)	(SEQ ID NO: 2183)
60	FHIT	TAAGTATTGATTTTAGTTTTA
	(SEQ ID NO: 76)	(SEQ ID NO: 2184)
61	FHIT	GTTACGTTAGCGGGTT
	(SEQ ID NO: 76)	(SEQ ID NO: 1521)
62	FHIT	GGTTATGTTAGTGGGT
	(SEQ ID NO: 76)	(SEQ ID NO: 1522)
63	GSTP1	GGCGATTTCGGGGATT
	(SEQ ID NO: 59)	(SEQ ID NO: 1525)
64	GSTP1	GGTGATTTTGGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1526)
65	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1527)
66	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1528)
67	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1527)
68	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1528)
69	GSTP1	AGTTCGCGGGATTTTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1529)
70	GSTP1	GGAGTTTGTGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1530)
71	GSTP1	AGTTTTCGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1531)
72	GSTP1	TAGTTTTTGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1532)
73	HIC1	TATCGAAGTTTTCGGG
	(SEQ ID NO: 85)	(SEQ ID NO: 1533)
74	HIC1	TATTGAAGTTTTTGGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1534)
75	HIC1	TAGCGGTTATTTCGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1535)
76	HIC1	TTTAGTGGTTATTTTGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1536)
77	HIC1	TACGTTTTTCGTAGCGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1537)
78	HIC1	ATTATGTTTTTTGTAGTGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1538)
79	HIC1	TTCGGTTTTGTCGTATA
	(SEQ ID NO: 85)	(SEQ ID NO: 1539)
80	HIC1	TTTGGTTTTGTTGTATAG
	(SEQ ID NO: 85)	(SEQ ID NO: 1540)
81	PGR	TTTCGAGGTCGGATTT
	(SEQ ID NO: 83)	(SEQ ID NO: 1543)
82	PGR	TTTGAGGTTGGATTTTT
	(SEQ ID NO: 83)	(SEQ ID NO: 1544)
83	PGR	GTGTCGTTTAGTCGTA
	(SEQ ID NO: 83)	(SEQ ID NO: 1545)
84	PGR	GTTGTTTAGTTGTAGGT
	(SEQ ID NO: 83)	(SEQ ID NO: 1546)
85	SERPINB5	TTATTAACGTGTTTGAGA
	(SEQ ID NO: 68)	(SEQ ID NO: 1549)
86	SERPINB5	TTATTAATGTGTTTGAGAA
	(SEQ ID NO: 68)	(SEQ ID NO: 1550)
87	SERPINB5	ATTGTCGTACGTATGT
	(SEQ ID NO: 68)	(SEQ ID NO: 1551)
88	SERPINB5	AGAGGATTGTTGTATGTA
	(SEQ ID NO: 68)	(SEQ ID NO: 1552)
89	SERPINB5	TTTTTTGTTCGAATATGT
	(SEQ ID NO: 68)	(SEQ ID NO: 1553)
90	SERPINB5	TTTGTTTGAATATGTTGG
	(SEQ ID NO: 68)	(SEQ ID NO: 1554)
91	RARB	ATGTCGAGAACGCGAG
	(SEQ ID NO: 88)	(SEQ ID NO: 1555)
92	RARB	GGATGTTGAGAATGTGA
	(SEQ ID NO: 88)	(SEQ ID NO: 1556)
93	RARB	AGCGATTCGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1557)
94	RARB	AGTGATTTGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1558)
95	RARB	AGCGATTCGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1557)
96	RARB	AGTGATTTGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1558)
97	RARB	TAGGATTCGGAACGTA
	(SEQ ID NO: 88)	(SEQ ID NO: 1559)
98	RARB	GGTAGGATTTGGAATGT
	(SEQ ID NO: 88)	(SEQ ID NO: 1560)
99	SFN	TAGTACGGTGTCGTAT
	(SEQ ID NO: 69)	(SEQ ID NO: 1561)
100	SFN	GTTTAGTATGGTGTTGT
	(SEQ ID NO: 69)	(SEQ ID NO: 1562)
101	SFN	TACGTATTTCGGGTTT
	(SEQ ID NO: 69)	(SEQ ID NO: 1563)
102	SFN	TATTTATGTATTTTGGGTT
	(SEQ ID NO: 69)	(SEQ ID NO: 1564)
103	SFN	TTCGTTTTTCGTAGGAG
	(SEQ ID NO: 69)	(SEQ ID NO: 1565)
104	SFN	TTTGTTTTTTGTAGGAGA
	(SEQ ID NO: 69)	(SEQ ID NO: 1566)
105	SFN	TTTATAGCGTTCGGTT
	(SEQ ID NO: 69)	(SEQ ID NO: 2185)
106	SFN	ATAGTGTTTGGTTTGTT
	(SEQ ID NO: 69)	(SEQ ID NO: 2186)
107	TERT	AGGTGTACGGTTTCGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2187)
108	TERT	AGGTGTATGGTTTTGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2188)
109	TERT	AGGTGTACGGTTTCGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2187)
110	TERT	AGGTGTATGGTTTTGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2188)
111	TERT	TATAACGAACGTCGTT
	(SEQ ID NO: 92)	(SEQ ID NO: 2142)
112	TERT	AGGTATAATGAATGTTGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2143)
113	TGFBR2	ATGGGGCGGACGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1567)
114	TGFBR2	ATGGGGTGGATGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1568)
115	TGFBR2	ATGGGGCGGACGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1567)
116	TGFBR2	ATGGGGTGGATGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1568)
117	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1569)
118	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1570)
119	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1569)
120	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1570)
121	TIMP3	TTATTAACGGAGGAAGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1571)
122	TIMP3	TATTAATGGAGGAAGGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1572)
123	CDH13	TAAAACGAGGGAGCGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1583)
124	CDH13	AAAATGAGGGAGTGTT
	(SEQ ID NO: 70)	(SEQ ID NO: 1584)
125	CDH13	TAGTCGCGTGTATGAA
	(SEQ ID NO: 70)	(SEQ ID NO: 1585)
126	CDH13	TGTAGTTGTGTGTATGA
	(SEQ ID NO: 70)	(SEQ ID NO: 1586)
127	CDH13	ATGAAAACGTCGTCGG
	(SEQ ID NO: 70)	(SEQ ID NO: 1587)
128	CDH13	AATGAAAATGTTGTTGG
	(SEQ ID NO: 70)	(SEQ ID NO: 1588)
129	CDH13	TAGTCGAGAATTTCGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1589)
130	CDH13	TGTAGTTGAGAATTTTGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1590)
131	TMS1/ASC	TTCGTTTCGGAGTCGA
	(SEQ ID NO: 84)	(SEQ ID NO: 1591)
132	TMS1/ASC	TTTGTTTTGGAGTTGAT
	(SEQ ID NO: 84)	(SEQ ID NO: 1592)
133	APAF1	GTGTCGTAGCGGTATT
	(SEQ ID NO: 82)	(SEQ ID NO: 1593)
134	APAF1	GGTGTTGTAGTGGTAT
	(SEQ ID NO: 82)	(SEQ ID NO: 1594)
135	APAF1	AGTAGCGTCGGGTTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1595)
136	APAF1	GAGTAGTGTTGGGTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1596)
137	SYK	GATCGATGCGGTTTAT
	(SEQ ID NO: 60)	(SEQ ID NO: 1599)
138	SYK	GGGATTGATGTGGTTT
	(SEQ ID NO: 60)	(SEQ ID NO: 1600)
139	SYK	TTATTCGGTCGGGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1603)
140	SYK	TTTATTTGGTTGGGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1604)
141	FABP3	GTGATGCGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1607)
142	FABP3	GTGATGTGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1608)
143	FABP3	GTGATGCGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1607)
144	FABP3	GTGATGTGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1608)
145	FABP3	TAAAGCGGTAGTTCGG
	(SEQ ID NO: 77)	(SEQ ID NO: 1609)
146	FABP3	AAGTGGTAGTTTGGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1610)
147	FABP3	TATTGGCGTTGACGTA
	(SEQ ID NO: 77)	(SEQ ID NO: 1611)
148	FABP3	TGGTGTTGATGTAGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1612)
149	RASSF1A	TACGGGTATTTTCGCGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1613)
150	RASSF1A	ATATGGGTATTTTTGTGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1614)
151	RASSF1A	AGAGCGCGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1615)
152	RASSF1A	GAGAGTGTGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1616)
153	RASSF1A	AGTAAATCGGATTAGGA
	(SEQ ID NO: 90)	(SEQ ID NO: 1617)
154	RASSF1A	AGTAAATTGGATTAGGAG
	(SEQ ID NO: 90)	(SEQ ID NO: 1618)
155	TWIST	AGTAAAGGCGTTGCGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1619)
156	TWIST	AGTAAAGGTGTTGTGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1620)
157	TWIST	AGTAAAGGCGTTGCGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1619)
158	TWIST	AGTAAAGGTGTTGTGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1620)
159	TWIST	TATTTTTCGAGGCGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1621)
160	TWIST	TTTTGAGGTGTAGTTTT
	(SEQ ID NO: 100)	(SEQ ID NO: 1622)
161	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1623)
162	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1624)
163	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1623)
164	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1624)
165	TWIST	TAGGTCGGGACGTAAA
	(SEQ ID NO: 100)	(SEQ ID NO: 1625)
166	TWIST	AGTAGGTTGGGATGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1626)
167	ESR2	TTTACGTGATCGAGTT
	(SEQ ID NO: 91)	(SEQ ID NO: 1631)
168	ESR2	AGTTTATGTGATTGAGTT
	(SEQ ID NO: 91)	(SEQ ID NO: 1632)
169	PLAU	TATTTGTCGCGTTGAT
	(SEQ ID NO: 62)	(SEQ ID NO: 1633)
170	PLAU	ATTTGTTGTGTTGATGA
	(SEQ ID NO: 62)	(SEQ ID NO: 1634)
171	PLAU	TGTAATTCGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1635)
172	PLAU	TTGTAATTTGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1636)
173	PLAU	TTGGAGATCGCGTTTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1637)
174	PLAU	TTGGAGATTGTGTTTTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1638)
175	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1639)
176	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1640)
177	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1639)
178	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1640)
179	STAT1	ATATGATTTCGGAATTTTA
	(SEQ ID NO: 109)	(SEQ ID NO: 2189)
180	STAT1	ATATGATTTTGGAATTTTAA
	(SEQ ID NO: 109)	(SEQ ID NO: 2190)
181	BRCA1	TTTCGTGGTAACGGAA
	(SEQ ID NO: 66)	(SEQ ID NO: 1645)
182	BRCA1	TTTGTGGTAATGGAAAA
	(SEQ ID NO: 66)	(SEQ ID NO: 1646)
183	LOT1	ATGGGTACGTTTAAGG
	(SEQ ID NO: 95)	(SEQ ID NO: 1649)
184	LOT1	TGGGTATGTTTAAGGG
	(SEQ ID NO: 95)	(SEQ ID NO: 1650)
185	LOT1	AAATTAGTTACGTTATTTAA
	(SEQ ID NO: 95)	(SEQ ID NO: 1651)
186	LOT1	TGAAATTAGTTATGTTATTTA
	(SEQ ID NO: 95)	(SEQ ID NO: 1652)
187	LOT1	ATGTCGGTTATTACGT
	(SEQ ID NO: 95)	(SEQ ID NO: 1653)
188	LOT1	TGTTGGTTATTATGTAGA
	(SEQ ID NO: 95)	(SEQ ID NO: 1654)
189	PRSS8	AGTTGGCGGAGTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1655)
190	PRSS8	AGTTGGTGGAGTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1656)
191	PRSS8	AGTTGGCGGAGTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1655)
192	PRSS8	AGTTGGTGGAGTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1656)
193	PRSS8	TTGGTGATTCGTTTATAT
	(SEQ ID NO: 72)	(SEQ ID NO: 1657)
194	PRSS8	GTTGGTGATTTGTTTATA
	(SEQ ID NO: 72)	(SEQ ID NO: 1658)
195	PRSS8	TGTTCGTTTCGGATAT
	(SEQ ID NO: 72)	(SEQ ID NO: 1659)
196	PRSS8	TTTGTTTTGGATATTTTAG
	(SEQ ID NO: 72)	(SEQ ID NO: 1660)
197	SLC19A1	GTCGTGCGGTTTTTAA
	(SEQ ID NO: 116)	(SEQ ID NO: 1663)
198	SLC19A1	GGTTGTGTGGTTTTTAA
	(SEQ ID NO: 116)	(SEQ ID NO: 1664)
199	SLC19A1	TTACGAAGGCGGTTTA
	(SEQ ID NO: 116)	(SEQ ID NO: 1665)
200	SLC19A1	TTTTATGAAGGTGGTTT
	(SEQ ID NO: 116)	(SEQ ID NO: 1666)
201	GJB2	GGATTTCGTCGGTATT
	(SEQ ID NO: 111)	(SEQ ID NO: 1667)
202	GJB2	GGGGATTTTGTTGGTA
	(SEQ ID NO: 111)	(SEQ ID NO: 1668)
203	HS3ST2	GAATCGGAGAGGCGAG
	(SEQ ID NO: 113)	(SEQ ID NO: 1671)
204	HS3ST2	AATTGGAGAGGTGAGG
	(SEQ ID NO: 113)	(SEQ ID NO: 1672)
205	HS3ST2	GGGTAATCGTTTGGTA
	(SEQ ID NO: 113)	(SEQ ID NO: 1673)
206	HS3ST2	GGGTAATTGTTTGGTAT
	(SEQ ID NO: 113)	(SEQ ID NO: 1674)
207	PRDM2	TGTAGAGACGACGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1675)
208	PRDM2	ATTGTAGAGATGATGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1676)
209	PRDM2	AGAGCGCGGTAGTAGT
	(SEQ ID NO: 114)	(SEQ ID NO: 1677)
210	PRDM2	TGAGAGTGTGGTAGTA
	(SEQ ID NO: 114)	(SEQ ID NO: 1678)
211	PRDM2	TGTTCGCGATGTTTTA
	(SEQ ID NO: 114)	(SEQ ID NO: 1679)
212	PRDM2	TGTTTGTGATGTTTTAGT
	(SEQ ID NO: 114)	(SEQ ID NO: 1680)
213	PRDM2	AGTATATAAACGTAGATTTT
	(SEQ ID NO: 114)	(SEQ ID NO: 1681)
214	PRDM2	AAGTATATAATGTAGATTTT
	(SEQ ID NO: 114)	(SEQ ID NO: 1682)
215	ALX4	AAGTCGATCGTTTTGT
	(SEQ ID NO: 64)	(SEQ ID NO: 1683)
216	ALX4	TGGAAGTTGATTGTTTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1684)
217	ALX4	TATTGCGAGGATTCGG
	(SEQ ID NO: 64)	(SEQ ID NO: 1685)
218	ALX4	ATTGTGAGGATTTGGT
	(SEQ ID NO: 64)	(SEQ ID NO: 1686)
219	ALX4	TTCGTAGCGTAGGGTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1687)
220	ALX4	TTTGTAGTGTAGGGTTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1688)
221	S100A7	TATAGTCGGGGTGATA
	(SEQ ID NO: 96)	(SEQ ID NO: 1689)
222	S100A7	TTTATAGTTGGGGTGAT
	(SEQ ID NO: 96)	(SEQ ID NO: 1690)
223	S100A7	AGTCGGGCGTTAGTAA
	(SEQ ID NO: 96)	(SEQ ID NO: 1691)
224	S100A7	GAGTTGGGTGTTAGTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1692)
225	S100A7	GGATGGCGGAAGTTTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1693)
226	S100A7	GGATGGTGGAAGTTTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1694)
227	S100A7	GGATGGCGGAAGTTTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1693)
228	S100A7	GGATGGTGGAAGTTTA
	(SEQ ID NO: 96)	(SEQ ID NO: 1694)
229	APC	GATTCGTATTTCGTAGT
	(SEQ ID NO: 65)	(SEQ ID NO: 1695)
230	APC	GATTCGTATTTCGTAGT
	(SEQ ID NO: 65)	(SEQ ID NO: 1695)
231	APC	AGCGTTTTGGTTCGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1696)
232	APC	AGTGTTTTGGTTTGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1697)
233	APC	AGCGTTTTGGTTCGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1696)
234	APC	AGTGTTTTGGTTTGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1697)
235	APC	TTAATCGGCGGGTTTT
	(SEQ ID NO: 65)	(SEQ ID NO: 1698)
236	APC	AGTTAATTGGTGGGTT
	(SEQ ID NO: 65)	(SEQ ID NO: 1699)
237	CDH1	AGGTATCGTTTTTCGT
	(SEQ ID NO: 79)	(SEQ ID NO: 2191)
238	CDH1	GAGGTATTGTTTTTTGTA
	(SEQ ID NO: 79)	(SEQ ID NO: 2192)
239	SEQ ID NO: 2	TAGGGGTTCGATTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2193)
240	SEQ ID NO: 2	AGGGGTTTGATTAGGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2194)
241	SEQ ID NO: 2	TAGGTATACGAAAGAGTA
	(SEQ ID NO: 2)	(SEQ ID NO: 1704)
242	SEQ ID NO: 2	TTAGGTATATGAAAGAGTA
	(SEQ ID NO: 2)	(SEQ ID NO: 1705)
243	IGFBP7	TAGTCGCGGAATGTTA
	(SEQ ID NO: 94)	(SEQ ID NO: 1708)
244	IGFBP7	TTGGTAGTTGTGGAAT
	(SEQ ID NO: 94)	(SEQ ID NO: 1709)
245	IGFBP7	ATTTTTTCGCGGGTAT
	(SEQ ID NO: 94)	(SEQ ID NO: 1710)
246	IGFBP7	TTTTTGTGGGTATTTTAG
	(SEQ ID NO: 94)	(SEQ ID NO: 1711)
247	IGFBP7	GGTATATTCGACGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1712)
248	IGFBP7	GGGTATATTTGATGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1713)
249	IGFBP7	GGTACGAGCGTTTTTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1714)
250	IGFBP7	TGGGTATGAGTGTTTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1715)
251	IGFBP7	AAAGCGTATTTAATTCGT
	(SEQ ID NO: 94)	(SEQ ID NO: 1716)
252	IGFBP7	AGTGTATTTAATTTGTGTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1717)
253	SOD2	GTCGTTTAGTCGGTTTA
	(SEQ ID NO: 105)	(SEQ ID NO: 1718)
254	SOD2	GTTGTTTAGTTGGTTTAT
	(SEQ ID NO: 105)	(SEQ ID NO: 1719)
255	SOD2	TATTAGGCGGTTGCGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1720)
256	SOD2	TATTAGGTGGTTGTGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1721)
257	SOD2	TATTAGGCGGTTGCGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1720)
258	SOD2	TATTAGGTGGTTGTGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1721)
259	NME1	AGTCGAGATTGCGTTA
	(SEQ ID NO: 107)	(SEQ ID NO: 2147)
260	NME1	AGTTGAGATTGTGTTAG
	(SEQ ID NO: 107)	(SEQ ID NO: 2148)
261	NME1	ATCGTTTGAATTCGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2149)
262	NME1	ATTGTTTGAATTTGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2150)
263	NME1	ATCGTTTGAATTCGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2149)
264	NME1	ATTGTTTGAATTTGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2150)
265	NME1	AATTCGAGATTAGTTCGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1724)
266	NME1	AATTTGAGATTAGTTTGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1725)
267	NME1	AATTCGAGATTAGTTCGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1724)
268	NME1	AATTTGAGATTAGTTTGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1725)
269	NME1	TTTTAGTACGTTGGAAA
	(SEQ ID NO: 107)	(SEQ ID NO: 2151)
270	NME1	TTAGTATGTTGGAAAGTA
	(SEQ ID NO: 107)	(SEQ ID NO: 2152)
271	THBS1	TAAAGGGGCGTTCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1726)
272	THBS1	AAGGGGTGTTTGTATT
	(SEQ ID NO: 81)	(SEQ ID NO: 1727)
273	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1728)
274	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1729)
275	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1728)
276	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1729)
277	THBS1	TTGTGCGTTCGGAGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1730)
278	THBS1	TGTGTTTGGAGTAGAG
	(SEQ ID NO: 81)	(SEQ ID NO: 1731)
279	ESR1	AAATCGGCGGGTTATT
	(SEQ ID NO: 75)	(SEQ ID NO: 1732)
280	ESR1	AGAAATTGGTGGGTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1733)
281	ESR1	AGATCGTGTTTTCGTA
	(SEQ ID NO: 75)	(SEQ ID NO: 2195)
282	ESR1	ATTGTGTTTTTGTAGGG
	(SEQ ID NO: 75)	(SEQ ID NO: 2196)
283	IL6	AGATGTCGTCGAGGAT
	(SEQ ID NO: 99)	(SEQ ID NO: 2197)
284	IL6	ATGTTGTTGAGGATGTA
	(SEQ ID NO: 99)	(SEQ ID NO: 2198)
285	IL6	AGTTTAGTCGGTTTCGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1738)
286	IL6	AGTTTAGTTGGTTTTGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1739)
287	IL6	AGTTTAGTCGGTTTCGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1738)
288	IL6	AGTTTAGTTGGTTTTGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1739)
289	CASP8	ATTTTTTAAACGGGTTTA
	(SEQ ID NO: 71)	(SEQ ID NO: 1742)
290	CASP8	TTTTAAATGGGTTTATAGG
	(SEQ ID NO: 71)	(SEQ ID NO: 1743)
291	HOXA5	TTCGAGTTCGGTTGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1746)
292	HOXA5	GTTTGAGTTTGGTTGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1747)
293	HOXA5	TAATTCGATTTCGGTTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1750)
294	HOXA5	TTTAATTTGATTTTGGTTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1751)
295	SNCG	TGCGGTAGTATTCGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1758)
296	SNCG	TGTGGTAGTATTTGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1759)
297	SNCG	TGCGGTAGTATTCGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1758)
298	SNCG	TGTGGTAGTATTTGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1759)
299	SNCG	TATCGGGGATAGTCGTT
	(SEQ ID NO: 73)	(SEQ ID NO: 2199)
300	SNCG	TATTGGGGATAGTTGTT
	(SEQ ID NO: 73)	(SEQ ID NO: 2200)
301	SNCG	TATCGGGGATAGTCGTT
	(SEQ ID NO: 73)	(SEQ ID NO: 2199)
302	SNCG	TATTGGGGATAGTTGTT
	(SEQ ID NO: 73)	(SEQ ID NO: 2200)
303	SNCG	TATCGGCGTTAATAGG
	(SEQ ID NO: 73)	(SEQ ID NO: 2201)
304	SNCG	TATTGGTGTTAATAGGAG
	(SEQ ID NO: 73)	(SEQ ID NO: 2202)
305	SNCG	ATTGTACGTAGGGTTG
	(SEQ ID NO: 73)	(SEQ ID NO:2203)
306	SNCG	TTTTATTGTATGTAGGGT
	(SEQ ID NO: 73)	(SEQ ID NO: 2204)
307	GPC3	AATAGTCGCGTTTAGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1760)
308	GPC3	TAGTTGTGTTTAGGGAT
	(SEQ ID NO: 118)	(SEQ ID NO: 1761)
309	GPC3	TTTAACGTAGTTTTGATCGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1762)
310	GPC3	TTTAATGTAGTTTTGATTGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1763)
311	GPC3	TTTAACGTAGTTTTGATCGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1762)
312	GPC3	TTTAATGTAGTTTTGATTGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1763)
313	CLDN7	TTACGTTAAGTCGGGT
	(SEQ ID NO: 87)	(SEQ ID NO: 1764)
314	CLDN7	AGTTATGTTAAGTTGGG
	(SEQ ID NO: 87)	(SEQ ID NO: 1765)
315	CLDN7	TAGCGTTTTAGGCGTA
	(SEQ ID NO: 87)	(SEQ ID NO: 1766)
316	CLDN7	TAGTGTTTTAGGTGTATT
	(SEQ ID NO: 87)	(SEQ ID NO: 1767)
317	CLDN7	TTAGGGGCGTTTCGTA
	(SEQ ID NO: 87)	(SEQ ID NO: 1768)
318	CLDN7	TTAGGGGTGTTTTGTAG
	(SEQ ID NO: 87)	(SEQ ID NO: 1769)
319	CLDN7	TAGAATTCGGCGGGGA
	(SEQ ID NO: 87)	(SEQ ID NO: 1770)
320	CLDN7	TAGAATTTGGTGGGGA
	(SEQ ID NO: 87)	(SEQ ID NO: 1771)
321	CLDN7	TAGAATTCGGCGGGGA
	(SEQ ID NO: 87)	(SEQ ID NO: 1770)
322	CLDN7	TAGAATTTGGTGGGGA
	(SEQ ID NO: 87)	(SEQ ID NO: 1771)
323	SLIT2	TTCGATAGTTAACGATG
	(SEQ ID NO: 112)	(SEQ ID NO: 1772)
324	SLIT2	TTTGATAGTTAATGATGGT
	(SEQ ID NO: 112)	(SEQ ID NO: 1773)
325	SLIT2	ATTTCGTCGTAGTTTG
	(SEQ ID NO: 112)	(SEQ ID NO: 1774)
326	SLIT2	TTTTGTTGTAGTTTGGA
	(SEQ ID NO: 112)	(SEQ ID NO: 1775)
327	SLIT2	TAGCGGGTTCGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1776)
328	SLIT2	TTAGTGGGTTTGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1777)
329	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1778)
330	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1779)
331	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1778)
332	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1779)
333	IGSF4	TAGTCGTAGAGTCGGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1782)
334	IGSF4	GTTGTAGAGTTGGGTT
	(SEQ ID NO: 74)	(SEQ ID NO: 1783)
335	IGSF4	TAGGTTTTCGGATTGA
	(SEQ ID NO: 74)	(SEQ ID NO: 1784)
336	IGSF4	GTAGGTTTTTGGATTGA
	(SEQ ID NO: 74)	(SEQ ID NO: 1785)
337	MCT1	ATTTTACGTAGGCGTT
	(SEQ ID NO: 101)	(SEQ ID NO: 1786)
338	MCT1	GATTTTATGTAGGTGTTT
	(SEQ ID NO: 101)	(SEQ ID NO: 1787)
339	MCT1	AGTTAGTCGCGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1788)
340	MCT1	AGAGTTAGTTGTGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1789)
341	SEQ ID NO: 6	AAGTTTATCGGCGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1792)
342	SEQ ID NO: 6	AGAAGTTTATTGGTGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1793)
343	SEQ ID NO: 6	ATTTCGGAATTTAAGCGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1794)
344	SEQ ID NO: 6	TTTTGGAATTTAAGTGTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1795)
345	SEQ ID NO: 6	TAATTTCGGACGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1796)
346	SEQ ID NO: 6	TTTTGGATGTGGAGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1797)
347	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1798)
348	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1799)
349	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1798)
350	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1799)
351	SEQ ID NO: 6	TTTCGGTTTTCGTTAAT
	(SEQ ID NO: 6)	(SEQ ID NO: 1800)
352	SEQ ID NO: 6	TTTGGTTTTTGTTAATTTAG
	(SEQ ID NO: 6)	(SEQ ID NO: 1801)
353	SEQ ID NO: 6	TGTGCGAAGTTAACGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1802)
354	SEQ ID NO: 6	TTGTGTGAAGTTAATGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1803)
355	SEQ ID NO: 8	ATAGGGCGGGATTTTA
	(SEQ ID NO: 8)	(SEQ ID NO: 2153)
356	SEQ ID NO: 8	GATAGGGTGGGATTTT
	(SEQ ID NO: 8)	(SEQ ID NO: 2154)
357	SEQ ID NO: 8	ATAAAGCGGGGTTTTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1804)
358	SEQ ID NO: 8	GGATAAAGTGGGGTTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1805)
359	SEQ ID NO: 8	AGGAGGCGAGAAATTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1806)
360	SEQ ID NO: 8	GAGGAGGTGAGAAATT
	(SEQ ID NO: 8)	(SEQ ID NO: 1807)
361	SEQ ID NO: 8	AGAAATTTCGGGGTAG
	(SEQ ID NO: 8)	(SEQ ID NO: 1808)
362	SEQ ID NO: 8	GAAATTTTGGGGTAGTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1809)
363	SEQ ID NO: 8	GGTAGTATCGTTTATAGA
	(SEQ ID NO: 8)	(SEQ ID NO: 1810)
364	SEQ ID NO: 8	GGGGTAGTATTGTTTATA
	(SEQ ID NO: 8)	(SEQ ID NO: 1811)
365	PROSTAGLANDIN E2	AGTGTATCGTTTTTCGG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1812)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
366	PROSTAGLANDIN E2	TAGTGTATTGTTTTTTGG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1813)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
367	PROSTAGLANDIN E2	TGCGTATCGTTAGTTA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1814)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
368	PROSTAGLANDIN E2	AGGTTGTGTATTGTTAG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1815)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
369	PROSTAGLANDIN E2	ATTATTTCGGCGGTGA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1816)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
370	PROSTAGLANDIN E2	GATTATTTTGGTGGTGA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1817)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
371	PROSTAGLANDIN E2	TAAGTCGCGTAAGGAG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1818)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
372	PROSTAGLANDIN E2
	RECEPTOR, EP4 SUBTYPE
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
373	PROSTAGLANDIN E2	GTATCGCGAGTTTGGA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1820)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
374	PROSTAGLANDIN E2	GTATTGTGAGTTTGGAG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1821)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
375	SEQ ID NO: 51	GTCGGGGTCGATTCGA
	(SEQ ID NO: 51)	(SEQ ID NO: 1822)
376	SEQ ID NO: 51	GTTGGGGTTGATTTGAT
	(SEQ ID NO: 51)	(SEQ ID NO: 1823)
377	SEQ ID NO: 51	AGGATTCGTTTGCGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1824)
378	SEQ ID NO: 51	AAGGATTTGTTTGTGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1825)
379	MGC34831	ATTAGCGTTTGGCGTT
	(SEQ ID NO: 52)	(SEQ ID NO: 1826)
380	MGC34831	AATTAGTGTTTGGTGTT
	(SEQ ID NO: 52)	(SEQ ID NO: 1827)
381	MGC34831	GTTTAGCGACGGTCGT
	(SEQ ID NO: 52)	(SEQ ID NO: 1828)
382	MGC34831	TGTTTAGTGATGGTTGT
	(SEQ ID NO: 52)	(SEQ ID NO: 1829)
383	SEQ ID NO: 54	TGTGTAGCGGCGATTA
	(SEQ ID NO: 54)	(SEQ ID NO: 1830)
384	SEQ ID NO: 54	GTGTGTAGTGGTGATT
	(SEQ ID NO: 54)	(SEQ ID NO: 1831)
385	SEQ ID NO: 54	ATTAGCGTTTGGTCGG
	(SEQ ID NO: 54)	(SEQ ID NO: 1832)
386	SEQ ID NO: 54	ATTAGTGTTTGGTTGGG
	(SEQ ID NO: 54)	(SEQ ID NO: 1833)
387	PDLIM1	TAGGTCGCGTAGTCGT
	(SEQ ID NO: 55)	(SEQ ID NO: 1834)
388	PDLIM1	TTAGGTTGTGTAGTTGT
	(SEQ ID NO: 55)	(SEQ ID NO: 1835)
389	SEQ ID NO: 15	AATCGTGCGGTTGATA
	(SEQ ID NO: 15)	(SEQ ID NO: 1836)
390	SEQ ID NO: 15	TGTAGAATTGTGTGGT
	(SEQ ID NO: 15)	(SEQ ID NO: 1837)
391	SEQ ID NO: 15	TTGCGTAGAAAATTCGAG
	(SEQ ID NO: 15)	(SEQ ID NO: 1838)
392	SEQ ID NO: 15	TTGTGTAGAAAATTTGAG
	(SEQ ID NO: 15)	(SEQ ID NO: 1839)
393	SEQ ID NO: 15	TTGCGTAGAAAATTCGAG
	(SEQ ID NO: 15)	(SEQ ID NO: 1838)
394	SEQ ID NO: 15	TTGTGTAGAAAATTTGAG
	(SEQ ID NO: 15)	(SEQ ID NO: 1839)
395	SEQ ID NO: 15	AAAATTCGAGGTCGGG
	(SEQ ID NO: 15)	(SEQ ID NO: 1840)
396	SEQ ID NO: 15	AAAATTTGAGGTTGGG
	(SEQ ID NO: 15)	(SEQ ID NO: 1841)
397	SEQ ID NO: 15	AAAATTCGAGGTCGGG
	(SEQ ID NO: 15)	(SEQ ID NO: 1840)
398	SEQ ID NO: 15	AAAATTTGAGGTTGGG
	(SEQ ID NO: 15)	(SEQ ID NO: 1841)
399	SEQ ID NO: 15	AATAGGCGATGTACGG
	(SEQ ID NO: 15)	(SEQ ID NO: 2205)
400	SEQ ID NO: 15	TAGGTGATGTATGGGT
	(SEQ ID NO: 15)	(SEQ ID NO: 2206)
401	SEQ ID NO: 15	TAATCGAGTTTAGCGG
	(SEQ ID NO: 15)	(SEQ ID NO: 2207)
402	SEQ ID NO: 15	TTAATTGAGTTTAGTGGT
	(SEQ ID NO: 15)	(SEQ ID NO: 2208)
403	DKK3	ATTCGTTTTAGTTCGAG
	(SEQ ID NO: 24)	(SEQ ID NO: 1842)
404	DKK3	ATTTGTTTTAGTTTGAGT
	(SEQ ID NO: 24)	(SEQ ID NO: 1843)
405	DKK3	TTCGATCGTTTTAGGA
	(SEQ ID NO: 24)	(SEQ ID NO: 1844)
406	DKK3	AGTTTTGATTGTTTTAGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1845)
407	DKK3	GAAAAGACGCGATTTT
	(SEQ ID NO: 24)	(SEQ ID NO: 1848)
408	DKK3	GAAAAGATGTGATTTTATT
	(SEQ ID NO: 24)	(SEQ ID NO: 1849)
409	SEQ ID NO: 28	TATCGACGTTTTTGGT
	(SEQ ID NO: 28)	(SEQ ID NO: 1850)
410	SEQ ID NO: 28	TATTGATGTTTTTGGTTT
	(SEQ ID NO: 28)	(SEQ ID NO: 1851)
411	SEQ ID NO: 29	TTGATGCGGAGTTCGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1852)
412	SEQ ID NO: 29	TTGATGTGGAGTTTGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1853)
413	SEQ ID NO: 29	TTGATGCGGAGTTCGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1852)
414	SEQ ID NO: 29	TTGATGTGGAGTTTGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1853)
415	SEQ ID NO: 29	TTCGAAGCGTGTATTA
	(SEQ ID NO: 29)	(SEQ ID NO: 2155)
416	SEQ ID NO: 29	GGGTTTGAAGTGTGTA
	(SEQ ID NO: 29)	(SEQ ID NO: 2156)
417	SEQ ID NO: 29	TAGGAACGGTAGGCGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1854)
418	SEQ ID NO: 29	TAGGAATGGTAGGTGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1855)
419	SEQ ID NO: 29	TAGGAACGGTAGGCGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1854)
420	SEQ ID NO: 29	TAGGAATGGTAGGTGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1855)
421	SEQ ID NO: 29	GTCGGAGGCGTTTGAG
	(SEQ ID NO: 29)	(SEQ ID NO: 1856)
422	SEQ ID NO: 29	GTTGGAGGTGTTTGAGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1857)
423	ARL7	TAGATTTCGTAGTTTTTTA
	(SEQ ID NO: 30)	(SEQ ID NO: 1858)
424	ARL7	TAGATTTTGTAGTTTTTTAA
	(SEQ ID NO: 30)	(SEQ ID NO: 1859)
425	ARL7	TGGGTACGTTTACGGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1860)
426	ARL7	TGGGTATGTTTATGGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1861)
427	ARL7	GAAGAAATCGTTTTTGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1862)
428	ARL7	GAAGAAATTGTTTTTGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1863)
429	ARL7	TAGTAGGATCGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1864)
430	ARL7	ATAGTAGGATTGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1865)
431	SEQ ID NO: 31	AACGTTGCGTTGGGTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1866)
432	SEQ ID NO: 31	AATGTTGTGTTGGGTAA
	(SEQ ID NO: 31)	(SEQ ID NO: 1867)
433	SEQ ID NO: 31	TAGCGTTTCGTGGTTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1868)
434	SEQ ID NO: 31	GTAGTGTTTTGTGGTTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1869)
435	THH	GTTCGTTGGCGTAAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1872)
436	THH	GGTTTGTTGGTGTAAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1873)
437	(SEQ ID NO: 36)	TTATTTGCGTTTCGAA
		(SEQ ID NO: 2209)
438	(SEQ ID NO: 36)	AATTATTTGTGTTTTGAAT
		(SEQ ID NO: 2210)
439	(SEQ ID NO: 36)	GGACGTTGCGATTGTA
		(SEQ ID NO: 2161)
440	(SEQ ID NO: 36)	GATGTTGTGATTGTAGT
		(SEQ ID NO: 2162)
441	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1878)
442	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1879)
443	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1878)
444	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1879)
445	SENP3	AGGACGTTTTTGATCGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1880)
446	SENP3	AGGATGTTTTTGATTGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1881)
447	SENP3	AGGACGTTTTTGATCGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1880)
448	SENP3	AGGATGTTTTTGATTGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1881)
449	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1882)
450	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1883)
451	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1882)
452	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1883)
453	SEQ ID NO: 42	GAGTCGGGTTGCGATG
	(SEQ ID NO: 42)	(SEQ ID NO: 1884)
454	SEQ ID NO: 42	GGAGTTGGGTTGTGAT
	(SEQ ID NO: 42)	(SEQ ID NO: 1885)
455	(SEQ ID NO: 117)	TAGCGGTTTTTTAGCGTA
		(SEQ ID NO: 1888)
456	(SEQ ID NO: 117)	AGTGGTTTTTTAGTGTAT
		(SEQ ID NO: 1889)
457	(SEQ ID NO: 117)	AGATGCGCGGGTAGAT
		(SEQ ID NO: 1890)
458	(SEQ ID NO: 117)	AGATGTGTGGGTAGAT
		(SEQ ID NO: 1891)
459	(SEQ ID NO: 117)	AGATGCGCGGGTAGAT
		(SEQ ID NO: 1890)
460	(SEQ ID NO: 117)	AGATGTGTGGGTAGAT
		(SEQ ID NO: 1891)
461	(SEQ ID NO: 117)	AGATAGTTCGTATTCGT
		(SEQ ID NO: 1892)
462	(SEQ ID NO: 117)	GTAGATAGTTTGTATTTGT
		(SEQ ID NO: 1893)
463	(SEQ ID NO: 117)	TTTGTTCGTAACGTTT
		(SEQ ID NO: 1894)
464	(SEQ ID NO: 117)	TGTTTGTAATGTTTAGAG
		(SEQ ID NO: 1895)
465	O60279	AGTAAACGAATAAGAAGT
	(SEQ ID NO: 47)	(SEQ ID NO: 1896)
466	O60279	AAGTAAATGAATAAGAAGT
	(SEQ ID NO: 47)	(SEQ ID NO: 1897)
467	O60279	TACGTTTTTTCGGATTA
	(SEQ ID NO: 47)	(SEQ ID NO: 1898)
468	O60279	TATGTTTTTTTGGATTAAG
	(SEQ ID NO: 47)	(SEQ ID NO: 1899)
469	O60279	TAATTATCGGCGGTGT
	(SEQ ID NO: 47)	(SEQ ID NO: 1900)
470	O60279	ATTATTGGTGGTGTTTT
	(SEQ ID NO: 47)	(SEQ ID NO: 1901)
471	O60279	GGACGGCGGAAAATTA
	(SEQ ID NO: 47)	(SEQ ID NO: 1902)
472	O60279	AGGGATGGTGGAAAAT
	(SEQ ID NO: 47)	(SEQ ID NO: 1903)
473	SEQ ID NO: 48	TATTTGGCGATTCGGA
	(SEQ ID NO: 48)	(SEQ ID NO: 1904)
474	SEQ ID NO: 48	TGGTGATTTGGAGATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1905)
475	SEQ ID NO: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1906)
476	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1907)
477	SEQ ID NO: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1906)
478	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1907)
479	SEQ ID NO: 48	AACGAATTTTTCGATATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1908)
480	SEQ ID NO: 48	TTTAATGAATTTTTTGATATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1909)
481	SEQ ID NO: 48	AAAATCGTATGCGTGT
	(SEQ ID NO: 48)	(SEQ ID NO: 1910)
482	SEQ ID NO: 48	GAAAATTGTATGTGTGTG
	(SEQ ID NO: 48)	(SEQ ID NO: 1911)
483	SEQ ID NO: 9	GTTTCGCGTTTAGGGA
	(SEQ ID NO: 9)	(SEQ ID NO: 1912)
484	SEQ ID NO: 9	GTTTTGTGTTTAGGGAT
	(SEQ ID NO: 9)	(SEQ ID NO: 1913)
485	SEQ ID NO: 9	AGTGTTCGTCGTAGTT
	(SEQ ID NO: 9)	(SEQ ID NO: 1914)
486	SEQ ID NO: 9	TGAGTGTTTGTTGTAGT
	(SEQ ID NO: 9)	(SEQ ID NO: 1915)
487	SEQ ID NO: 9	TTTTGTTCGCGTTGAA
	(SEQ ID NO: 9)	(SEQ ID NO: 1916)
488	SEQ ID NO: 9	TTGTTTGTGTTGAAGTA
	(SEQ ID NO: 9)	(SEQ ID NO: 1917)
489	SEQ ID NO: 9	GGGTCGCGAGGTAGTT
	(SEQ ID NO: 9)	(SEQ ID NO: 1918)
490	SEQ ID NO: 9	TGGGTTGTGAGGTAGT
	(SEQ ID NO: 9)	(SEQ ID NO: 1919)
491	SEQ ID NO: 9	TTTGTGCGACGTTATT
	(SEQ ID NO: 9)	(SEQ ID NO: 1920)
492	SEQ ID NO: 9	GGTTTGTGTGATGTTAT
	(SEQ ID NO: 9)	(SEQ ID NO: 1921)
493	SEQ ID NO: 9	ATGGCGGTTTCGATTT
	(SEQ ID NO: 9)	(SEQ ID NO: 1922)
494	SEQ ID NO: 9	GATGGTGGTTTTGATTT
	(SEQ ID NO: 9)	(SEQ ID NO: 2923)
495	SEQ ID NO: 5	AATGAGCGAGAAAGTA
	(SEQ ID NO: 5)	(SEQ ID NO: 1924)
496	SEQ ID NO: 5	AGAATGAGTGAGAAAGT
	(SEQ ID NO: 5)	(SEQ ID NO: 1925)
497	SEQ ID NO: 5	ATTAAACGGGATGGTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1926)
498	SEQ ID NO: 5	AATATTAAATGGGATGGT
	(SEQ ID NO: 5)	(SEQ ID NO: 1927)
499	SEQ ID NO: 5	GAGTTGCGAGGATTTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1928)
500	SEQ ID NO: 5	GGAGTTGTGAGGATTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1929)
501	SEQ ID NO: 5	GGGAATCGTTGATTTT
	(SEQ ID NO: 5)	(SEQ ID NO: 1930)
502	SEQ ID NO: 5	AGGGGAATTGTTGATT
	(SEQ ID NO: 5)	(SEQ ID NO: 1931)
503	SEQ ID NO: 7	TAGTCGTCGTGTAGGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1932)
504	SEQ ID NO: 7	TAGGTAGTTGTTGTGTA
	(SEQ ID NO: 7)	(SEQ ID NO: 1933)
505	SEQ ID NO: 7	TATAGGTACGCGATGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1934)
506	SEQ ID NO: 7	AGGTATGTGATGAGGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1935)
507	SEQ ID NO: 7	ATGATTTGCGTTACGT
	(SEQ ID NO: 7)	(SEQ ID NO: 1938)
508	SEQ ID NO: 7	ATGATTTGTGTTATGTTT
	(SEQ ID NO: 7)	(SEQ ID NO: 1939)
509	SEQ ID NO: 7	TAACGTTGTGGTTCGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1940)
510	SEQ ID NO: 7	TAATGTTGTGGTTTGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1941)
511	SEQ ID NO: 7	TAACGTTGTGGTTCGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1940)
512	SEQ ID NO: 7	TAATGTTGTGGTTTGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1941)
513	SEQ ID NO: 1	GGTCGGCGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1942)
514	SEQ ID NO: 1	GGTTGGTGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1943)
515	SEQ ID NO: 1	GGTCGGCGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1942)
516	SEQ ID NO: 1	GGTTGGTGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1943)
517	SEQ ID NO: 1	GATTCGAACGGATTTT
	(SEQ ID NO: 1)	(SEQ ID NO: 1944)
518	SEQ ID NO: 1	GGGATTTGAATGGATTT
	(SEQ ID NO: 1)	(SEQ ID NO: 1945)
519	SEQ ID NO: 1	TGGGTCGGGATTCGAA
	(SEQ ID NO: 1)	(SEQ ID NO: 1946)
520	SEQ ID NO: 1	TGGGTTGGGATTTGAA
	(SEQ ID NO: 1)	(SEQ ID NO: 1947)
521	SEQ ID NO: 1	TGGGTCGGGATTCGAA
	(SEQ ID NO: 1)	(SEQ ID NO: 1946)
522	SEQ ID NO: 1	TGGGTTGGGATTTGAA
	(SEQ ID NO: 1)	(SEQ ID NO: 1947)
523	SEQ ID NO: 1	GTCGGAAGTTTCGGGA
	(SEQ ID NO: 1)	(SEQ ID NO: 1948)
524	SEQ ID NO: 1	GTTGGAAGTTTTGGGAT
	(SEQ ID NO: 1)	(SEQ ID NO: 1949)
525	SEQ ID NO: 1	TGGATATCGTAGGGTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1950)
526	SEQ ID NO: 1	TGGATATTGTAGGGTAG
	(SEQ ID NO: 1)	(SEQ ID NO: 1951)
527	PROSTAGLANDIN E2	AGGTAATCGAGGCGGT
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1952)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
528	PROSTAGLANDIN E2	AGGTAATTGAGGTGGT
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1953)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
529	PROSTAGLANDIN E2	AGGTAATCGAGGCGGT
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1952)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
530	PROSTAGLANDIN E2	AGGTAATTGAGGTGGT
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1953)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
531	PROSTAGLANDIN E2	GGCGTCGAAAGTCGTT
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1954)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
532	PROSTAGLANDIN E2	GGTGTTGAAAGTTGTTG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1955)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
533	PROSTAGLANDIN E2	TAATCGTTTGTTTACGT
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1956)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
534	PROSTAGLANDIN E2	AATTGTTTGTTTATGTAGT
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1957
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
535	ORPHAN NUCLEAR	TTACGGAGGCGTTTTA
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1958)
	1-FETOPROTEIN TRANS-
	SCRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR) (B1-
	BINDING FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
536	ORPHAN NUCLEAR	TTTTATGGAGGTGTTTT
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1959)
	1-FETOPROTEIN TRANS-
	SCRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR) (B1-
	BINDING FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
537	ORPHAN NUCLEAR	AGGCGAATTTATCGGG
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1960)
	1-FETOPROTEIN TRANS-
	SCRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR) (B1-
	BINDING FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
538	ORPHAN NUCLEAR	GGTGAATTTATTGGGG
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1961)
	1-FETOPROTEIN TRANS-
	SCRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR) (B1-
	BINDING FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
539	ORPHAN NUCLEAR	TAGTCGAAGTAGGCGT
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1962)
	1-FETOPROTEIN TRANS-
	SCRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR) (B1-
	BINDING FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
540	ORPHAN NUCLEAR	TAGTTGAAGTAGGTGTT
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1963)
	1-FETOPROTEIN TRANS-
	SCRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR) (B1-
	BINDING FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
541	ORPHAN NUCLEAR	TTTTCGACGAAGTTTT
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1964)
	1-FETOPROTEIN TRANS-
	SCRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR) (B1-
	BINDING FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
542	ORPHAN NUCLEAR	TTTTGATGAAGTTTTGTT
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1965)
	1-FETOPROTEIN TRANS-
	SCRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR) (B1-
	BINDING FACTOR) (HB1F)
	(CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
543	LIM DOMAIN KINASE 1	TGTAGTCGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1966)
	(SEQ ID NO: 12)
544	LIM DOMAIN KINASE 1	TGTAGTTGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1967)
	(SEQ ID NO: 12)
545	LIM DOMAIN KINASE 1	TGTAGTCGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1966)
	(SEQ ID NO: 12)
546	LIM DOMAIN KINASE 1	TGTAGTTGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1967)
	(SEQ ID NO: 12)
547	LIM DOMAIN KINASE 1	GGATTATCGCGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1968)
	(SEQ ID NO: 12)
548	LIM DOMAIN KINASE 1	GGATTATTGTGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1969)
	(SEQ ID NO: 12)
549	LIM DOMAIN KINASE 1	GGATTATCGCGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1968)
	(SEQ ID NO: 12)
550	LIM DOMAIN KINASE 1	GGATTATTGTGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1969)
	(SEQ ID NO: 12)
551	LIM DOMAIN KINASE 1	GTCGGTAGTTTATCGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1970)
	(SEQ ID NO: 12)
552	LIM DOMAIN KINASE 1	GTTGGTAGTTTATTGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1971)
	(SEQ ID NO: 12)
553	LIM DOMAIN KINASE 1	GTCGGTAGTTTATCGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1970)
	(SEQ ID NO: 12)
554	LIM DOMAIN KINASE 1	GTTGGTAGTTTATTGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1971)
	(SEQ ID NO: 12)
555	LIM DOMAIN KINASE 1	TAGGAGACGTTACGTT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1972)
	(SEQ ID NO: 12)
556	LIM DOMAIN KINASE 1	AGATGTTATGTTAGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1973)
	(SEQ ID NO: 12)
557	BCL11B	AAGTCGTCGGAGTTAG
	(SEQ ID NO: 50)	(SEQ ID NO: 1976)
558	BCL11B	GTGAAGTTGTTGGAGT
	(SEQ ID NO: 50)	(SEQ ID NO: 1977)
559	BCL11B	TTGAGGCGTTACGGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1978)
560	BCL11B	TTGAGGTGTTATGGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1979)
561	BCL11B	TTGAGGCGTTACGGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1978)
562	BCL11B	TTGAGGTGTTATGGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1979)
563	MSF	GTTTCGAAATTGGCGT
	(SEQ ID NO: 13)	(SEQ ID NO: 1980)
564	MSF	TTTGAAATTGGTGTGG
	(SEQ ID NO: 13)	(SEQ ID NO: 1981)
565	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1982)
566	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1983)
567	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1982)
568	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1983)
569	MSF	TTACGGTTCGATTTTG
	(SEQ ID NO: 13)	(SEQ ID NO: 1984)
570	MSF	TATGGTTTGATTTTGGG
	(SEQ ID NO: 13)	(SEQ ID NO: 1985)
571	SEQ ID NO: 14	TAAGGCGTTTTCGATA
	(SEQ ID NO: 14)	(SEQ ID NO: 1986)
572	SEQ ID NO: 14	GTAAGGTGTTTTTGATAT
	(SEQ ID NO: 14)	(SEQ ID NO: 1987)
573	SEQ ID NO: 16	ATCGTTGGTCGGATTT
	(SEQ ID NO: 16)	(SEQ ID NO: 1990)
574	SEQ ID NO: 16	TAGGATTGTTGGTTGGA
	(SEQ ID NO: 16)	(SEQ ID NO: 1991)
575	SEQ ID NO: 16	AGGAGTTTTCGTGTCGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1992)
576	SEQ ID NO: 16	AGGAGTTTTTGTGTTGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1993)
577	SEQ ID NO: 16	AGGAGTTTTCGTGTCGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1992)
578	SEQ ID NO: 16	AGGAGTTTTTGTGTTGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1993)
579	SEQ ID NO: 16	TTACGGATAGGGCGAT
	(SEQ ID NO: 16)	(SEQ ID NO: 1994)
580	SEQ ID NO: 16	TATGGATAGGGTGATTT
	(SEQ ID NO: 16)	(SEQ ID NO: 1995)
581	SEQ ID NO: 16	AGGCGTTGTCGGTGAT
	(SEQ ID NO: 16)	(SEQ ID NO: 1996)
582	SEQ ID NO: 16	AGGTGTTGTTGGTGATA
	(SEQ ID NO: 16)	(SEQ ID NO: 1997)
583	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1998)
584	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1999)
585	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1998)
586	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1999)
587	SEQ ID NO: 17	ATTTAGTCGTGCGTTT
	(SEQ ID NO: 17)	(SEQ ID NO: 2000)
588	SEQ ID NO: 17	TGATTTAGTTGTGTGTT
	(SEQ ID NO: 17)	(SEQ ID NO: 2001)
589	SEQ ID NO: 18	TTTACGCGGGGTTTTA
	(SEQ ID NO: 18)	(SEQ ID NO: 2002)
590	SEQ ID NO: 18	TTTATGTGGGGTTTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2003)
591	SEQ ID NO: 18	TTACGTCGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2004)
592	SEQ ID NO: 18	TTTTATGTTGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2005)
593	SEQ ID NO: 18	TATTTGGACGTCGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2006)
594	SEQ ID NO: 18	TATTTGGATGTTGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2007)
595	SEQ ID NO: 18	TATTTGGACGTCGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2006)
596	SEQ ID NO: 18	TATTTGGATGTTGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2007)
597	SEQ ID NO: 18	GAGGCGTATTAGGTCGG
	(SEQ ID NO: 18)	(SEQ ID NO: 2008)
598	SEQ ID NO: 18	AGGTGTATTAGGTTGGG
	(SEQ ID NO: 18)	(SEQ ID NO: 2009)
599	SEQ ID NO: 18	AAAGCGGAGTCGTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2010)
600	SEQ ID NO: 18	AGTGGAGTTGTTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2011)
601	SEQ ID NO: 19	AGGTTTTCGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2012)
602	SEQ ID NO: 19	TAGGTTTTTGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2013)
603	SEQ ID NO: 19	TGAGATTCGTTTTTTAAA
	(SEQ ID NO: 19)	(SEQ ID NO: 2014)
604	SEQ ID NO: 19	GGTGAGATTTGTTTTTTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2015)
605	PRDM6	AGTTTTAAGCGTTTGGT
	(SEQ ID NO: 20)	(SEQ ID NO: 2016)
606	PRDM6	AGTTTTAAGTGTTTGGT
	(SEQ ID NO: 20)	(SEQ ID NO: 2017)
607	PRDM6	AGTTTTAAGCGTTTGGT
	(SEQ ID NO: 20)	(SEQ ID NO: 2016)
608	PRDM6	AGTTTTAAGTGTTTGGT
	(SEQ ID NO: 20)	(SEQ ID NO: 2017)
609	PRDM6	GAAGTTCGGATTTCGG
	(SEQ ID NO: 20)	(SEQ ID NO: 2018)
610	PRDM6	GGAAGTTTGGATTTTGG
	(SEQ ID NO: 20)	(SEQ ID NO: 2019)
611	PRDM6	TTGTCGGGTTACGGGA
	(SEQ ID NO: 20)	(SEQ ID NO: 2020)
612	PRDM6	GTTGGGTTATGGGAGA
	(SEQ ID NO: 20)	(SEQ ID NO: 2021)
613	PRDM6	TTCGTAGAATTGTCGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2022)
614	PRDM6	TTTGTAGAATTGTTGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2023)
615	PRDM6	TTCGTAGAATTGTCGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2022)
616	PRDM6	TTTGTAGAATTGTTGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2023)
617	RAP2B	GGTCGGGTAATCGTTA
	(SEQ ID NO: 21)	(SEQ ID NO: 2024)
618	RAP2B	GTTGGGTAATTGTTAGA
	(SEQ ID NO: 21)	(SEQ ID NO: 2025)
619	NR2E1	AATGTAGCGGCGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2028)
620	NR2E1	TAAATGTAGTGGTGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2029)
621	NR2E1	GTCGTTATCGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2030)
622	NR2E1	GTTGTTATTGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2031)
623	NR2E1	GTCGTTATCGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2030)
624	NR2E1	GTTGTTATTGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2031)
625	NR2E1	GACGTAAGTTTCGGGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2032)
626	NR2E1	GGATGTAAGTTTTGGG
	(SEQ ID NO: 22)	(SEQ ID NO: 2033)
627	NR2E1	TTTTTAGTCGCGAGAA
	(SEQ ID NO: 22)	(SEQ ID NO: 2034)
628	NR2E1	TTTTTAGTTGTGAGAAGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2035)
629	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2036)
630	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2037)
631	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2036)
632	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2037)
633	NR2E1	AGGCGAGTCGGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2038)
634	NR2E1	AGGTGAGTTGGAGTTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2039)
635	NR2E1	TAAGTCGAGCGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2040)
636	NR2E1	TAGTAAGTTGAGTGAGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2041)
637	NR2E1	AGGGACGCGAAAATTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2042)
638	NR2E1	GGAGGGATGTGAAAAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2043)
639	PCDH7	ATCGTAGTCGGTTTTA
	(SEQ ID NO: 23)	(SEQ ID NO: 2044)
640	PCDH7	GATTATTGTAGTTGGTTT
	(SEQ ID NO: 23)	(SEQ ID NO: 2045)
641	RTTN	TAGTGGCGCGGTAGTT
	(SEQ ID NO: 25)	(SEQ ID NO: 2046)
642	RTTN	TAGTGGTGTGGTAGTTT
	(SEQ ID NO: 25)	(SEQ ID NO: 2047)
643	RTTN	TAGGACGTGTTTTCGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2048)
644	RTTN	AGGATGTGTTTTTGGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2049)
645	SNAP25	ATACGGAATATCGTATTT
	(SEQ ID NO: 33)	(SEQ ID NO: 2052)
646	SNAP25	GTGTATATATGGAATATTGT
	(SEQ ID NO: 33)	(SEQ ID NO: 2053)
647	SEQ ID NO: 26	TTAAGTATCGAGGCGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2054)
648	SEQ ID NO: 26	TTTTAAGTATTGAGGTGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2055)
649	SEQ ID NO: 26	AATTTTGGTCGTTTAGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2056)
650	SEQ ID NO: 26	AAATTTTGGTTGTTTAGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2057)
651	SEQ ID NO: 26	TTCGTATTGACGTTAAT
	(SEQ ID NO: 26)	(SEQ ID NO: 2058)
652	SEQ ID NO: 26	TTTGTATTGATGTTAATAGA
	(SEQ ID NO: 26)	(SEQ ID NO: 2059)
653	GIRK2	AGTTGTTCGTAGGCGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2060)
654	GIRK2	AGTTGTTTGTAGGTGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2061)
655	GIRK2	AGTTGTTCGTAGGCGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2060)
656	GIRK2	AGTTGTTTGTAGGTGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2061)
657	GIRK2	TTATTTCGTTCGTAGTT
	(SEQ ID NO: 27)	(SEQ ID NO: 2062)
658	GIRK2	TTTGTTTGTAGTTAGGTA
	(SEQ ID NO: 27)	(SEQ ID NO: 2063)
659	GIRK2	TTAGTCGAAAGGCGAG
	(SEQ ID NO: 27)	(SEQ ID NO: 2064)
660	GIRK2	TAGTTGAAAGGTGAGG
	(SEQ ID NO: 27)	(SEQ ID NO: 2065)
661	SEQ ID NO: 28	ATTAGGCGAGTTTCGT
	(SEQ ID NO: 28)	(SEQ ID NO: 2066)
662	SEQ ID NO: 28	TTAGGTGAGTTTTGTTT
	(SEQ ID NO: 28)	(SEQ ID NO: 2067)
663	SEQ ID NO: 31	TTTACGTAGGGCGATT
	(SEQ ID NO: 31)	(SEQ ID NO: 2068)
664	SEQ ID NO: 31	ATTTTTATGTAGGGTGAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2069)
665	SEQ ID NO: 31	GATACGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2070)
666	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2071)
667	SEQ ID NO: 31	GATACGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2070)
668	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2071)
669	SEQ ID NO: 31	TTCGGGCGTTTTATAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2072)
670	SEQ ID NO: 31	GGTTTGGGTGTTTTATA
	(SEQ ID NO: 31)	(SEQ ID NO: 2073)
671	HOXB13	GTCGTTATTATTTCGAGG
	(SEQ ID NO: 34)	(SEQ ID NO: 2074)
672	HOXB13	GTTGTTATTATTTTGAGGA
	(SEQ ID NO: 34)	(SEQ ID NO: 2075)
673	HOXB13	TTCGTAGAATCGAAGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2211)
674	HOXB13	TAATTTGTAGAATTGAAGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2212)
675	HOXB13	TTACGATTGAGCGTAT
	(SEQ ID NO: 34)	(SEQ ID NO: 2213)
676	HOXB13	TATGATTGAGTGTATAGG
	(SEQ ID NO: 34)	(SEQ ID NO: 2214)
677	HOXB13	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2076)
678	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2077)
679	HOXB13	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2076)
680	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2077)
681	HOXB13	TTGGTCGCGTAGTAAA
	(SEQ ID NO: 34)	(SEQ ID NO: 2078)
682	HOXB13	TGGTTGTGTAGTAAAGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2079)
683	(SEQ ID NO: 35)	GGAGGTGCGAATTTAA
		(SEQ ID NO: 2080)
684	(SEQ ID NO: 35)	GGGAGGTGTGAATTTA
		(SEQ ID NO: 2081)
685	(SEQ ID NO: 35)	AAATAGTCGTTTGGGA
		(SEQ ID NO: 2082)
686	(SEQ ID NO: 35)	AAATAGTTGTTTGGGAG
		(SEQ ID NO: 2083)
687	(SEQ ID NO: 35)	AGAAAATATACGAGATTTAT
		(SEQ ID NO: 2084)
688	(SEQ ID NO: 35)	AGAAAATATATGAGATTTATT
		(SEQ ID NO: 2085)
689	(SEQ ID NO: 35)	TAAAGACGGGAAGAGA
		(SEQ ID NO: 2086)
690	(SEQ ID NO: 35)	ATAAAGATGGGAAGAGA
		(SEQ ID NO: 2087)
691	MGC10561	ATATTTAGCGTAGTTATTT
	(SEQ ID NO: 37)	(SEQ ID NO: 2171)
692	MGC10561	TAGTATATTTAGTGTAGTTAT
	(SEQ ID NO: 37)	(SEQ ID NO: 2172)
693	MGC10561	TTTTTTACGTTAAGGGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2088)
694	MGC10561	TTTTTATGTTAAGGGGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2089)
695	MGC10561	TTTGTTTTTCGAGTAGA
	(SEQ ID NO: 37)	(SEQ ID NO: 2090)
696	MGC10561	TGTTTTTTGAGTAGAGG
	(SEQ ID NO: 37)	(SEQ ID NO: 2091)
697	LMX1A	GTCGGGTTTTTCGGAA
	(SEQ ID NO: 38)	(SEQ ID NO: 2092)
698	LMX1A	GTTGGGTTTTTTGGAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2093)
699	LMX1A	GTCGAGATTTTATCGAAA
	(SEQ ID NO: 38)	(SEQ ID NO: 2094)
700	LMX1A	GTTGAGATTTTATTGAAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2095)
701	LMX1A	TTCGTTTTTAACGTGG
	(SEQ ID NO: 38)	(SEQ ID NO: 2215)
702	LMX1A	TTTGTTTTTAATGTGGTT
	(SEQ ID NO: 38)	(SEQ ID NO: 2216)
703	LMX1A	AGTATTCGGGCGGGTA
	(SEQ ID NO: 38)	(SEQ ID NO: 2096)
704	LMX1A	GTAGTATTTGGGTGGG
	(SEQ ID NO: 38)	(SEQ ID NO: 2097)
705	LMX1A	AACGAAATTACGTGTAT
	(SEQ ID NO: 38)	(SEQ ID NO: 2098)
706	LMX1A	TGAAATGAAATTATGTGTA
	(SEQ ID NO: 38)	(SEQ ID NO: 2099)
707	GS1	TGCGAGTTAGCGGTTA
	(SEQ ID NO: 40)	(SEQ ID NO: 2100)
708	GS1	TTGTGAGTTAGTGGTT
	(SEQ ID NO: 40)	(SEQ ID NO: 2101)
709	GS1	AGTTTCGAGGTTTTCGG
	(SEQ ID NO: 40)	(SEQ ID NO: 2102)
710	GS1	AAGTTTTGAGGTTTTTGG
	(SEQ ID NO: 40)	(SEQ ID NO: 2103)
711	TITF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2104)
712	TITF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2105)
713	TITF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2104)
714	TITF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2105)
715	TITF1	GGTTCGTTTAAGTTCGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2106)
716	TITF1	GGTTTGTTTAAGTTTGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2107)
717	TITF1	GGTTCGTTTAAGTTCGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2106)
718	TITF1	GGTTTGTTTAAGTTTGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2107)
719	TITF1	TTAGGTCGCGTTTGTA
	(SEQ ID NO: 41)	(SEQ ID NO: 2108)
720	TITF1	AGGTTGTGTTTGTAGA
	(SEQ ID NO: 41)	(SEQ ID NO: 2109)
721	TITF1	TATTTCGTTTTCGTAATT
	(SEQ ID NO: 41)	(SEQ ID NO: 2110)
722	TITF1	TTTGTTTTTGTAATTAGATT
	(SEQ ID NO: 41)	(SEQ ID NO: 2111)
723	DDX51	AGATTTTCGGCGAGAT
	(SEQ ID NO: 43)	(SEQ ID NO: 2112)
724	DDX51	ATTTTTGGTGAGATAGG
	(SEQ ID NO: 43)	(SEQ ID NO: 2113)
725	DDX51	TACGTGTGGTTTTCGGTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2114)
726	DDX51	TATGTGTGGTTTTTGGTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2115)
727	DDX51	TACGTGTGGTTTTCGGTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2114)
728	DDX51	TATGTGTGGTTTTTGGTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2115)
729	DDX51	AACGTGCGGGGTTTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2116)
730	DDX51	TGAATGTGTGGGGTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2117)
731	SEQ ID NO: 46	GAGTCGGGTTATCGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2120)
732	SEQ ID NO: 46	GGAGTTGGGTTATTGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2121)
733	SEQ ID NO: 46	TTACGGATGTTTCGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2122)
734	SEQ ID NO: 46	TTTATGGATGTTTTGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2123)
735	SEQ ID NO: 46	TGACGTATTTTCGGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2124)
736	SEQ ID NO: 46	GGTGATGTATTTTTGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2125)
737	SEQ ID NO: 46	ATAGTCGGAATCGTTG
	(SEQ ID NO: 46)	(SEQ ID NO: 2126)
738	SEQ ID NO: 46	TAGTTGGAATTGTTGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2127)
739	SEQ ID NO: 2	ATTGGGTTTCGCGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2128)
740	SEQ ID NO: 2	ATTGGGTTTTGTGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2129)
741	SEQ ID NO: 2	ATTGGGTTTCGCGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2128)
742	SEQ ID NO: 2	ATTGGGTTTTGTGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2129)
743	SEQ ID NO: 2	TAGTAGTCGGCGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2130)
744	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2131)
745	SEQ ID NO: 2	TAGTAGTCGGCGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2130)
746	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2131)
747	SEQ ID NO: 2	TGTCGTACGTTATGTT
	(SEQ ID NO: 2)	(SEQ ID NO: 2217)
748	SEQ ID NO: 2	GGTGTTGTATGTTATGT
	(SEQ ID NO: 2)	(SEQ ID NO: 2218)
749	SEQ ID NO: 2	TTGATTGGCGGACGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1706)
750	SEQ ID NO: 2	TTGATTGGTGGATGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1707)
751	SEQ ID NO: 2	TTGATTGGCGGACGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1706)
752	SEQ ID NO: 2	TTGATTGGTGGATGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1707)
753	SEQ ID NO: 3	TTGCGTTAATTCGGTA
	(SEQ ID NO: 3)	(SEQ ID NO: 2132)
754	SEQ ID NO: 3	AATTTGTGTTAATTTGGT
	(SEQ ID NO: 3)	(SEQ ID NO: 2133)
755	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2134)
756	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2135)
757	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2134)
758	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2135)
759	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2136)
760	SEQ ID NO: 3	GGTTGAAGAGTTGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2137)
761	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2136)
762	SEQ ID NO: 3	GGTTGAAGAGTTGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2137)
763	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2138)
764	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2139)
765	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2138)
766	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2139)

TABLE 19
DCIS vs. benign breast conditions
*No:	Gene	Oligo:
1	SCGB3A1	TAGTGTTCGACGTTGT
	(SEQ ID NO: 115)	(SEQ ID NO: 1475)
2	SCGB3A1	TAGTGTTTGATGTTGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 1476)
3	SASH1	TAGATTCGAGGTGCGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1477)
4	SASH1	TAGATTTGAGGTGTGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1478)
5	SASH1	TAGATTCGAGGTGCGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1477)
6	SASH1	TAGATTTGAGGTGTGG
	(SEQ ID NO: 102)	(SEQ ID NO: 1478)
7	SASH1	ATTCGGTATTCGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1479)
8	SASH1	ATTTGGTATTTGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1480)
9	SASH1	ATTCGGTATTCGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1479)
10	SASH1	ATTTGGTATTTGGGTAG
	(SEQ ID NO: 102)	(SEQ ID NO: 1480)
11	SASH1	AGTCGGAATCGGAGTT
	(SEQ ID NO: 102)	(SEQ ID NO: 1481)
12	SASH1	GTTGGAATTGGAGTTTA
	(SEQ ID NO: 102)	(SEQ ID NO: 1482)
13	ARH1/NOEY2	TAAAACGTTCGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1485)
14	ARH1/NOEY2	TTTAAAATGTTTGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1486)
15	ARH1/NOEY2	TGTATTCGTCGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1487)
16	ARH1/NOEY2	AATGTATTTGTTGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO; 1488)
17	ARH1/NOEY2	TTAGACGGAGTTCGGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1489)
18	ARH1/NOEY2	TAGATGGAGTTTGGAGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1490)
19	ARH1/NOEY2	TAGACGTAGGCGTATT
	(SEQ ID NO: 97)	(SEQ ID NO: 1491)
20	ARH1/NOEY2	GGGTAGATGTAGGTGT
	(SEQ ID NO: 97)	(SEQ ID NO: 1492)
21	CCND2	TTAGGGTCGATCGTGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1493)
22	CCND2	TAGGGTTGATTGTGTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1494)
23	CCND2	TTATCGTAGTCGGTTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1495)
24	CCND2	GATTTTATTGTAGTTGGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1496)
25	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1497)
26	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1498)
27	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1497)
28	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1498)
29	CDKN1A	ATTAGGGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1501)
30	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1502)
31	CDKN1A	ATTAGUGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1501)
32	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1502)
33	CDKN2A	GGCGTTGTTTAACGTAT
	(SEQ ID NO: 57)	(SEQ ID NO: 1503)
34	CDKN2A	GGGTGTTGTTTAATGTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1504)
35	CDKN2A	AATAGTTACGGTCGGA
	(SEQ ID NO: 57)	(SEQ ID NO: 1505)
36	CDKN2A	AGTTATGGTTGGAGGT
	(SEQ ID NO: 57)	(SEQ ID NO: 1506)
37	CDKN2A	GTCGGAGGTCGATTTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1507)
38	CDKN2A	GGTTGGAGGTTGATTTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1508)
39	EYA4	GGTATAAAATCGTAAATTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1513)
40	EYA4	GGGIATAAAATTGTAAATTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1514)
41	EYA4	GTTTAGATACGAAATGTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1517)
42	EYA4	GTTTAGATATGAAATGTTAT
	(SEQ ID NO: 58)	(SEQ ID NO: 1518)
43	FHIT	TTTAAGTATCGATTTTAGT
	(SEQ ID NO: 76)	(SEQ ID NO: 2183)
44	FHIT	TAAGTATTGATTTTAGTTTTA
	(SEQ ID NO: 76)	(SEQ ID NO: 2184)
45	FHIT	GTTACGTTAGCGGGTT
	(SEQ ID NO: 76)	(SEQ ID NO: 1521)
46	FHIT	GGTTATGTTAGTGGGT
	(SEQ ID NO: 76)	(SEQ ID NO: 1522)
47	FHIT	TTCGGGGACGTTATAG
	(SEQ ID NO: 76)	(SEQ ID NO: 1523)
48	FHIT	GGTTTGGGGATGTTAT
	(SEQ ID NO: 76)	(SEQ ID NO: 1524)
49	GSTP1	GGCGATTTCGGGGATT
	(SEQ ID NO: 59)	(SEQ ID NO: 1525)
50	GSTP1	GGTGATTTTGGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1526)
51	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1527)
52	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1528)
53	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1527)
54	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1528)
55	GSTP1	AGTTCGCGGGATTTTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1529)
56	GSTP1	GGAGTTTGTGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1530)
57	GSTP1	AGTTTTCGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1531)
58	GSTP1	TAGTTTTTGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1532)
59	HIC1	TATCGAAGTTTTCGGG
	(SEQ ID NO: 85)	(SEQ ID NO: 1533)
60	HIC1	TATTGAAGTTTTTGGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1534)
61	MLH1	AGGCGGCGATAGATTA
	(SEQ ID NO: 89)	(SEQ ID NO: 1541)
62	MLH1	ATGAGGTGGTGATAGA
	(SEQ ID NO: 89)	(SEQ ID NO: 1542)
63	PGR	TTTCGAGGTCGGATTT
	(SEQ ID NO: 83)	(SEQ ID NO: 1543)
64	PGR	TTTGAGGTTGGATTTTT
	(SEQ ID NO: 83)	(SEQ ID NO: 1544)
65	PGR	TTCGACGAAAAGACGT
	(SEQ ID NO: 83)	(SEQ ID NO: 2219)
66	PGR	TTTTTGATGAAAAGATGT
	(SEQ ID NO: 83)	(SEQ ID NO: 2220)
67	PGR	TTTTTTCGACGAAAAGA
	(SEQ ID NO: 83)	(SEQ ID NO: 1547)
68	PGR	AGGATTTTTTTGATGAAA
	(SEQ ID NO: 83)	(SEQ ID NO: 1548)
69	SERPINB5	TTATTAACGTGTTTGAGA
	(SEQ ID NO: 68)	(SEQ ID NO: 1549)
70	SERPINBS	TTATTAATGTGTTTGAGAA
	(SEQ ID NO: 68)	(SEQ ID NO: 1550)
71	RARB	ATGTCGAGAACGCGAG
	(SEQ ID NO: 88)	(SEQ ID NO: 1555)
72	RARB	GGATGTTGAGAATGTGA
	(SEQ ID NO: 88)	(SEQ ID NO: 1556)
73	RARB	AGCGATTCGAGTAGGG
	(SEQ ID NO: 88)	(SEQ TD NO: 1557)
74	RARB	AGTGATTTGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1558)
75	RARB	AGCGATTCGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1557)
76	RARB	AGTGATTTGAGTAGGG
	(SEQ ID NO: 88)	(SEQ ID NO: 1558)
77	RARB	TAGGATTCGGAACGTA
	(SEQ ID NO: 88)	(SEQ ID NO: 1559)
78	RARB	GGTAGGATTTGGAATGT
	(SEQ 10 NO: 88)	(SEQ ID NO: 1560)
79	TERT	AGGTGTACGGTTTCGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2187)
80	TERT	AGGTGTATGGTTTTGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2188)
81	TERT	AGGTGTACGGTTTCGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2187)
82	TERT	AGGTGTATGGTTTTGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2188)
83	TGFBR2	ATGGGGCGGACGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1567)
84	TGFBR2	ATGGGGTGGATGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1568)
85	TGFBR2	ATGGGGCGGACGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1567)
86	TGFBR2	ATGGGGTGGATGAATA
	(SEQ ID NO: 93)	(SEQ ID NO: 1568)
87	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1569)
88	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1570)
89	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1569)
90	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1570)
91	TIMP3	TTATTAACGGAGGAAGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1571)
92	TIMP3	TATTAATGGAGGAAGGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1572)
93	TIMP3	TTCGTTATGTGTACGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1573)
94	TIMP3	TTTGTTATGTGTATGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1574)
95	TIMP3	TTCGTTATGTGTACGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1573)
96	TIMP3	TTTGTTATGTGTATGGAA
	(SEQ SD NO: 103)	(SEQ ID NO: 1574)
97	TIMP3	GAGTATTTCGAGTTTGT
	(SEQ ID NO: 103)	(SEQ ID NO: 1575)
98	TIMP3	AGTATTTTGAGTTTGTATT
	(SEQ ID NO: 103)	(SEQ ID NO: 1576)
99	TIMP3	TAACGTTAATCGAGT
	(SEQ ID NO: 103)	(SEQ ID NO: 1577)
100	TIMP3	TAGGTGGTAATTGA
	(SEQ ID NO: 103)	(SEQ ID NO: 1578)
101	TP73	TTTCGGAGTTGCGAGT
	(SEQ ID NO: 86)	(SEQ ID NO: 1581)
102	TP73	TAGTTTTGGAGTTGTGA
	(SEQ ID NO: 86)	(SEQ ID NO: 1582)
103	CDH13	TAAAACGAGGGAGCGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1583)
104	CDH13	AAAATGAGGGAGTGTT
	(SEQ ID NO: 70)	(SEQ ID NO: 1584)
105	CDH13	TATCGCGTGTATGAA
	(SEQ ID NO: 70)	(SEQ ID NO: 585)
106	CDH13	TGTAGTTGTGTGTATGA
	(SEQ ID NO: 70)	(SEQ ID NO: 1586)
107	CDH13	ATGCGTCGTCGG
	(SEQ ID NO: 70)	(SEQ ID NO: 1587)
108	CDH13	AATGAAAATTTGTTGG
	(SEQ ID NO: 70)	(SEQ ID NO: 1588)
109	CDH13	TAGTCGAGAATTTCGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1589)
110	CDH13	TGTAGTTGAGAATTTTGT
	(SEQ ID NO: 70)	(SEQ ID NO: 1590)
111	TMS1/ASC	TTCGTTTCGGAGTCGA
	(SEQ ID NO: 84)	(SEQ ID NO: 1591)
112	TMS1/ASC	TTTGTTTTGGAGTTGAT
	(SEQ ID NO: 84)	(SEQ ID NO: 1592)
113	APAF1	AGTAGCGTCGGGTTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1595)
114	APAF1	GAGTAGTGTTGGGTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1596)
115	SYK	GAAGTTATCGCGTTGG
	(SEQ ID NO: 60)	(SEQ ID NO: 1597)
116	SYK	AGAAGTTATTGTGTTGG
	(SEQ ID NO: 60)	(SEQ ID NO: 1598)
117	SYK	GATCGATGCGGTTTAT
	(SEQ ID NO: 60)	(SEQ ID NO: 1599)
118	SYK	GGGATTGATTGGTTT
	(SEQ ID NO: 60)	(SEQ ID NO: 1600)
119	FABP3	GATGGGCGTATTAGTT
	(SEQ ID NO: 77)	(SEQ ID NO: 1605)
120	FABP3	GGGATGGGTGTATTAG
	(SEQ ID NO: 77)	(SEQ ID NO: 1606)
121	FADP3	GTGATGCGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1607)
122	FABP3	GTGATGTGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1608)
123	FABP3	GTGATGCGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1607)
124	FABP3	GTGATGTGAGGGTTAT
	(SEQ ID NO: 77)	(SEQ ID NO: 1608)
125	FABP3	TAAAGCGGTAGTTCGG
	(SEQ ID NO: 77)	(SEQ ID NO: 1609)
126	FABP3	AAGTGGTAGTTTGGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1610)
127	FABP3	TATTGGCGTTGACGTA
	(SEQ ID NO: 77)	(SEQ ID NO: 1611)
128	FABP3	TGGTGTTGATGTAGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1612)
129	RASSF1A	TACGGGTATTTTCGCGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1613)
130	RASSF1A	ATATGGGTATTTTTGTGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1614)
131	RASSF1A	AGAGCGCGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1615)
132	RASSF1A	GAGAGTGIGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1616)
133	RASSF1A	AGTAAATCGGATTAGGA
	(SEQ ID NO: 90)	(SEQ ID NO: 1617)
134	RASSF1A	AGTAAATTGGATTAGGAG
	(SEQ ID NO: 90)	(SEQ ID NO: 1618)
135	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1623)
136	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1624)
137	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1623)
138	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1624)
139	TWIST	TAGGTCGGGACGTAAA
	(SEQ ID NO: 100)	(SEQ ID NO: 1625)
140	TWIST	AGTAGGTTGGGATGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1626)
141	ESR2	TTTACGTGATCGAGTT
	(SEQ ID NO: 91)	(SEQ ID NO: 1631)
142	ESR2	AGITTATGTGATTGAGTT
	(SEQ ID NO: 91)	(SEQ ID NO: 1632)
143	PLAU	TATTTGTCGCGTTGAT
	(SEQ ID NO: 62)	(SEQ ID NO: 1633)
144	PLAU	ATTTGTTGTGTTGATGA
	(SEQ ID NO: 62)	(SEQ ID NO: 1634)
145	PLAU	TGTAATTCGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NQ: 1635)
146	PLAU	TTGTAATTTGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1636)
147	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1639)
148	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1640)
149	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1639)
150	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1640)
151	SLC19A1	GTCGTGCGGTTTTTAA
	(SEQ ID NO: 116)	(SEQ ID NO: 1663)
152	SLC19A1	GGTTGTGTGGTTTTTAA
	(SEQ ID NO: 116)	(SEQ ID NO: 1664)
153	SLC19A1	TTACGAAGGCGGTTTA
	(SEQ ID NO: 116)	(SEQ ID NO: 1665)
154	SLC19A1	TTTTATGAAGGTGGTTT
	(SEQ ID NO: 116)	(SEQ ID NO: 1666)
155	GJB2	GGATTTCGTCGGTATT
	(SEQ ID NO: 111)	(SEQ ID NO: 1667)
156	GJB2	GGGGATTTTGTTGGTA
	(SEQ ID NO: 111)	(SEQ ID NO: 1668)
157	HS3ST2	GAATCGGAGAGGCGAG
	(SEQ ID NO: 113)	(SEQ ID NO: 1671)
158	HS3ST2	AATTGGAGAGGTGAGG
	(SEQ ID NO: 113)	(SEQ ID NO: 1672)
159	HS3ST2	GGGTAATCGTTTGGTA
	(SEQ ID NO: 113)	(SEQ ID NO: 1673)
160	HS3ST2	GGGTAATTGTTTGGTAT
	(SEQ ID NO: 113)	(SEQ ID NO: 1674)
161	PRDM2	TGTAGAGACGACGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1675)
162	PRDM2	ATTGTAGAGATGATGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1676)
163	S100A7	TATAGTCGGGGTGATA
	(SEQ ID NO: 96)	(SEQ ID NO: 1689)
164	S100A7	TTTATAGTTGGGGTGAT
	(SEQ ID NO: 96)	(SEQ ID NO: 1690)
165	APC	GATTCGTATTTCGTAGT
	(SEQ ID NO: 65)	(SEQ ID NO: 1695)
166	AFC	GATTCGTATTTCGTAGT
	(SEQ ID NO: 65)	(SEQ ID NO: 1695)
167	APC	AGCGTTTTGGTTCGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1696)
168	APC	AGTGTTTTGGTTTGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1697)
169	APC	AGCGTTTTGGTTCGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1696)
170	AFC	AGTGTTTTGGTTTGTAT
	(SEQ ID NO: 65)	(SEQ ID NO: 1697)
171	APC	TTAATCGGCGGGTTTT
	(SEQ ID NO: 65)	(SEQ ID NO: 1698)
172	APC	AGTTAATTGGTGGGTT
	(SEQ ID NO: 65)	(SEQ ID NO: 1699)
173	APC	ATTTTCGAGTTCGGTA
	(SEQ ID NO: 65)	(SEQ ID NO: 1700)
174	APC	TTTTTGAGTTTGGTAGT
	(SEQ ID NO: 65)	(SEQ ID NO: 1701)
175	SEQ ID NO: 2	TTGATTGGCGGACGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1706)
176	SEQ ID NO: 2	TTGATTGGTGGATGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1707)
177	SEQ ID NO: 2	TTGATTGGCGGACGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1706)
178	SEQ ID NO: 2	TTGATTGGTGGATGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 1707)
179	IGEBP7	TAGTCGCGGAATGTTA
	(SEQ ID NO: 94)	(SEQ ID NO: 1708)
180	IGEBP7	TTGGTAGTTGTGGAAT
	(SEQ ID NO: 94)	(SEQ ID NO: 1709)
181	IGEBP7	ATTTTTTCGCGGGTAT
	(SEQ ID NO: 94)	(SEQ ID NO: 1710)
182	IGEBP7	TTTTTGTGGGTATTTTAG
	(SEQ ID NO: 94)	(SEQ ID NO: 1711)
183	IGFEF7	GGTATATTCGACGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1712)
184	IGFBP7	GGGTATATTTGATGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1713)
185	SOD2	TATTAGGCGGTTGCGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1720)
186	SOD2	TATTAGGTGGTTGTGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1721)
187	SOD2	TATTAGGCGGTTGCGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1720)
188	SOD2	TATTAGGTGGTTGTGG
	(SEQ ID NO: 105)	(SEQ ID NO: 1721)
189	THBS1	TAAAGGGGCGTTCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1726)
190	THBS1	AAGGGGTGTTTGTATT
	(SEQ ID NO: 81)	(SEQ ID NO: 1727)
191	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1728)
192	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1729)
193	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1728)
194	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1729)
195	ESR1	AAATCGGCGGGTTATT
	(SEQ ID NO: 75)	(SEQ ID NO: 1732)
196	ESR1	AGAAATTGGTGGGTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1733)
197	ESR1	AGTTGCGGACGGTTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1734)
198	ESR1	AGTTGTGGATGGTTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1735)
199	ESR1	AGTTGCGGACGGTTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1734)
200	ESR1	AGTTGTGGATGGTTTA
	(SEQ ID NO: 75)	(SEQ ID NO: 1735)
201	CASP8	TGTATTCGAGGCGGTA
	(SEQ ID NO: 71)	(SEQ ID NO: 1740)
202	CASP8	TTGTATTTGAGGTGGT
	(SEQ ID NO: 71)	(SEQ ID NO: 1741)
203	HOXA5	TTCGAGTTCGGTTGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1746)
204	HOXA5	GTTTGAGTTTGGTTGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1747)
205	HOXA5	TAGTTITCGGTCGGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1748)
206	HOXA5	TAGTITTTGGTTGGAAG
	(SEQ ID NO: 78)	(SEQ ID NO: 1749)
207	HOXA5	TAATTCGATTTCGGTTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1750)
208	HOXA5	TTTAATTTGATTTTGGTTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1751)
209	HOXA5	ATCGGTAGTTGACGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1752)
210	HOXA5	ATTGGTAGTTGATGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1753)
211	HOXA5	ATCGGTAGTTGACGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1752)
212	HOXA5	ATTGGTAGTTGATGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1753)
213	RARA	GAATTAGTATCGGTTTTT
	(SEQ ID NO: 108)	(SEQ ID NO: 1756)
214	RARA	ATTAGTATTGGTTTTTGG
	(SEQ ID NO: 108)	(SEQ ID NO: 1757)
215	SNCG	TGCGGTAGTATTCGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1758)
216	SNCG	TGTGGTAGTATTTGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1759)
217	SNCG	TGCGGTAGTATTCGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1758)
218	SNCG	TGTGGTAGTATTTGAGT
	(SEQ ID NO: 73)	(SEQ ID NO: 1759)
219	SNCG	TATCGGGGATAGTCGTT
	(SEQ ID NO: 73)	(SEQ ID NO: 2199)
220	SNCG	TATTGGGGATAGTTGTT
	(SEQ ID NO: 73)	(SEQ ID NO: 2200)
221	SNCG	TATCGGGGATAGTCGTT
	(SEQ ID NO: 73)	(SEQ ID NO: 2199)
222	SNCG	TATTGGGGATAGTTGTT
	(SEQ ID NO: 73)	(SEQ ID NO: 2200)
223	SNCG	TATCGGCGTTAATAGG
	(SEQ ID NO: 73)	(SEQ ID NO: 2201)
224	SNCG	TATTGGTGTTAATAGGAG
	(SEQ ID NO: 73)	(SEQ ID NO: 2202)
225	SLIT2	TTCGATAGTTAACGATG
	(SEQ ID NO: 112)	(SEQ ID NO: 1772)
226	SLIT2	TTTGATAGTTAATGATGGT
	(SEQ ID NO: 112)	(SEQ ID NO: 1773)
227	SLIT2	ATTTCGTCGTAGTTTG
	(SEQ ID NO: 112)	(SEQ ID NO: 1774)
228	SLIT2	TTTTGTTGTAGTTTGGA
	(SEQ ID NO: 112)	(SEQ ID NO: 1775)
229	SLIT2	TAGCGGGTTCGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1776)
230	SLIT2	TTAGTGGGTTTGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1777)
231	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1778)
232	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1779)
233	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1778)
234	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1779)
235	IGSF4	AGGTAGATCGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1780)
236	IGSF4	AGGTAGATTGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1781)
237	IGSF4	AGGTAGATCGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1780)
238	IGSF4	AGGTAGATTGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1781)
239	IGSF4	TAGGTTTTCGGATTGA
	(SEQ ID NO: 74)	(SEQ ID NO: 1784)
240	IGSF4	GTAGGTTTTTGGATTGA
	(SEQ ID NO: 74)	(SEQ ID NO: 1785)
241	MCT1	ATTTTACGTAGGCGTT
	(SEQ ID NO: 101)	(SEQ ID NO: 1786)
242	MCT1	GATTTTATGTAGGTGTTT
	(SEQ ID NO: 101)	(SEQ ID NO: 1787)
243	MCT1	AGTTAGTCGCGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1788)
244	MCT1	AGAGTTAGTTGTGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1789)
245	MCT1	TATACGAGGAAGGTCGG
	(SEQ ID NO: 101)	(SEQ ID NO: 1790)
246	MCT1	TATATGAGGAAGGTTGG
	(SEQ ID NO: 101)	(SEQ ID NO: 1791)
247	MCT1	TATACGAGGAAGGTCGG
	(SEQ ID NO: 101)	(SEQ ID NO: 1790)
248	MCT1	TATATGAGGAAGGTTGG
	(SEQ ID NO: 101)	(SEQ ID NO: 1791)
249	SEQ ID NO: 6	AAGTTTATCGGCGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1792)
250	SEQ ID NO: 6	AGAAGTTTATTGGTGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1793)
251	SEQ ID NO: 6	ATTTCGGAATTTAAGCGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1794)
252	SEQ ID NO: 6	TTTTGGAATTTAAGTGTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1795)
253	SEQ ID NO: 6	TAATTTCGGACGCGGA
	(SEQ ID NO: 6)	(SECQ ID NO: 1796)
254	SEQ ID NO: 6	TTTTGGATGTGGAGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1797)
255	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1798)
256	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1799)
257	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1798)
258	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1799)
259	SEQ ID NO: 6	TTTCGGTTTTCGTTAAT
	(SEQ ID NO: 6)	(SEQ ID NO: 1800)
260	SEQ ID NO: 6	TTTGGTTTTTGTTAATTTAG
	(SEQ ID NO: 6)	(SEQ ID NO: 1801)
261	SEQ ID NO: 6	TGTGCGAAGTTAACGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1802)
262	SEQ ID NO: 6	TTGTGTGAAGTTAATGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1803)
263	SEQ ID NO: 8	ATAAAGCGGGGTTTTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1804)
264	SEQ ID NO: 8	GGATAAAGTGGGGTTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1805)
265	PROSTAGLANDIN E2	AGTGTATCGTTTTTCGG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1812)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
266	PROSTAGLANDIN E2	TAGTGTATTGTTTTTTGG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1813)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
267	PROSTAGLANDIN E2	TGCGTATCGTTAGTTA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1814)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
268	PROSTAGLANDIN E2	AGGTTGTGTATTGTTAG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1815)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
269	PROSTAGLANDIN E2	ATTATTTCGGCGGTGA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1816)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
270	PROSTAGLANDIN E2	GATTATTTTGGTGGTGA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1817)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
271	PROSTAGLANDIN E2	TAAGTCGCGTAAGGAG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1818)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
272	PROSTAGLANDIN E2	AAGTTGTGTAAGGAGTA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1819)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
273	PROSTAGLANDIN E2	GTATCGCGAGTTTGGA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1820)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
274	PROSTAGLANDIN E2	GTATTGTGAGTTTGGAG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1821)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
275	SEQ ID NO: 51	GTCGGGGTCGATTCGA
	(SEQ ID NO: 51)	(SEQ ID NO: 1822)
276	SEQ ID NO: 51	GTTGGGGTTGATTTGAT
	(SEQ ID NO: 51)	(SEQ ID NO: 1823)
277	SEQ ID NO: 51	AGGATTCGTTTGCGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1824)
278	SEQ ID NO: 51	AAGGATTTGTTTGTGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1825)
279	MGC34831	ATTAGCGTTTGGCGTT
	(SEQ ID NO: 52)	(SEQ ID NO: 1826)
280	MGC34831	AATTAGTGTTTGGTGTT
	(SEQ ID NO: 52)	(SEQ ID NO: 1827)
281	MGC34831	GTTTAGCGACGGTCGT
	(SEQ ID NO: 52)	(SEQ ID NO: 1828)
282	MGC34831	TGTTTAGTGATGGTTGT
	(SEQ ID NO: 52)	(SEQ ID NO: 1829)
283	SEQ ID NO: 54	TGTGTAGCGGCGATTA
	(SEQ ID NO: 54)	(SEQ ID NO: 1830)
284	SEQ ID NO: 54	GTGTGTAGTGGTGATT
	(SEQ ID NO: 54)	(SEQ ID NO: 1831)
285	SEQ ID NO: 54	ATTAGCGTTTGGTCGG
	(SEQ ID NO: 54)	(SEQ ID NO: 1832)
286	SEQ ID NO: 54	ATTAGTGTTTGGTTGGG
	(SEQ ID NO: 54)	(SEQ ID NO: 1833)
287	PDLIM1	TAGGTCGCGTAGTCGT
	(SEQ ID NO: 55)	(SEQ ID NO: 1834)
288	PDLIM1	TTAGGTTGTGTAGTTGT
	(SEQ ID NO: 55)	(SEQ ID NO: 1835)
289	DKK3	ATTCGTTTTAGTTCGAG
	(SEQ ID NO: 24)	(SEQ ID NO: 1842)
290	DKK3	ATTTGTTTTAGTTTGAGT
	(SEQ ID NO: 24)	(SEQ ID NO: 1843)
291	DKK3	TTCGATCGTTTTAGGA
	(SEQ ID NO: 24)	(SEQ ID NO: 1844)
292	DKK3	AGTTTTGATTGTTTTAGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1845)
293	DKK3	GAAAAGACGCGATTTT
	(SEQ ID NO: 24)	(SEQ ID NO: 1848)
294	DKK3	GAAAAGATGTGATTTTATT
	(SEQ ID NO: 24)	(SEQ ID NO: 1849)
295	SEQ ID NO: 29	TTGATGCGGAGTTCGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1852)
296	SEQ ID NO: 29	TTGATGTGGAGTTTGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1853)
297	SEQ ID NO: 29	TTGATGCGGAGTTCGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1852)
298	SEQ ID NO: 29	TTGATGTGGAGTTTGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1853)
299	SEQ ID NO: 29	TTCGAAGCGTGTATTA
	(SEQ ID NO: 29)	(SEQ ID NO: 2155)
300	SEQ ID NO: 29	GGGTTTGAAGTGTGTA
	(SEQ ID NO: 29)	(SEQ ID NO: 2156)
301	SEQ ID NO: 29	TAGGAACGGTAGGCGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1854)
302	SEQ ID NO: 29	TAGGAATGGTAGGTGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1855)
303	SEQ ID NO: 29	TAGGAACGGTAGGCGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1854)
304	SEQ ID NO: 29	TAGGAATGGTAGGTGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1855)
305	SEQ ID NO: 29	GTCGGAGGCGTTTGAG
	(SEQ ID NO: 29)	(SEQ ID NO: 1856)
306	SEQ ID NO: 29	GTTGGAGGTGTTTGAGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1857)
307	ARL7	TAGATTTCGTAGTTTTTTA
	(SEQ ID NO: 30)	(SEQ ID NO: 1858)
308	ARL7	TAGATTTTGTAGTTTTTTAA
	(SEQ ID NO: 30)	(SEQ ID NO: 1859)
309	ARL7	TGGGTACGTTTACGGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1860)
310	ARL7	TGGGTATGTTTATGGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1861)
311	ARL7	GAAGAAATCGTTTTTGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1862)
312	ARL7	GAAGAAATTGTTTTTGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1863)
313	ARL7	TAGTAGGATCGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1864)
314	ARL7	ATAGTAGGATTGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1865)
315	SEQ ID NO: 31	AACGTTGCTTGGGTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1866)
316	SEQ ID NO: 31	AATGTTGTGTTGGGTAA
	(SEQ ID NO: 31)	(SEQ ID NO: 1867)
317	SEQ ID NO: 31	TAGCGTTTCGTGGTTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1868)
318	SEQ ID NO: 31	GTAGTGTTTTGTGGTTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1869)
319	THH	GTTCGTTGGCGTAAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1872)
320	THH	GGTTTGTTGGTGTAAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1873)
321	(SEQ ID NO: 36)	GGACGTTGCGATTGTA
		(SEQ ID NO: 2161)
322	(SEQ ID NO: 36)	GATGTTGTGATTGTAGT
		(SEQ ID NO: 2162)
323	SENP3	TATTCGGATCGGGTTT
	(SEQ ID NO: 39)	(SEQ ID NO: 1876)
324	SENP3	TTTATTTGGATTGGGTT
	(SEQ ID NO: 39)	(SEQ ID NO: 1877)
325	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1878)
326	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1879)
327	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1878)
328	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1879)
329	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1882)
330	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1883)
331	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1882)
332	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1883)
333	SEQ ID NO: 42	GAGTCGGGTTGCGATG
	(SEQ ID NO: 42)	(SEQ ID NO: 1884)
334	SEQ ID NO: 42	GGAGTTGGGTTGTGAT
	(SEQ ID NO: 42)	(SEQ ID NO: 1885)
335	SEQ ID NO: 42	ATGGGTTGCGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1886)
336	SEQ ID NO: 42	ATGGGTTGCGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1887)
337	SEQ ID NO: 42	ATGGGTTGCGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1886)
338	SEQ ID NO: 42	ATGGGTTGTGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1887)
339	(SEQ ID NO: 117)	TAGCGGTTTTTTAGCGTA
		(SEQ ID NO: 1888)
340	(SEQ ID NO: 117)	AGTGGTTTTTTAGTGTAT
		(SEQ ID NO: 1889)
341	(SEQ ID NO: 117)	AGATGCGCGGGTAGAT
		(SEQ ID NO: 1890)
342	(SEQ ID NO: 117)	AGATGTGTGGGTAGAT
		(SEQ ID NO: 1891)
343	(SEQ ID NO: 117)	AGATGCGCGGGTAGAT
		(SEQ ID NO: 1890)
344	(SEQ ID NO: 117)	AGATGTGTGGGTAGAT
		(SEQ ID NO: 1891)
345	(SEQ ID NO: 117)	AGATAGTTCGTATTCGT
		(SEQ ID NO: 1892)
346	(SEQ ID NO: 117)	GTAGATAGTTTGTATTTGT
		(SEQ ID NO: 1893)
347	(SEQ ID NO: 117)	TTTGTTCGTAAGGTTT
		(SEQ ID NO: 1894)
348	(SEQ ID NO: 117)	TGTTTGTAATGTTTAGAG
		(SEQ ID NO: 1895)
349	O60279	GGACGGCGGAAAATTA
	(SEQ ID NO: 47)	(SEQ ID NO: 1902)
350	O60279	AGGGATGGTGGAAAAT
	(SEQ ID NO: 47)	(SEQ ID NO: 1903)
351	SEQ ID NO: 48	TATTTGGCGATTCGGA
	(SEQ ID NO: 48)	(SEQ ID NO: 1904)
352	SEQ ID NO: 48	TGGTGATTTGGAGATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1905)
353	SEQ ID NO: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1906)
354	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1907)
355	SEQ ID NO: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1906)
356	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1907)
357	SEQ ID NO: 48	AAAATCGTATGCGTGT
	(SEQ ID NO: 48)	(SEQ ID NO: 1910)
358	SEQ ID NO: 48	GAAAATTGTATGTGTGTG
	(SEQ ID NO: 48)	(SEQ ID NO: 1911)
359	SEQ ID NO: 9	AGTGTTCGTCGTAGTT
	(SEQ ID NO: 9)	(SEQ ID NO: 1914)
360	SEQ ID NO: 9	TGAGTGTTTGTTGTAGT
	(SEQ ID NO: 9)	(SEQ ID NO: 1915)
361	SEQ ID NO: 4	TTTTGTTCGCGTTGAA
	(SEQ ID NO: 4)	(SEQ ID NO: 1916)
362	SEQ ID NO: 4	TTGTTTGTGTTGAAGTA
	(SEQ ID NO: 4)	(SEQ ID NO: 1917)
363	SEQ ID NO: 4	GGGTCGCGAGGTAGTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1918)
364	SEQ ID NO: 4	TGGGTTGTGAGGTAGT
	(SEQ ID NO: 4)	(SEQ ID NO: 1919)
365	SEQ ID NO: 4	TTTGTGCGACGTTATT
	(SEQ ID NO: 4)	(SEQ ID NO: 1920)
366	SEQ ID NO: 4	GGTTTGTGTGATGTTAT
	(SEQ ID NO: 4)	(SEQ ID NO: 1921)
367	SEQ ID NO: 4	ATGGCGGTTTCGATTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1922)
368	SEQ ID NO: 4	GATGGTGGTTTTGATTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1923)
369	SEQ ID NO: 7	TAGTCGTCGTGTAGGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1932)
370	SEQ ID NO: 7	TAGGTAGTTGTTGTGTA
	(SEQ ID NO: 7)	(SEQ ID NO: 1933)
371	SEQ ID NO: 7	TATAGGTACGCGATGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1934)
372	SEQ ID NO: 7	AGGTATGTGATGAGGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1935)
373	SEQ ID NO: 7	ATGATTTGCGTTACGT
	(SEQ ID NO: 7)	(SEQ ID NO: 1938)
374	SEQ ID NO: 7	ATGATTTGTGTTATGTTT
	(SEQ ID NO: 7)	(SEQ ID NO: 1939)
375	SEQ ID NO: 7	TAACGTTGTGGTTCGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1940)
376	SEQ ID NO: 7	TAATGTTGTGGTTTGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1941)
377	SEQ ID NO: 7	TAACGTTGTGGTTCGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1940)
378	SEQ ID NO: 7	TAATGTTGTGGTTTGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1941)
379	PROSTAGLANDIN E2	AGGTAATCGAGGCGGT
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1952)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
380	PROSTAGLANDIN E2	AGGTAATTGAGGTGGT
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1953)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
381	PROSTAGLANDIN E2	AGGTAATCGAGGCGGT
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1952)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
382	PROSTAGLANDIN E2	AGGTAATTGAGGTGGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1953)
	TYPE (PROSTANOID
	EP4 RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 11)
383	PROSTAGLANDIN E2	TTACGGAGGCGTTTTA
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1958)
	TYPE (PROSTANOID
	EP4 RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 11)
384	PROSTAGLANDIN E2	TTTTATGGAGGTGTTTT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1959)
	TYPE (PROSTANOID
	EP4 RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 11)
385	PROSTAGLANDIN E2	AGGCGAATTTATCGGG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1960)
	TYPE (PROSTANOID
	EP4 RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 11)
386	PROSTAGLANDIN E2	GGTGAATTTATTGGGG
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1961)
	TYPE (PROSTANOID
	EP4 RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 11)
387	PROSTAGLANDIN E2	TAGTCGAAGTAGGCGT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1962)
	TYPE (PROSTANOID
	EP4 RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 11)
388	PROSTAGLANDIN E2	TAGTTGAAGTAGGTGTT
	RECEPTOR, EP4 SUB-	(SEQ ID NO: 1963)
	TYPE (PROSTANOID
	EP4 RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 11)
389	LIM DOMAIN KINASE	TGTAGTCGGGAGGTTA
	1 (EC 2.7.1.37)	(SEQ ID NO: 1966)
	(LIMK-1)
	(SEQ ID NO: 12)
390	LIM DOMAIN KINASE	IGTAGITGGGAGGTTA
	1 (EC 2.7.1.37)	(SEQ ID NO: 1967)
	(LIMK-1)
	(SEQ ID NO: 12)
391	LIM DOMAIN KINASE	TGTAGTCGGGAGGTTA
	1 (EC 2.7.1.37)	(SEQ ID NO: 1966)
	(LIMK-1)
	(SEQ ID NO: 12)
392	LIM DOMAIN KINASE	TGTAGTTGGGAGGTTA
	1 (EC 2.7.1.37)	(SEQ ID NO: 1967)
	(LIMK-1)
	(SEQ ID NO: 12)
393	LIM DOMAIN KINASE	GGATTATCGCGGGGGT
	1 (EC 2.7.1.37)	(SEQ ID NO: 1968)
	(LIMK-1)
	(SEQ ID NO: 12)
394	LIM DOMAIN KINASE	GGATTATTGTGGGGGT
	1 (EC 2.7.1.37)	(SEQ ID NO: 1969)
	(LIMK-1)
	(SEQ ID NO: 12)
395	LIM DOMAIN KINASE	GGATTATCGCGGGGGT
	1 (EC 2.7.1.37)	(SEQ ID NO: 1968)
	(LIMK-1)
	(SEQ ID NO: 12)
396	LIM DOMAIN KINASE	GGATTATTGTGGGGGT
	1 (EC 2.7.1.37)	(SEQ ID NO: 1969)
	(LIMK-1)
	(SEQ ID NO: 12)
397	LIM DOMAIN KINASE	GTCGGTAGTTTATCGGAT
	1 (EC 2.7.1.37)	(SEQ ID NO: 1970)
	(LIMK-1)
	(SEQ ID NO: 12)
398	LIM DOMAIN KINASE	GTTGGTAGTTTATTGGAT
	1 (EC 2.7.1.37)	(SEQ ID NO: 1971)
	(LIMK-1)
	(SEQ ID NO: 12)
399	LIM DOMAIN KINASE	GTTGGTAGTTTATTGGAT
	1 (EC 2.7.1.37)	(SEQ ID NO: 1970)
	(LIMK-1)
	(SEQ ID NO: 12)
400	LIM DOMAIN KINASE	GTTGGTAGTTTATTGGAT
	1 (EC 2.7.1.37)	(SEQ ID NO: 1971)
	(LIMK-1)
	(SEQ ID NO: 12)
401	BCL11B	TAGGTTTCGATTCGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1974)
402	BCL11B	TTAGGTTTTGATTTGTTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1975)
403	BCL11B	AAGTCGTCGGAGTTAG
	(SEQ ID NO: 50)	(SEQ ID NO: 1976)
404	BCL11B	GTGAAGTTGTTGGAGT
	(SEQ ID NO: 50)	(SEQ ID NO: 1977)
405	MSF	GTTTCGAAATTGGCGT
	(SEQ ID NO: 13)	(SEQ ID NO: 1980)
406	MSF	TTTGAAATTGGTGTGG
	(SEQ ID NO: 13)	(SEQ ID NO: 1981)
407	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1982)
408	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1983)
409	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1982)
410	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1983)
411	MSF	TTACGGTTCGATTTTG
	(SEQ ID NO: 13)	(SEQ ID NO: 1984)
412	MSF	TATGGTTTGATTTTGGG
	(SEQ ID NO: 13)	(SEQ ID NO: 1985)
413	SEQ ID NO: 14	TAAGGCGTTTTCGATA
	(SEQ ID NO: 14)	(SEQ ID NO: 2986)
414	SEQ ID NO: 14	GTAAGGTGTTTTTGATAT
	(SEQ ID NO: 14)	(SEQ ID NO: 1987)
415	SEQ ID NO: 16	AGGAGTTTTCGTGTCGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1992)
416	SEQ ID NO: 16	AGGAGTTTTTGTGTTGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1993)
417	SEQ ID NO: 16	AGGAGTTTTCGTGTCGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1992)
418	SEQ ID NO: 16	AGGAGTTTTTGTGTTGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1993)
419	SEQ ID NO: 16	AGGCGTTGTCGGTGAT
	(SEQ ID NO: 16)	(SEQ ID NO: 1996)
420	SEQ ID NO: 16	AGGTGTTGTTGGTGATA
	(SEQ ID NO: 16)	(SEQ ID NO: 1997)
421	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1998)
422	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1999)
423	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1998)
424	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1999)
425	SEQ ID NO: 17	ATTTAGTCGTGCGTTT
	(SEQ ID NO: 17)	(SEQ ID NO: 2000)
426	SEQ ID NO: 17	TGATTTAGTTGTGTGTT
	(SEQ ID NO: 17)	(SEQ ID NO: 2001)
427	SEQ ID NO: 18	TTTACGCGGGGTTTTA
	(SEQ ID NO: 18)	(SEQ ID NO: 2002)
428	SEQ ID NO: 18	TTTATGTGGGGTTTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2003)
429	SEQ ID NO: 18	TTACGTCGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2004)
430	SEQ ID NO: 18	TTTTATGTTGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2005)
431	SEQ ID NO: 18	AAAGCGGAGTCGTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2010)
432	SEQ ID NO: 18	AGTGGAGTTGTTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2011)
433	SEQ ID NO: 19	AGGTTTTCGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2012)
434	SEQ ID NO: 19	TAGGTTTTTGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2013)
435	NR2E1	AATGTAGCGGCGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2028)
436	NR2E1	TAAATGTAGTGGTGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2029)
437	NR2E1	GTCGTTATCGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2030)
438	NR2E1	GTTGTTATTGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2031)
439	NR2E1	GTCGTTATCGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2030)
440	NR2E1	GTTGTTATTGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2031)
441	NR2E1	GACGTAAGTTTCGGGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2032)
442	NR2E1	GGATGTAAGTTTTGGG
	(SEQ ID NO: 22)	(SEQ ID NO: 2033)
443	NR2E1	TTTTTAGTCGCGAGAA
	(SEQ ID NO: 22)	(SEQ ID NO: 2034)
444	NR2E1	TTTTTAGTTGTGAGAAGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2035)
445	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2036)
446	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2037)
447	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2036)
448	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2037)
449	NR2E1	AGGCGAGTCGGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2038)
450	NR2E1	AGGTGAGTTGGAGTTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2039)
451	NR2E1	AGGGACGCGAAAATTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2042)
452	NR2E1	GGAGGGATGTGAAAAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2043)
453	PCDH7	ATCGTAGTCGGTTTTA
	(SEQ ID NO: 23)	(SEQ ID NO: 2044)
454	PCDH7	GATTATTGTAGTTGGTTT
	(SEQ ID NO: 23)	(SEQ ID NO: 2045)
455	RTTN	TAGATTGACGGGACGA
	(SEQ ID NO: 25)	(SEQ ID NO: 2221)
456	RTTN	TAGATTGATGGGATGAG
	(SEQ ID NO: 25)	(SEQ ID NO: 2222)
457	RTTN	TAGTGGCGCGGTAGTT
	(SEQ ID NO: 25)	(SEQ ID NO: 2046)
458	RTTN	TAGTGGTGTGGTAGTTT
	(SEQ ID NO: 25)	(SEQ ID NO: 2047)
459	RTTN	TAGGACGTGTTTTCGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2048)
460	RTTN	AGGATGTGTTTTTGGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2049)
461	SNAP25	TATTTCGAGTTAGAGTTACGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2050)
462	SNAP25	TATTTTGAGTTAGAGTTATGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2051)
463	SNAP25	TATTTCGAGTTAGAGTTACGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2050)
464	SNAP25	TATTTTGAGTTAGAGTTATGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2051)
465	GIRK2	AGTTGTTCGTAGGCGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2060)
466	GIRK2	AGTTGTTTGTAGGTGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2061)
467	GIRK2	AGTTGTTCGTAGGCGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2060)
468	GIRK2	AGTTGTTTGTAGGTGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2061)
469	GIRK2	TTATTTCGTTCGTAGTT
	(SEQ ID NO: 27)	(SEQ ID NO: 2062)
470	GIRK2	TTTGTTTGTAGTTAGGTA
	(SEQ ID NO: 27)	(SEQ ID NO: 2063)
471	GIRK2	TTAGTCGAAAGGCGAG
	(SEQ ID NO: 27)	(SEQ ID NO: 2064)
472	GIRK2	TAGTTGAAAGGTGAGG
	(SEQ ID NO: 27)	(SEQ ID NO: 2065)
473	SEQ ID NO: 28	ATTAGGCGAGTTTCGT
	(SEQ ID NO: 28)	(SEQ ID NO: 2066)
474	SEQ ID NO: 28	TTAGGTGAGTTTTGTTT
	(SEQ ID NO: 28)	(SEQ ID NO: 2067)
475	SEQ ID NO: 31	TTTACGTAGGGCGATT
	(SEQ ID NO: 31)	(SEQ ID NO: 2068)
476	SEQ ID NO: 31	ATTTTTATGTAGGGTGAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2069)
477	SEQ ID NO: 31	GATACGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2070)
478	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2071)
479	SEQ ID NO: 31	GATACGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2070)
480	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2071)
481	SEQ ID NO: 31	TTCGGGCGTTTTATAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2072)
482	SEQ ID NO: 31	GGTTTGGGTGTTTTATA
	(SEQ ID NO: 31)	(SEQ ID NO: 2073)
483	HOXB13	GTCGTTATTATTTCGAGG
	(SEQ ID NO: 34)	(SEQ ID NO: 2074)
484	HOXB13	GTTGTTATTATTTTGAGGA
	(SEQ ID NO: 34)	(SEQ ID NO: 2075)
485	HOXB13	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2076)
486	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2077)
487	HOX513	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2076)
488	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2077)
489	LMXIA	GTGGGGTTTTTCGGAA
	(SEQ ID NO: 36)	(SEQ ID NO: 2092)
490	LMXIA	GTTGGGTTTTTTGGAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2093)
491	TITF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2104)
492	TITF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2105)
493	TITF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2104)
494	TITF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2105)
495	TITF1	GGTTCGTTTAAGTTCGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2106)
496	TITF1	GGTTTGTTTAAGTTTGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2107)
497	TITF1	GGTTCGTTTAAGTTCGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2106)
498	TITF1	GGTTTGTTTAAGTTTGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2107)
499	TITFI	TATTTCGTTTTCGTAATT
	(SEQ ID NO: 41)	(SEQ ID NO: 2110)
500	TITF1	TTTGTTTTTGTAATTAGATT
	(SEQ ID NO: 41)	(SEQ ID NO: 2111)
501	DDX51	AACGTGCGGGGTTTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2116)
502	DDX51	TGAATGTGTGGGGTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2117)
503	SEQ ID NO: 46	GAGTCGGGTTATCGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2120)
504	SEQ ID NO: 46	GGAGTTGGGTTATTGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2121)
505	SEQ ID NO: 46	TTACGGATGTTTCGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2122)
506	SEQ ID NO: 46	TTTATGGATGTTTTGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2123)
507	SEQ ID NO: 46	TGACGTATTTTCGGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2124)
508	SEQ ID NO: 46	GGTGATGTATTTTTGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2125)
509	SEQ ID NO: 46	ATAGTCGGAATCGTTG
	(SEQ ID NO: 46)	(SEQ ID NO: 2126)
510	SEQ ID NO: 46	TAGTTGGAATTGTTGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2127)
511	SEQ ID NO: 2	TAGTAGTCGGCGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2130)
512	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2131)
513	SEQ ID NO: 2	TAGTAGTGGGCGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2130)
514	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2131)
515	SEQ ID NO: 3	TTGCGTTAATTCGGTA
	(SEQ ID NO: 3)	(SEQ ID NO: 2132)
516	SEQ ID NO: 3	AATTTGTGTTAATTTGGT
	(SEQ ID NO: 3)	(SEQ ID NO: 2133)
517	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2134)
518	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2135)
519	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2134)
520	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2135)
521	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2136)
522	SEQ ID NO: 3	GGTTGAAGAGTTGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2137)
523	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2136)
524	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2137)
525	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2138)
526	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2139)
527	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2138)
528	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2139)

TABLE 20
Breast cancer vs. benign breast conditions
No:	Gene	Oligo:
1	SCGB3A1	GGCGTAGAAGGCGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2140)
2	SCGB3A1	GGTGTAGAAGGTGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2141)
3	SCGB3A1	GGCGTAGAAGGCGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2140)
4	SCGB3A1	GGTGTAGAAGGTGTTT
	(SEQ ID NO: 115)	(SEQ ID NO: 2141)
5	SCGB3A1	TAGTGTTCGACGTTGT
	(SEQ ID NO: 115)	(SEQ ID NO: 1475)
6	SCGB3A1	TAGTGTTTGATGTTGTT
	(SEQ ID NO: 115)	(SEQ ID NO: 1476)
7	ARH1/NOEY2	TAAAACGTTCGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1485)
8	ARH1/NOEY2	TTTAAAATGTTTGGTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1486)
9	ARH1/NOEY2	TGTATTCGTCGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1487)
10	ARH1/NOEY2	AATGTATTTGTTGTTAGG
	(SEQ ID NO: 97)	(SEQ ID NO: 1488)
11	ARH1/NOEY2	TTAGACGGAGTTCGGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1489)
12	ARH1/NOEY2	TAGATGGAGTTTGGAGA
	(SEQ ID NO: 97)	(SEQ ID NO: 1490)
13	ARH1/NOEY2	TAGACGTAGGCGTATT
	(SEQ ID NO: 97)	(SEQ ID NO: 1491)
14	ARH1/NOEY2	GGGTAGATGTAGGTGT
	(SEQ ID NO: 97)	(SEQ ID NO: 1492)
15	CCND2	TTAGGGTCGATCGTGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1493)
16	CCND2	TAGGGTTGATTGTGTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1494)
17	CCND2	TTATCGTAGTCGGTTT
	(SEQ ID NO: 104)	(SEQ ID NO: 1495)
18	CCND2	GATTTTATTGTAGTTGGT
	(SEQ ID NO: 104)	(SEQ ID NO: 1496)
19	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1497)
20	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1498)
21	CCND2	GAGTGAGGCGCGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1497)
22	CCND2	GAGTGAGGTGTGAAAT
	(SEQ ID NO: 104)	(SEQ ID NO: 1498)
23	CCND2	AAGGATCGAGCGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1499)
24	CCND2	AAGGATTGAGTGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1500)
25	CCND2	AAGGATCGAGCGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1499)
26	CCND2	AAGGATTGAGTGTGGA
	(SEQ ID NO: 104)	(SEQ ID NO: 1500)
27	CDKN1A	ATTAGGGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1501)
28	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1502)
29	CDKN1A	ATTAGGGTCGCGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1501)
30	CDKN1A	ATTAGGGTTGTGTTGA
	(SEQ ID NO: 67)	(SEQ ID NO: 1502)
31	CDKN2A	GGCGTTGTTTAACGTAT
	(SEQ ID NO: 57)	(SEQ ID NO: 1503)
32	CDKN2A	GGGTGTTGTTTAATGTA
	(SEQ ID NO: 57)	(SEQ ID NO: 1504)
33	DAPK1	TTTCGGAGATTCGGTT
	(SEQ ID NO: 98)	(SEQ ID NO: 1509)
34	DAPK1	TTTGGAGATTTGGTTTT
	(SEQ ID NO: 98)	(SEQ ID NO: 1510)
35	DAPK1	TTTTAGCGTCGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1511)
36	DAPK1	TTTTAGTGTTGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1512)
37	DAPK1	TTTTAGCGTCGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1511)
38	DAPK1	TTTTAGTGTTGGGGAG
	(SEQ ID NO: 98)	(SEQ ID NO: 1512)
39	EYA4	GGTATAAAATCGTAAATTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1513)
40	EYA4	GGGTATAAAATTGTAAATTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1514)
41	EYA4	TATGTAGTCGCGTAGT
	(SEQ ID NO: 58)	(SEQ ID NO: 1515)
42	EYA4	TTTATGTAGTTGTGTAGT
	(SEQ ID NO: 58)	(SEQ ID NO: 1516)
43	EYA4	GTTTAGATACGAAATGTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1517)
44	EYA4	GTTTAGATATGAAATGTTAT
	(SEQ ID NO: 58)	(SEQ ID NO: 1518)
45	EYA4	AGTTTTGACGTCGTTT
	(SEQ ID NO: 58)	(SEQ ID NO: 1519)
46	EYA4	TTGATGTTGTTTTGGAA
	(SEQ ID NO: 58)	(SEQ ID NO: 1520)
47	FHIT	GTTACGTTAGCGGGTT
	(SEQ ID NO: 76)	(SEQ ID NO: 1521)
48	FHIT	GGTTATGTTAGTGGGT
	(SEQ ID NO: 76)	(SEQ ID NO: 1522)
49	GSTP1	GGCGATTTCGGGGATT
	(SEQ ID NO: 59)	(SEQ ID NO: 1525)
50	GSTP1	GGTGATTTTGGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1526)
51	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1527)
52	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1528)
53	GSTP1	GACGTTCGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1527)
54	GSTP1	GATGTTTGGGGTGTAG
	(SEQ ID NO: 59)	(SEQ ID NO: 1528)
55	GSTP1	AGTTCGCGGGATTTTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1529)
56	GSTP1	GGAGTTTGTGGGATTT
	(SEQ ID NO: 59)	(SEQ ID NO: 1530)
57	GSTP1	AGTTTTCGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1531)
58	GSTP1	TAGTTTTTGTTATTAGTGA
	(SEQ ID NO: 59)	(SEQ ID NO: 1532)
59	HIC1	TATCGAAGTTTTCGGG
	(SEQ ID NO: 85)	(SEQ ID NO: 1533)
60	HIC1	TATTGAAGTTTTTGGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1534)
61	HIC1	TAGCGGTTATTTCGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1535)
62	HIC1	TTTAGTGGTTATTTTGGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1536)
63	HIC1	TACGTTTTTCGTAGCGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1537)
64	HIC1	ATTATGTTTTTTGTAGTGT
	(SEQ ID NO: 85)	(SEQ ID NO: 1538)
65	HIC1	TTCGGTTTTGTCGTATA
	(SEQ ID NO: 85)	(SEQ ID NO: 1539)
66	HIC1	TTTGGTTTTGTTGTATAG
	(SEQ ID NO: 85)	(SEQ ID NO: 1540)
67	SERPINB5	ATTGTCGTACGTATGT
	(SEQ ID NO: 68)	(SEQ ID NO: 1551)
68	SERPINB5	AGAGGATTGTTGTATGTA
	(SEQ ID NO: 68)	(SEQ ID NO: 1552)
69	SERPINB5	TTTTTTGTTCGAATATGT
	(SEQ ID NO: 68)	(SEQ ID NO: 1553)
70	SERPINB5	TTTGTTTGAATATGTTGG
	(SEQ ID NO: 68)	(SEQ ID NO: 1554)
71	TERT	TATAACGAACGTCGTT
	(SEQ ID NO: 92)	(SEQ ID NO: 2142)
72	TERT	AGGTATAATGAATGTTGT
	(SEQ ID NO: 92)	(SEQ ID NO: 2143)
73	TGFBR2	AAGACGGTTAGGTCGG
	(SEQ ID NO: 93)	(SEQ ID NO: 2144)
74	TGFBR2	AAGATGGTTAGGTTGG
	(SEQ ID NO: 93)	(SEQ ID NO: 2145)
75	TGFBR2	AAGACGGTTAGGTCGG
	(SEQ ID NO: 93)	(SEQ ID NO: 2144)
76	TGFBR2	AAGATGGTTAGGTTGG
	(SEQ ID NO: 93)	(SEQ ID NO: 2145)
77	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1569)
78	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1570)
79	THRB	GGGCGGTTAAGTCGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1569)
80	THRB	GGGTGGTTAAGTTGAG
	(SEQ ID NO: 106)	(SEQ ID NO: 1570)
81	TIMP3	TTATTAACGGAGGAAGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1571)
82	TIMP3	TATTAATGGAGGAAGGG
	(SEQ ID NO: 103)	(SEQ ID NO: 1572)
83	TIMP3	TTCGTTATGTGTACGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1573)
84	TIMP3	TTTGTTATGTGTATGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1574)
85	TIMP3	TTCGTTATGTGTACGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1573)
86	TIMP3	TTTGTTATGTGTATGGAA
	(SEQ ID NO: 103)	(SEQ ID NO: 1574)
87	TIMP3	GAGTATTTCGAGTTTGT
	(SEQ ID NO: 103)	(SEQ ID NO: 1575)
88	TIMP3	AGTATTTTGAGTTTGTATT
	(SEQ ID NO: 103)	(SEQ ID NO: 1576)
89	TIMP3	TAAGCGTTAATCGAGT
	(SEQ ID NO: 103)	(SEQ ID NO: 1577)
90	TIMP3	TAGGTAAGTGTTAATTGA
	(SEQ ID NO: 103)	(SEQ ID NO: 1578)
91	TP73	TAGGATTCGCGTTTTT
	(SEQ ID NO: 86)	(SEQ ID NO: 1579)
92	TP73	GGTAGGATTTGTGTTTT
	(SEQ ID NO: 86)	(SEQ ID NO: 1580)
93	CDH13	TAGTCGCGTGTATGAA
	(SEQ ID NO: 70)	(SEQ ID NO: 1585)
94	CDH13	TGTAGTTGTGTGTATGA
	(SEQ ID NO: 70)	(SEQ ID NO: 1586)
95	TMS1/ASC	TTCGTTTCGGAGTCGA
	(SEQ ID NO: 84)	(SEQ ID NO: 1591)
96	TMS1/ASC	TTTGTTTTGGAGTTGAT
	(SEQ ID NO: 84)	(SEQ ID NO: 1592)
97	APAF1	GTGTCGTAGCGGTATT
	(SEQ ID NO: 82)	(SEQ ID NO: 1593)
98	APAF1	GGTGTTGTAGTGGTAT
	(SEQ ID NO: 82)	(SEQ ID NO: 1594)
99	APAF1	AGTAGCGTCGGGTTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1595)
100	APAF1	GAGTAGTGTTGGGTTT
	(SEQ ID NO: 82)	(SEQ ID NO: 1596)
101	SYK	GAAGTTATCGCGTTGG
	(SEQ ID NO: 60)	(SEQ ID NO: 1597)
102	SYK	AGAAGTTATTGTGTTGG
	(SEQ ID NO: 60)	(SEQ ID NO: 1598)
103	SYK	GATCGATGCGGTTTAT
	(SEQ ID NO: 60)	(SEQ ID NO: 1599)
104	SYK	GGGATTGATGTGGTTT
	(SEQ ID NO: 60)	(SEQ ID NO: 1600)
105	SYK	TTATTCGGTCGGGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1603)
106	SYK	TTTATTTGGTTGGGATT
	(SEQ ID NO: 60)	(SEQ ID NO: 1604)
107	FABP3	TAAAGCGGTAGTTCGG
	(SEQ ID NO: 77)	(SEQ ID NO: 1609)
108	FABP3	AAGTGGTAGTTTGGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1610)
109	FABP3	TATTGGCGTTGACGTA
	(SEQ ID NO: 77)	(SEQ ID NO: 1611)
110	FABP3	TGGTGTTGATGTAGGT
	(SEQ ID NO: 77)	(SEQ ID NO: 1612)
111	RASSF1A	TACGGGTATTTTCGCGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1613)
112	RASSF1A	ATATGGGTATTTTTGTGT
	(SEQ ID NO: 90)	(SEQ ID NO: 1614)
113	RASSF1A	AGAGCGCGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1615)
114	RASSF1A	GAGAGTGTGTTTAGTTT
	(SEQ ID NO: 90)	(SEQ ID NO: 1616)
115	RASSF1A	AGTAAATCGGATTAGGA
	(SEQ ID NO: 90)	(SEQ ID NO: 1617)
116	RASSF1A	AGTAAATTGGATTAGGAG
	(SEQ ID NO: 90)	(SEQ ID NO: 1618)
117	TWIST	AGTAAAGGCGTTGCGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1619)
118	TWIST	AGTAAAGGTGTTGTGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1620)
119	TWIST	AGTAAAGGCGTTGCGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1619)
120	TWIST	AGTAAAGGTGTTGTGT
	(SEQ ID NO: 100)	(SEQ ID NO: 1620)
121	TWIST	TATTTTTCGAGGCGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1621)
122	TWIST	TTTTGAGGTGTAGTTTT
	(SEQ ID NO: 100)	(SEQ ID NO: 1622)
123	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1623)
124	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1624)
125	TWIST	ATTGGGTCGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1623)
126	TWIST	ATTGGGTTGTTGTAGA
	(SEQ ID NO: 100)	(SEQ ID NO: 1624)
127	TWIST	TAGGTCGGGACGTAAA
	(SEQ ID NO: 100)	(SEQ ID NO: 1625)
128	TWIST	AGTAGGTTGGGATGTA
	(SEQ ID NO: 100)	(SEQ ID NO: 1626)
129	ESR2	ATAAGCGATTTAACGAT
	(SEQ ID NO: 91)	(SEQ ID NO: 1629)
130	ESR2	AAGTGATTTAATGATAAGT
	(SEQ ID NO: 91)	(SEQ ID NO: 1630)
131	PLAU	TATTTGTCGCGTTGAT
	(SEQ ID NO: 62)	(SEQ ID NO: 1633)
132	PLAU	ATTTGTTGTGTTGATGA
	(SEQ ID NO: 62)	(SEQ ID NO: 1634)
133	PLAU	TGTAATTCGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1635)
134	PLAU	TTGTAATTTGGGGATTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1636)
135	PLAU	TTGGAGATCGCGTTTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1637)
136	PLAU	TTGGAGATTGTGTTTTT
	(SEQ ID NO: 62)	(SEQ ID NO: 1638)
137	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1639)
138	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1640)
139	PLAU	GAGCGTTGCGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1639)
140	PLAU	GAGTGTTGTGGAAGTA
	(SEQ ID NO: 62)	(SEQ ID NO: 1640)
141	STAT1	GTTATTTTCGAGAGTTG
	(SEQ ID NO: 109)	(SEQ ID NO: 1641)
142	STAT1	GTTATTTTTGAGAGTTGT
	(SEQ ID NO: 109)	(SEQ ID NO: 1642)
143	LOT1	ATGGGTACGTTTAAGG
	(SEQ ID NO: 95)	(SEQ ID NO: 1649)
144	LOT1	TGGGTATGTTTAAGGG
	(SEQ ID NO: 95)	(SEQ ID NO: 1650)
145	GJB2	GGATTTCGTCGGTATT
	(SEQ ID NO: 111)	(SEQ ID NO: 1667)
146	GJB2	GGGGATTTTGTTGGTA
	(SEQ ID NO: 111)	(SEQ ID NO: 1668)
147	PRDM2	TGTAGAGACGACGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1675)
148	PRDM2	ATTGTAGAGATGATGATT
	(SEQ ID NO: 114)	(SEQ ID NO: 1676)
149	PRDM2	AGAGCGCGGTAGTAGT
	(SEQ ID NO: 114)	(SEQ ID NO: 1677)
150	PRDM2	TGAGAGTGTGGTAGTA
	(SEQ ID NO: 114)	(SEQ ID NO: 1678)
151	PRDM2	TGTTCGCGATGTTTTA
	(SEQ ID NO: 114)	(SEQ ID NO: 1679)
152	PRDM2	TGTTTGTGATGTTTTAGT
	(SEQ ID NO: 114)	(SEQ ID NO: 1680)
153	ALX4	AAGTCGATCGTTTTGT
	(SEQ ID NO: 64)	(SEQ ID NO: 1683)
154	ALX4	TGGAAGTTGATTGTTTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1684)
155	ALX4	ATATCGTTCGGGGGAA
	(SEQ ID NO: 64)	(SEQ ID NO: 2146)
156	ALX4	ATATCGTTCGGGGGAA
	(SEQ ID NO: 64)	(SEQ ID NO: 2146)
157	ALX4	TATTGCGAGGATTCGG
	(SEQ ID NO: 64)	(SEQ ID NO: 1685)
158	ALX4	ATTGTGAGGATTTGGT
	(SEQ ID NO: 64)	(SEQ ID NO: 1686)
159	ALX4	TTCGTAGCGTAGGGTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1687)
160	ALX4	TTTGTAGTGTAGGGTTT
	(SEQ ID NO: 64)	(SEQ ID NO: 1688)
161	IGFBP7	ATTTTTTCGCGGGTAT
	(SEQ ID NO: 94)	(SEQ ID NO: 1710)
162	IGFBP7	TTTTTGTGGGTATTTTAG
	(SEQ ID NO: 94)	(SEQ ID NO: 1711)
163	IGFBP7	GGTATATTCGACGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1712)
164	IGFBP7	GGGTATATTTGATGGGG
	(SEQ ID NO: 94)	(SEQ ID NO: 1713)
165	IGFBP7	GGTACGAGCGTTTTTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1714)
166	IGFBP7	TGGGTATGAGTGTTTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1715)
167	IGFBP7	AAAGCGTATTTAATTCGT
	(SEQ ID NO: 94)	(SEQ ID NO: 1716)
168	IGFBP7	AGTGTATTTAATTTGTGTT
	(SEQ ID NO: 94)	(SEQ ID NO: 1717)
169	NME1	AGTCGAGATTGCGTTA
	(SEQ ID NO: 107)	(SEQ ID NO: 2147)
170	NME1	AGTTGAGATTGTGTTAG
	(SEQ ID NO: 107)	(SEQ ID NO: 2148)
171	NME1	ATCGTTTGAATTCGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2149)
172	NME1	ATTGTTTGAATTTGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2150)
173	NME1	ATCGTTTGAATTCGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2149)
174	NME1	ATTGTTTGAATTTGGGA
	(SEQ ID NO: 107)	(SEQ ID NO: 2150)
175	NME1	AATTCGAGATTAGTTCGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1724)
176	NME1	AATTTGAGATTAGTTTGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1725)
177	NME1	AATTCGAGATTAGTTCGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1724)
178	NME1	AATTTGAGATTAGTTTGG
	(SEQ ID NO: 107)	(SEQ ID NO: 1725)
179	NME1	TTTTAGTACGTTGGAAA
	(SEQ ID NO: 107)	(SEQ ID NO: 2151)
180	NME1	TTAGTATGTTGGAAAGTA
	(SEQ ID NO: 107)	(SEQ ID NO: 2152)
181	THBS1	TAAAGGGGCGTTCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1726)
182	THBS1	AAGGGGTGTTTGTATT
	(SEQ ID NO: 81)	(SEQ ID NO: 1727)
183	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1728)
184	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1729)
185	THBS1	GGTTAGTTCGGGCGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1728)
186	THBS1	GGTTAGTTTGGGTGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1729)
187	THBS1	TTGTGCGTTCGGAGTA
	(SEQ ID NO: 81)	(SEQ ID NO: 1730)
188	THBS1	TGTGTTTGGAGTAGAG
	(SEQ ID NO: 81)	(SEQ ID NO: 1731)
189	IL6	TTCGGTTATACGTAGG
	(SEQ ID NO: 99)	(SEQ ID NO: 1736)
190	IL6	TTTTGGTTATATGTAGGG
	(SEQ ID NO: 99)	(SEQ ID NO: 1737)
191	IL6	AGTTTAGTCGGTTTCGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1738)
192	IL6	AGTTTAGTTGGTTTTGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1739)
193	IL6	AGTTTAGTCGGTTTCGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1738)
194	IL6	AGTTTAGTTGGTTTTGT
	(SEQ ID NO: 99)	(SEQ ID NO: 1739)
195	HOXA5	TAGTTTTCGGTCGGAA
	(SEQ ID NO: 78)	(SEQ ID NO: 1748)
196	HOXA5	TAGTTTTTGGTTGGAAG
	(SEQ ID NO: 78)	(SEQ ID NO: 1749)
197	HOXA5	ATCGGTAGTTGACGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1752)
198	HOXA5	ATTGGTAGTTGATGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1753)
199	HOXA5	ATCGGTAGTTGACGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1752)
200	HOXA5	ATTGGTAGTTGATGGTT
	(SEQ ID NO: 78)	(SEQ ID NO: 1753)
201	GPC3	AATAGTCGCGTTTAGG
	(SEQ ID NO: 118)	(SEQ ID NO: 1760)
202	GPC3	TAGTTGTGTTTAGGGAT
	(SEQ ID NO: 118)	(SEQ ID NO: 1761)
203	CLDN7	TTACGTTAAGTCGGGT
	(SEQ ID NO: 87)	(SEQ ID NO: 1764)
204	CLDN7	AGTTATGTTAAGTTGGG
	(SEQ ID NO: 87)	(SEQ ID NO: 1765)
205	SLIT2	ATTTCGTCGTAGTTTG
	(SEQ ID NO: 112)	(SEQ ID NO: 1774)
206	SLIT2	TTTTGTTGTAGTTTGGA
	(SEQ ID NO: 112)	(SEQ ID NO: 1775)
207	SLIT2	TAGCGGGTTCGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1776)
208	SLIT2	TTAGTGGGTTTGTAGTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1777)
209	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1778)
210	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1779)
211	SLIT2	AAGGCGCGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1778)
212	SLIT2	AAGGTGTGGAAGTTTA
	(SEQ ID NO: 112)	(SEQ ID NO: 1779)
213	IGSF4	AGGTAGATCGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1780)
214	IGSF4	AGGTAGATTGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1781)
215	IGSF4	AGGTAGATCGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1780)
216	IGSF4	AGGTAGATTGAGGAGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1781)
217	IGSF4	TAGTCGTAGAGTCGGG
	(SEQ ID NO: 74)	(SEQ ID NO: 1782)
218	IGSF4	GTTGTAGAGTTGGGTT
	(SEQ ID NO: 74)	(SEQ ID NO: 1783)
219	MCT1	AGTTAGTCGCGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1788)
220	MCT1	AGAGTTAGTTGTGTTTTA
	(SEQ ID NO: 101)	(SEQ ID NO: 1789)
221	SEQ ID NO: 6	AAGTTTATCGGCGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1792)
222	SEQ ID NO: 6	AGAAGTTTATTGGTGTTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1793)
223	SEQ ID NO: 6	ATTTCGGAATTTAAGCGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1794)
224	SEQ ID NO: 6	TTTTGGAATTTAAGTGTT
	(SEQ ID NO: 6)	(SEQ ID NO: 1795)
225	SEQ ID NO: 6	TAATTTCGGACGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1796)
226	SEQ ID NO: 6	TTTTGGATGTGGAGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1797)
227	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1798)
228	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1799)
229	SEQ ID NO: 6	TTACGGTGAAGGCGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1798)
230	SEQ ID NO: 6	TTATGGTGAAGGTGGA
	(SEQ ID NO: 6)	(SEQ ID NO: 1799)
231	SEQ ID NO: 6	TTTCGGTTTTCGTTAAT
	(SEQ ID NO: 6)	(SEQ ID NO: 1800)
232	SEQ ID NO: 6	TTTGGTTTTTGTTAATTTAG
	(SEQ ID NO: 6)	(SEQ ID NO: 1801)
233	SEQ ID NO: 6	TGTGCGAAGTTAACGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1802)
234	SEQ ID NO: 6	TTGTGTGAAGTTAATGT
	(SEQ ID NO: 6)	(SEQ ID NO: 1803)
235	SEQ ID NO: 8	ATAGGGCGGGATTTTA
	(SEQ ID NO: 8)	(SEQ ID NO: 2153)
236	SEQ ID NO: 8	GATAGGGTGGGATTTT
	(SEQ ID NO: 8)	(SEQ ID NO: 2154)
237	SEQ ID NO: 8	ATAAAGCGGGGTTTTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1804)
238	SEQ ID NO: 8	GGATAAAGTGGGGTTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1805)
239	SEQ ID NO: 8	AGGAGGCGAGAAATTT
	(SEQ ID NO: 8)	(SEQ ID NO: 1806)
240	SEQ ID NO: 8	GAGGAGGTGAGAAATT
	(SEQ ID NO: 8)	(SEQ ID NO: 1807)
241	SEQ ID NO: 8	AGAAATTTCGGGGTAG
	(SEQ ID NO: 8)	(SEQ ID NO: 1808)
242	SEQ ID NO: 8	GAAATTTTGGGGTAGTA
	(SEQ ID NO: 8)	(SEQ ID NO: 1809)
243	SEQ ID NO: 8	GGTAGTATCGTTTATAGA
	(SEQ ID NO: 8)	(SEQ ID NO: 1810)
244	SEQ ID NO: 8	GGGGTAGTATTGTTTATA
	(SEQ ID NO: 8)	(SEQ ID NO: 1811)
245	PROSTAGLANDIN E2	AGTGTATCGTTTTTCGG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1812)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
246	PROSTAGLANDIN E2	TAGTGTATTGTTTTTTGG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1813)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
247	PROSTAGLANDIN E2	TGCGTATCGTTAGTTA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1814)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
248	PROSTAGLANDIN E2	AGGTTGTGTATTGTTAG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1815)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
249	PROSTAGLANDIN E2	ATTATTTCGGCGGTGA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1816)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
250	PROSTAGLANDIN E2	GATTATTTTGGTGGTGA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1817)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
251	PROSTAGLANDIN E2	TAAGTCGCGTAAGGAG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1818)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
252	PROSTAGLANDIN E2	AAGTTGTGTAAGGAGTA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1819)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
253	PROSTAGLANDIN E2	GTATCGCGAGTTTGGA
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1820)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
254	PROSTAGLANDIN E2	GTATTGTGAGTTTGGAG
	RECEPTOR, EP4 SUBTYPE	(SEQ ID NO: 1821)
	(PROSTANOID EP4
	RECEPTOR) (PGE
	RECEPTOR, EP4 SUBTYPE)
	(SEQ ID NO: 10)
255	SEQ ID NO: 51	GTCGGGGTCGATTCGA
	(SEQ ID NO: 51)	(SEQ ID NO: 1822)
256	SEQ ID NO: 51	GTTGGGGTTGATTTGAT
	(SEQ ID NO: 51)	(SEQ ID NO: 1823)
257	SEQ ID NO: 51	AGGATTCGTTTGCGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1824)
258	SEQ ID NO: 51	AAGGATTTGTTTGTGTT
	(SEQ ID NO: 51)	(SEQ ID NO: 1825)
259	MGC34831	ATTAGCGTTTGGCGTT
	(SEQ ID NO: 52)	(SEQ ID NO: 1826)
260	MGC34831	AATTAGTGTTTGGTGTT
	(SEQ ID NO: 52)	(SEQ ID NO: 1827)
261	MGC34831	GTTTAGCGACGGTCGT
	(SEQ ID NO: 52)	(SEQ ID NO: 1828)
262	MGC34831	TGTTTAGTGATGGTTGT
	(SEQ ID NO: 52)	(SEQ ID NO: 1829)
263	SEQ ID NO: 54	TGTGTAGCGGCGATTA
	(SEQ ID NO: 54)	(SEQ ID NO: 1830)
264	SEQ ID NO: 54	GTGTGTAGTGGTGATT
	(SEQ ID NO: 54)	(SEQ ID NO: 1831)
265	SEQ ID NO: 54	ATTAGCGTTTGGTCGG
	(SEQ ID NO: 54)	(SEQ ID NO: 1832)
266	SEQ ID NO: 54	ATTAGTGTTTGGTTGGG
	(SEQ ID NO: 54)	(SEQ ID NO: 1833)
267	PDLIM1	TAGGTCGCGTAGTCGT
	(SEQ ID NO: 55)	(SEQ ID NO: 1834)
268	PDLIM1	TTAGGTTGTGTAGTTGT
	(SEQ ID NO: 55)	(SEQ ID NO: 1835)
269	DKK3	ATTCGTTTTAGTTCGAG
	(SEQ ID NO: 24)	(SEQ ID NO: 1842)
270	DKK3	ATTTGTTTTAGTTTGAGT
	(SEQ ID NO: 24)	(SEQ ID NO: 1843)
271	DKK3	TTCGATCGTTTTAGGA
	(SEQ ID NO: 24)	(SEQ ID NO: 1844)
272	DKK3	AGTTTTGATTGTTTTAGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1845)
273	DKK3	ATTCGTTCGGAGACGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1846)
274	DKK3	TTTGTTTGGAGATGGG
	(SEQ ID NO: 24)	(SEQ ID NO: 1847)
275	DKK3	GAAAAGACGCGATTTT
	(SEQ ID NO: 24)	(SEQ ID NO: 1848)
276	DKK3	GAAAAGATGTGATTTTATT
	(SEQ ID NO: 24)	(SEQ ID NO: 1849)
277	SEQ ID NO: 28	TATCGACGTTTTTGGT
	(SEQ ID NO: 28)	(SEQ ID NO: 1850)
278	SEQ ID NO: 28	TATTGATGTTTTTGGTTT
	(SEQ ID NO: 28)	(SEQ ID NO: 1851)
279	SEQ ID NO: 29	TTGATGCGGAGTTCGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1852)
280	SEQ ID NO: 29	TTGATGTGGAGTTTGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1853)
281	SEQ ID NO: 29	TTGATGCGGAGTTCGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1852)
282	SEQ ID NO: 29	TTGATGTGGAGTTTGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1853)
283	SEQ ID NO: 29	TTCGAAGCGTGTATTA
	(SEQ ID NO: 29)	(SEQ ID NO: 2155)
284	SEQ ID NO: 29	GGGTTTGAAGTGTGTA
	(SEQ ID NO: 29)	(SEQ ID NO: 2156)
285	SEQ ID NO: 29	TTTTCGCGTTTGCGAA
	(SEQ ID NO: 29)	(SEQ ID NO: 2157)
286	SEQ ID NO: 29	TTTGTGTTTGTGAAAGG
	(SEQ ID NO: 29)	(SEQ ID NO: 2158)
287	SEQ ID NO: 29	TAGGAACGGTAGGCGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1854)
288	SEQ ID NO: 29	TAGGAATGGTAGGTGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1855)
289	SEQ ID NO: 29	TAGGAACGGTAGGCGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1854)
290	SEQ ID NO: 29	TAGGAATGGTAGGTGG
	(SEQ ID NO: 29)	(SEQ ID NO: 1855)
291	SEQ ID NO: 29	GTCGGAGGCGTTTGAG
	(SEQ ID NO: 29)	(SEQ ID NO: 1856)
292	SEQ ID NO: 29	GTTGGAGGTGTTTGAGA
	(SEQ ID NO: 29)	(SEQ ID NO: 1857)
293	ARL7	TAGATTTCGTAGTTTTTTA
	(SEQ ID NO: 30)	(SEQ ID NO: 1858)
294	ARL7	TAGATTTTGTAGTTTTTTAA
	(SEQ ID NO: 30)	(SEQ ID NO: 1859)
295	ARL7	TGGGTACGTTTACGGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1860)
296	ARL7	TGGGTATGTTTATGGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1861)
297	ARL7	GAAGAAATCGTTTTTGT
	(SEQ ID NO: 30)	(SEQ ID NO: 1862)
298	ARL7	GAAGAAATTGTTTTTGTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1863)
299	ARL7	TAGTAGGATCGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1864)
300	ARL7	ATAGTAGGATTGGTTTTT
	(SEQ ID NO: 30)	(SEQ ID NO: 1865)
301	SEQ ID NO: 31	AACGTTGCGTTGGGTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1866)
302	SEQ ID NO: 31	AATGTTGTGTTGGGTAA
	(SEQ ID NO: 31)	(SEQ ID NO: 1867)
303	SEQ ID NO: 31	TAGCGTTTCGTGGTTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1868)
304	SEQ ID NO: 31	GTAGTGTTTTGTGGTTA
	(SEQ ID NO: 31)	(SEQ ID NO: 1869)
305	THH	TTCGGAAGAAAAGCGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1870)
306	THH	TTTGGAAGAAAAGTGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1871)
307	THH	TTCGGAAGAAAAGCGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1870)
308	THH	TTTGGAAGAAAAGTGAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1871)
309	THH	GTTCGTTGGCGTAAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1872)
310	THH	GGTTTGTTGGTGTAAAT
	(SEQ ID NO: 32)	(SEQ ID NO: 1873)
311	(SEQ ID NO: 36)	TTCGTTGGAGATCGTAA
		(SEQ ID NO: 2159)
312	(SEQ ID NO: 36)	GTTTGTTGGAGATTGTA
		(SEQ ID NO: 2160)
313	(SEQ ID NO: 36)	GGACGTTGCGATTGTA
		(SEQ ID NO: 2161)
314	(SEQ ID NO: 36)	GATGTTGTGATTGTAGT
		(SEQ ID NO: 2162)
315	SENP3	TATTCGGATCGGGTTT
	(SEQ ID NO: 39)	(SEQ ID NO: 1876)
316	SENP3	TTTATTTGGATTGGGTT
	(SEQ ID NO: 39)	(SEQ ID NO: 1877)
317	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1878)
318	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1879)
319	SENP3	TAGTCGAAAGTAGGACGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1878)
320	SENP3	TAGTTGAAAGTAGGATGT
	(SEQ ID NO: 39)	(SEQ ID NO: 1879)
321	SENP3	AGGACGTTTTTGATCGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1880)
322	SENP3	AGGATGTTTTTGATTGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1881)
323	SENP3	AGGACGTTTTTGATCGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1880)
324	SENP3	AGGATGTTTTTGATTGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1881)
325	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1882)
326	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1883)
327	SENP3	AGTTATCGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1882)
328	SENP3	AGTTATTGTTAGGAGGG
	(SEQ ID NO: 39)	(SEQ ID NO: 1883)
329	SEQ ID NO: 42	GAGTCGGGTTGCGATG
	(SEQ ID NO: 42)	(SEQ ID NO: 1884)
330	SEQ ID NO: 42	GGAGTTGGGTTGTGAT
	(SEQ ID NO: 42)	(SEQ ID NO: 1885)
331	SEQ ID NO: 42	ATGGGTTGCGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1886)
332	SEQ ID NO: 42	ATGGGTTGTGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1887)
333	SEQ ID NO: 42	ATGGGTTGCGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1886)
334	SEQ ID NO: 42	ATGGGTTGTGATTTTTA
	(SEQ ID NO: 42)	(SEQ ID NO: 1887)
335	(SEQ ID NO: 117)	TAGCGGTTTTTTAGCGTA
		(SEQ ID NO: 1888)
336	(SEQ ID NO: 117)	AGTGGTTTTTTAGTGTAT
		(SEQ ID NO: 1889)
337	(SEQ ID NO: 117)	AGATGCGCGGGTAGAT
		(SEQ ID NO: 1890)
338	(SEQ ID NO: 117)	AGATGTGTGGGTAGAT
		(SEQ ID NO: 1891)
339	(SEQ ID NO: 117)	AGATGCGCGGGTAGAT
		(SEQ ID NO: 1890)
340	(SEQ ID NO: 117)	AGATGTGTGGGTAGAT
		(SEQ ID NO: 1891)
341	(SEQ ID NO: 117)	AGATAGTTCGTATTCGT
		(SEQ ID NO: 1892)
342	(SEQ ID NO: 117)	GTAGATAGTTTGTATTTGT
		(SEQ ID NO: 1893)
343	(SEQ ID NO: 117)	TTTGTTCGTAACGTTT
		(SEQ ID NO: 1894)
344	(SEQ ID NO: 117)	TGTTTGTAATGTTTAGAG
		(SEQ ID NO: 1895)
345	O60279	TACGTTTTTTCGGATTA
	(SEQ ID NO: 47)	(SEQ ID NO: 1898)
346	O60279	TATGTTTTTTTGGATTAAG
	(SEQ ID NO: 47)	(SEQ ID NO: 1899)
347	O60279	GGACGGCGGAAAATTA
	(SEQ ID NO: 47)	(SEQ ID NO: 1902)
348	O60279	AGGGATGGTGGAAAAT
	(SEQ ID NO: 47)	(SEQ ID NO: 1903)
349	SEQ ID NO: 48	TATTTGGCGATTCGGA
	(SEQ ID NO: 48)	(SEQ ID NO: 1904)
350	SEQ ID NO: 48	TGGTGATTTGGAGATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1905)
351	SEQ ID NO: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1906)
352	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1907)
353	SEQ ID NO: 48	TAGGGTTACGTGTCGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1906)
354	SEQ ID NO: 48	TAGGGTTATGTGTTGG
	(SEQ ID NO: 48)	(SEQ ID NO: 1907)
355	SEQ ID NO: 48	AACGAATTTTTCGATATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1908)
356	SEQ ID NO: 48	TTTAATGAATTTTTTGATATT
	(SEQ ID NO: 48)	(SEQ ID NO: 1909)
357	SEQ ID NO: 48	AAAATCGTATGCGTGT
	(SEQ ID NO: 48)	(SEQ ID NO: 1910)
358	SEQ ID NO: 48	GAAAATTGTATGTGTGTG
	(SEQ ID NO: 48)	(SEQ ID NO: 1911)
359	SEQ ID NO: 9	GTTTCGCGTTTAGGGA
	(SEQ ID NO: 9)	(SEQ ID NO: 1912)
360	SEQ ID NO: 9	GTTTTGTGTTTAGGGAT
	(SEQ ID NO: 9)	(SEQ ID NO: 1913)
361	SEQ ID NO: 9	AGTGTTCGTCGTAGTT
	(SEQ ID NO: 9)	(SEQ ID NO: 1914)
362	SEQ ID NO: 9	TGAGTGTTTGTTGTAGT
	(SEQ ID NO: 9)	(SEQ ID NO: 1915)
363	SEQ ID NO: 9	TTTTGTTCGCGTTGAA
	(SEQ ID NO: 9)	(SEQ ID NO: 1916)
364	SEQ ID NO: 4	TTGTTTGTGTTGAAGTA
	(SEQ ID NO: 4)	(SEQ ID NO: 1917)
365	SEQ ID NO: 4	GGGTCGCGAGGTAGTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1918)
366	SEQ ID NO: 4	TGGGTTGTGAGGTAGT
	(SEQ ID NO: 4)	(SEQ ID NO: 1919)
367	SEQ ID NO: 4	TTTGTGCGACGTTATT
	(SEQ ID NO: 4)	(SEQ ID NO: 1920)
368	SEQ ID NO: 4	GGTTTGTGTGATGTTAT
	(SEQ ID NO: 4)	(SEQ ID NO: 1921)
369	SEQ ID NO: 4	ATGGCGGTTTCGATTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1922)
370	SEQ ID NO: 4	GATGGTGGTTTTGATTT
	(SEQ ID NO: 4)	(SEQ ID NO: 1923)
371	SEQ ID NO: 5	AATGAGCGAGAAAGTA
	(SEQ ID NO: 5)	(SEQ ID NO: 1924)
372	SEQ ID NO: 5	AGAATGAGTGAGAAAGT
	(SEQ ID NO: 5)	(SEQ ID NO: 1925)
373	SEQ ID NO: 5	TATGAGGTCGTATTGG
	(SEQ ID NO: 5)	(SEQ ID NO: 2163)
374	SEQ ID NO: 5	TATGAGGTTGTATTGGT
	(SEQ ID NO: 5)	(SEQ ID NO: 2164)
375	SEQ ID NO: 7	TAGTCGTCGTGTAGGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1932)
376	SEQ ID NO: 7	TAGGTAGTTGTTGTGTA
	(SEQ ID NO: 7)	(SEQ ID NO: 1933)
377	SEQ ID NO: 7	TATAGGTACGCGATGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1934)
378	SEQ ID NO: 7	AGGTATGTGATGAGGA
	(SEQ ID NO: 7)	(SEQ ID NO: 1935)
379	SEQ ID NO: 7	TATGGTTACGTACGAG
	(SEQ ID NO: 7)	(SEQ ID NO: 1936)
380	SEQ ID NO: 7	ATGGTTATGTATGAGTTT
	(SEQ ID NO: 7)	(SEQ ID NO: 1937)
381	SEQ ID NO: 7	ATGATTTGCGTTACGT
	(SEQ ID NO: 7)	(SEQ ID NO: 1938)
382	SEQ ID NO: 7	ATGATTTGTGTTATGTTT
	(SEQ ID NO: 7)	(SEQ ID NO: 1939)
383	SEQ ID NO: 7	TAACGTTGTGGTTCGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1940)
384	SEQ ID NO: 7	TAATGTTGTGGTTTGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1941)
385	SEQ ID NO: 7	TAACGTTGTGGTTCGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1940)
386	SEQ ID NO: 7	TAATGTTGTGGTTTGAA
	(SEQ ID NO: 7)	(SEQ ID NO: 1941)
387	SEQ ID NO: 1	GGTCGGCGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1942)
388	SEQ ID NO: 1	GGTTGGTGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1943)
389	SEQ ID NO: 1	GGTCGGCGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1942)
390	SEQ ID NO: 1	GGTTGGTGTTGATTTTA
	(SEQ ID NO: 1)	(SEQ ID NO: 1943)
391	ORPHAN NUCLEAR	TTACGGAGGCGTTTTA
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1958)
	1-FETOPROTEIN TRANS-
	CRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR)
	(B1-BINDING FACTOR)
	(HB1F) (CYP7A PRO-
	MOTER BINDING FACTOR)
	(SEQ ID NO: 11)
392	ORPHAN NUCLEAR	TTTTATGGAGGTGTTTT
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1959)
	1-FETOPROTEIN TRANS-
	CRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR)
	(B1-BINDING FACTOR)
	(HB1F) (CYP7A PRO-
	MOTER BINDING FACTOR)
	(SEQ ID NO: 11)
393	ORPHAN NUCLEAR	AGGCGAATTTATCGGG
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1960)
	1-FETOPROTEIN TRANS-
	CRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR)
	(B1-BINDING FACTOR)
	(HB1F) (CYP7A PRO-
	MOTER BINDING FACTOR)
	(SEQ ID NO: 11)
394	ORPHAN NUCLEAR	GGTGAATTTATTGGGG
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1961)
	1-FETOPROTEIN TRANS-
	CRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR)
	(B1-BINDING FACTOR)
	(HB1F) (CYP7A PRO-
	MOTER BINDING FACTOR)
	(SEQ ID NO: 11)
395	ORPHAN NUCLEAR	TAGTCGAAGTAGGCGT
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1962)
	1-FETOPROTEIN TRANS-
	CRIPTION FACTOR)
	(HEPATOCYTIC TRANS-
	CRIPTION FACTOR)
	(B1-BINDING FACTOR)
	(HB1F) (CYP7A PRO-
	MOTER BINDING FACTOR)
	(SEQ ID NO: 11)
396	ORPHAN NUCLEAR	TAGTTGAAGTAGGTGTT
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1963)
	1-FETOPROTEIN
	TRANSCRIPTION FACTOR)
	(HEPATOCYTIC
	TRANSCRIPTION FACTOR)
	(B1-BINDING FACTOR)
	(HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
397	ORPHAN NUCLEAR	TTTTCGACGAAGTTTT
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1964)
	1-FETOPROTEIN
	TRANSCRIPTION FACTOR)
	(HEPATOCYTIC
	TRANSCRIPTION FACTOR)
	(B1-BINDING FACTOR)
	(HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
398	ORPHAN NUCLEAR	TTTTGATGAAGTTTTGTT
	RECEPTOR NR5A2 (ALPHA-	(SEQ ID NO: 1965)
	1-FETOPROTEIN
	TRANSCRIPTION FACTOR)
	(HEPATOCYTIC
	TRANSCRIPTION FACTOR)
	(B1-BINDING FACTOR)
	(HB1F) (CYP7A PROMOTER
	BINDING FACTOR)
	(SEQ ID NO: 11)
399	LIM DOMAIN KINASE 1	TGTAGTCGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1966)
	(SEQ ID NO: 12)
400	LIM DOMAIN KINASE 1	TGTAGTTGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1967)
	(SEQ ID NO: 12)
401	LIM DOMAIN KINASE 1	TGTAGTCGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1966)
	(SEQ ID NO: 12)
402	LIM DOMAIN KINASE 1	TGTAGTTGGGAGGTTA
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1967)
	(SEQ ID NO: 12)
403	LIM DOMAIN KINASE 1	GGATTATCGCGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1968)
	(SEQ ID NO: 12)
404	LIM DOMAIN KINASE 1	GGATTATTGTGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1969)
	(SEQ ID NO: 12)
405	LIM DOMAIN KINASE 1	GGATTATCGCGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1968)
	(SEQ ID NO: 12)
406	LIM DOMAIN KINASE 1	GGATTATTGTGGGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1969)
	(SEQ ID NO: 12)
407	LIM DOMAIN KINASE 1	GTCGGTAGTTTATCGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1970)
	(SEQ ID NO: 12)
408	LIM DOMAIN KINASE 1	GTTGGTAGTTTATTGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1971)
	(SEQ ID NO: 12)
409	LIM DOMAIN KINASE 1	GTCGGTAGTTTATCGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1970)
	(SEQ ID NO: 12)
410	LIM DOMAIN KINASE 1	GTTGGTAGTTTATTGGAT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1971)
	(SEQ ID NO: 12)
411	LIM DOMAIN KINASE 1	TAGGAGACGTTACGTT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1972)
	(SEQ ID NO: 12)
412	LIM DOMAIN KINASE 1	AGATGTTATGTTAGGGT
	(EC 2.7.1.37) (LIMK-1)	(SEQ ID NO: 1973)
	(SEQ ID NO: 12)
413	BCL11B	TAGGTTTCGATTCGTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1974)
414	BCL11B	TTAGGTTTTGATTTGTTT
	(SEQ ID NO: 50)	(SEQ ID NO: 1975)
415	BCL11B	AAGTCGTCGGAGTTAG
	(SEQ ID NO: 50)	(SEQ ID NO: 1976)
416	BCL11B	GTGAAGTTGTTGGAGT
	(SEQ ID NO: 50)	(SEQ ID NO: 1977)
417	MSF	GTTTCGAAATTGGCGT
	(SEQ ID NO: 13)	(SEQ ID NO: 1980)
418	MSF	TTTGAAATTGGTGTGG
	(SEQ ID NO: 13)	(SEQ ID NO: 1981)
419	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1982)
420	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1983)
421	MSF	TTCGGTTTACGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1982)
422	MSF	TTTGGTTTATGGGTTGTA
	(SEQ ID NO: 13)	(SEQ ID NO: 1983)
423	MSF	TTACGGTTCGATTTTG
	(SEQ ID NO: 13)	(SEQ ID NO: 1984)
424	MSF	TATGGTTTGATTTTGGG
	(SEQ ID NO: 13)	(SEQ ID NO: 1985)
425	SEQ ID NO: 14	TAAGGCGTTTTCGATA
	(SEQ ID NO: 14)	(SEQ ID NO: 1986)
426	SEQ ID NO: 14	GTAAGGTGTTTTTGATAT
	(SEQ ID NO: 14)	(SEQ ID NO: 1987)
427	SEQ ID NO: 16	AGGAGTTTTCGTGTCGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1992)
428	SEQ ID NO: 16	AGGAGTTTTTGTGTTGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1993)
429	SEQ ID NO: 16	AGGAGTTTTCGTGTCGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1992)
430	SEQ ID NO: 16	AGGAGTTTTTGTGTTGT
	(SEQ ID NO: 16)	(SEQ ID NO: 1993)
431	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1998)
432	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1999)
433	SEQ ID NO: 17	TACGTTTCGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1998)
434	SEQ ID NO: 17	TATGTTTTGGGTTTGTTA
	(SEQ ID NO: 17)	(SEQ ID NO: 1999)
435	SEQ ID NO: 17	ATTTAGTCGTGCGTTT
	(SEQ ID NO: 17)	(SEQ ID NO: 2000)
436	SEQ ID NO: 17	TGATTTAGTTGTGTGTT
	(SEQ ID NO: 17)	(SEQ ID NO: 2001)
437	SEQ ID NO: 18	TTTACGCGGGGTTTTA
	(SEQ ID NO: 18)	(SEQ ID NO: 2002)
438	SEQ ID NO: 18	TTTATGTGGGGTTTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2003)
439	SEQ ID NO: 18	TTACGTCGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2004)
440	SEQ ID NO: 18	TTTTATGTTGTTATTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2005)
441	SEQ ID NO: 18	TATTTGGACGTCGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2006)
442	SEQ ID NO: 18	TATTTGGATGTTGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2007)
443	SEQ ID NO: 18	TATTTGGACGTCGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2006)
444	SEQ ID NO: 18	TATTTGGATGTTGGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2007)
445	SEQ ID NO: 18	AAAGCGGAGTCGTTAG
	(SEQ ID NO: 18)	(SEQ ID NO: 2010)
446	SEQ ID NO: 18	AGTGGAGTTGTTAGGT
	(SEQ ID NO: 18)	(SEQ ID NO: 2011)
447	SEQ ID NO: 19	AGGTTTTCGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2012)
448	SEQ ID NO: 19	TAGGTTTTTGTTGTAGTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2013)
449	SEQ ID NO: 19	TTTGATATCGAGGGAG
	(SEQ ID NO: 19)	(SEQ ID NO: 2165)
450	SEQ ID NO: 19	TTTGATATTGAGGGAGG
	(SEQ ID NO: 19)	(SEQ ID NO: 2166)
451	SEQ ID NO: 19	GGTGTACGGAGGAAAG
	(SEQ ID NO: 19)	(SEQ ID NO: 2167)
452	SEQ ID NO: 19	GGTGTATGGAGGAAAG
	(SEQ ID NO: 19)	(SEQ ID NO: 2168)
453	SEQ ID NO: 19	GGTGTACGGAGGAAAG
	(SEQ ID NO: 19)	(SEQ ID NO: 2167)
454	SEQ ID NO: 19	GGTGTATGGAGGAAAG
	(SEQ ID NO: 19)	(SEQ ID NO: 2168)
455	SEQ ID NO: 19	TGAGATTCGTTTTTTAAA
	(SEQ ID NO: 19)	(SEQ ID NO: 2014)
456	SEQ ID NO: 19	GGTGAGATTTGTTTTTTA
	(SEQ ID NO: 19)	(SEQ ID NO: 2015)
457	PRDM6	TTGTCGGGTTACGGGA
	(SEQ ID NO: 20)	(SEQ ID NO: 2020)
458	PRDM6	GTTGGGTTATGGGAGA
	(SEQ ID NO: 20)	(SEQ ID NO: 2021)
459	PRDM6	TTCGTAGAATTGTCGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2022)
460	PRDM6	TTTGTAGAATTGTTGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2023)
461	PRDM6	TTCGTAGAATTGTCGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2022)
462	PRDM6	TTTGTAGAATTGTTGAAG
	(SEQ ID NO: 20)	(SEQ ID NO: 2023)
463	NR2E1	AATGTAGCGGCGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2028)
464	NR2E1	TAAATGTAGTGGTGTTAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2029)
465	NR2E1	GTCGTTATCGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2030)
466	NR2E1	GTTGTTATTGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2031)
467	NR2E1	GTCGTTATCGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2030)
468	NR2E1	GTTGTTATTGGTTTGGA
	(SEQ ID NO: 22)	(SEQ ID NO: 2031)
469	NR2E1	GACGTAAGTTTCGGGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2032)
470	NR2E1	GGATGTAAGTTTTGGG
	(SEQ ID NO: 22)	(SEQ ID NO: 2033)
471	NR2E1	TTTTTAGTCGCGAGAA
	(SEQ ID NO: 22)	(SEQ ID NO: 2034)
472	NR2E1	TTTTTAGTTGTGAGAAGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2035)
473	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2036)
474	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2037)
475	NR2E1	TTCGGGTGATATCGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2036)
476	NR2E1	TTTGGGTGATATTGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2037)
477	NR2E1	AGGCGAGTCGGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2038)
478	NR2E1	AGGTGAGTTGGAGTTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2039)
479	NR2E1	TAAGTCGAGCGAGTTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2040)
480	NR2E1	TAGTAAGTTGAGTGAGT
	(SEQ ID NO: 22)	(SEQ ID NO: 2041)
481	NR2E1	AGGGACGCGAAAATTT
	(SEQ ID NO: 22)	(SEQ ID NO: 2042)
482	NR2E1	GGAGGGATGTGAAAAT
	(SEQ ID NO: 22)	(SEQ ID NO: 2043)
483	PCDH7	ATCGTAGTCGGTTTTA
	(SEQ ID NO: 23)	(SEQ ID NO: 2044)
484	PCDH7	GATTATTGTAGTTGGTTT
	(SEQ ID NO: 23)	(SEQ ID NO: 2045)
485	RTTN	TAGGACGTGTTTTCGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2048)
486	RTTN	AGGATGTGTTTTTGGG
	(SEQ ID NO: 25)	(SEQ ID NO: 2049)
487	SNAP25	TATTTCGAGTTAGAGTTACGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2050)
488	SNAP25	TATTTTGAGTTAGAGTTATGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2051)
489	SNAP25	TATTTCGAGTTAGAGTTACGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2050)
490	SNAP25	TATTTTGAGTTAGAGTTATGA
	(SEQ ID NO: 33)	(SEQ ID NO: 2051)
491	SNAP25	ATACGGAATATCGTATTT
	(SEQ ID NO: 33)	(SEQ ID NO: 2052)
492	SNAP25	GTGTATATATGGAATATTGT
	(SEQ ID NO: 33)	(SEQ ID NO: 2053)
493	SNAP25	GTTATTATTCGGTACGT
	(SEQ ID NO: 33)	(SEQ ID NO: 2169)
494	SNAP25	AGTTATTATTTGGTATGTAT
	(SEQ ID NO: 33)	(SEQ ID NO: 2170)
495	SEQ ID NO: 26	TTAAGTATCGAGGCGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2054)
496	SEQ ID NO: 26	TTTTAAGTATTGAGGTGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2055)
497	SEQ ID NO: 26	AATTTTGGTCGTTTAGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2056)
498	SEQ ID NO: 26	AAATTTTGGTTGTTTAGT
	(SEQ ID NO: 26)	(SEQ ID NO: 2057)
499	GIRK2	AGTTGTTCGTAGGCGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2060)
500	GIRK2	AGTTGTTTGTAGGTGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2061)
501	GIRK2	AGTTGTTCGTAGGCGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2060)
502	GIRK2	AGTTGTTTGTAGGTGA
	(SEQ ID NO: 27)	(SEQ ID NO: 2061)
503	GIRK2	TTATTTCGTTCGTAGTT
	(SEQ ID NO: 27)	(SEQ ID NO: 2062)
504	GIRK2	TTTGTTTGTAGTTAGGTA
	(SEQ ID NO: 27)	(SEQ ID NO: 2063)
505	GIRK2	TTAGTCGAAAGGCGAG
	(SEQ ID NO: 27)	(SEQ ID NO: 2064)
506	GIRK2	TAGTTGAAAGGTGAGG
	(SEQ ID NO: 27)	(SEQ ID NO: 2065)
507	SEQ ID NO: 28	ATTAGGCGAGTTTCGT
	(SEQ ID NO: 28)	(SEQ ID NO: 2066)
508	SEQ ID NO: 28	TTAGGTGAGTTTTGTTT
	(SEQ ID NO: 28)	(SEQ ID NO: 2067)
509	SEQ ID NO: 31	TTTACGTAGGGCGATT
	(SEQ ID NO: 31)	(SEQ ID NO: 2068)
510	SEQ ID NO: 31	ATTTTTATGTAGGGTGAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2069)
511	SEQ ID NO: 31	GATACGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2070)
512	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2071)
513	SEQ ID NO: 31	GATACGGTTAGGCGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2070)
514	SEQ ID NO: 31	GATATGGTTAGGTGGG
	(SEQ ID NO: 31)	(SEQ ID NO: 2071)
515	SEQ ID NO: 31	TTCGGGCGTTTTATAT
	(SEQ ID NO: 31)	(SEQ ID NO: 2072)
516	SEQ ID NO: 31	GGTTTGGGTGTTTTATA
	(SEQ ID NO: 31)	(SEQ ID NO: 2073)
517	HOXB13	GTCGTTATTATTTCGAGG
	(SEQ ID NO: 34)	(SEQ ID NO: 2074)
518	HOXB13	GTTGTTATTATTTTGAGGA
	(SEQ ID NO: 34)	(SEQ ID NO: 2075)
519	HOXB13	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2076)
520	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2077)
521	HOXB13	AAGTTAGCGGGTTCGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2076)
522	HOXB13	AAGTTAGTGGGTTTGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2077)
523	HOXB13	TTGGTCGCGTAGTAAA
	(SEQ ID NO: 34)	(SEQ ID NO: 2078)
524	HOXB13	TGGTTGTGTAGTAAAGT
	(SEQ ID NO: 34)	(SEQ ID NO: 2079)
525	(SEQ ID NO: 35)	AAATAGTCGTTTGGGA
		(SEQ ID NO: 2082)
526	(SEQ ID NO: 35)	AAATAGTTGTTTGGGAG
		(SEQ ID NO: 2083)
527	(SEQ ID NO: 35)	TAAAGACGGGAAGAGA
		(SEQ ID NO: 2086)
528	(SEQ ID NO: 35)	ATAAAGATGGGAAGAGA
		(SEQ ID NO: 2087)
529	MGC10561	ATATTTAGCGTAGTTATTT
	(SEQ ID NO: 37)	(SEQ ID NO: 2171)
530	MGC10561	TAGTATATTTAGTGTAGTTAT
	(SEQ ID NO: 37)	(SEQ ID NO: 2172)
531	LMX1A	GTCGGGTTTTTCGGAA
	(SEQ ID NO: 38)	(SEQ ID NO: 2092)
532	LMX1A	GTTGGGTTTTTTGGAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2093)
533	LMX1A	GTCGAGATTTTATCGAAA
	(SEQ ID NO: 38)	(SEQ ID NO: 2094)
534	LMX1A	GTTGAGATTTTATTGAAAG
	(SEQ ID NO: 38)	(SEQ ID NO: 2095)
535	LMX1A	AGTATTCGGGCGGGTA
	(SEQ ID NO: 38)	(SEQ ID NO: 2096)
536	LMX1A	GTAGTATTTGGGTGGG
	(SEQ ID NO: 38)	(SEQ ID NO: 2097)
537	LMX1A	AACGAAATTACGTGTAT
	(SEQ ID NO: 38)	(SEQ ID NO: 2098)
538	LMX1A	TGAAATGAAATTATGTGTA
	(SEQ ID NO: 38)	(SEQ ID NO: 2099)
539	GS1	TGCGAGTTAGCGGTTA
	(SEQ ID NO: 40)	(SEQ ID NO: 2100)
540	GS1	TTGTGAGTTAGTGGTT
	(SEQ ID NO: 40)	(SEQ ID NO: 2101)
541	TITF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2104)
542	TITF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2105)
543	TITF1	GTCGTGGGGATCGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2104)
544	TITF1	GTTGTGGGGATTGTAT
	(SEQ ID NO: 41)	(SEQ ID NO: 2105)
545	TITF1	GGTTCGTTTAAGTTCGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2106)
546	TITF1	GGTTTGTTTAAGTTTGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2107)
547	TITF1	GGTTCGTTTAAGTTCGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2106)
548	TITF1	GGTTTGTTTAAGTTTGG
	(SEQ ID NO: 41)	(SEQ ID NO: 2107)
549	TITF1	TTAGGTCGCGTTTGTA
	(SEQ ID NO: 41)	(SEQ ID NO: 2108)
550	TITF1	AGGTTGTGTTTGTAGA
	(SEQ ID NO: 41)	(SEQ ID NO: 2109)
551	TITF1	TATTTCGTTTTCGTAATT
	(SEQ ID NO: 41)	(SEQ ID NO: 2110)
552	TITF1	TTTGTTTTTGTAATTAGATT
	(SEQ ID NO: 41)	(SEQ ID NO: 2111)
553	DDX51	TAGGCGAGCGTTAGGT
	(SEQ ID NO: 43)	(SEQ ID NO: 2173)
554	DDX51	GGTGAGTGTTAGGTTA
	(SEQ ID NO: 43)	(SEQ ID NO: 2174)
555	DDX51	AACGTGCGGGGTTTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2116)
556	DDX51	TGAATGTGTGGGGTTT
	(SEQ ID NO: 43)	(SEQ ID NO: 2117)
557	SEQ ID NO: 45	TGTAGTATCGGGGGAG
	(SEQ ID NO: 45)	(SEQ ID NO: 2175)
558	SEQ ID NO: 45	TGTAGTATTGGGGGAG
	(SEQ ID NO: 45)	(SEQ ID NO: 2176)
559	SEQ ID NO: 45	TGTAGTATCGGGGGAG
	(SEQ ID NO: 45)	(SEQ ID NO: 2175)
560	SEQ ID NO: 45	TGTAGTATTGGGGGAG
	(SEQ ID NO: 45)	(SEQ ID NO: 2176)
561	SEQ ID NO: 45	GAGTCGGGTTATCGTT
	(SEQ ID NO: 45)	(SEQ ID NO: 2120)
562	SEQ ID NO: 45	GGAGTTGGGTTATTGT
	(SEQ ID NO: 45)	(SEQ ID NO: 2121)
563	SEQ ID NO: 45	TTACGGATGTTTCGGT
	(SEQ ID NO: 45)	(SEQ ID NO: 2122)
564	SEQ ID NO: 45	TTTATGGATGTTTTGGT
	(SEQ ID NO: 45)	(SEQ ID NO: 2123)
565	SEQ ID NO: 45	TGACGTATTTTCGGTT
	(SEQ ID NO: 45)	(SEQ ID NO: 2124)
566	SEQ ID NO: 46	GGTGATGTATTTTTGGT
	(SEQ ID NO: 46)	(SEQ ID NO: 2125)
567	SEQ ID NO: 46	ATAGTCGGAATCGTTG
	(SEQ ID NO: 46)	(SEQ ID NO: 2126)
568	SEQ ID NO: 46	TAGTTGGAATTGTTGTT
	(SEQ ID NO: 46)	(SEQ ID NO: 2127)
569	SEQ ID NO: 2	ATTGGGTTTCGCGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2128)
570	SEQ ID NO: 2	ATTGGGTTTTGTGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2129)
571	SEQ ID NO: 2	ATTGGGTTTCGCGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2128)
572	SEQ ID NO: 2	ATTGGGTTTTGTGTAGG
	(SEQ ID NO: 2)	(SEQ ID NO: 2129)
573	SEQ ID NO: 2	TAGTAGTCGGCGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2130)
574	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2131)
575	SEQ ID NO: 2	TAGTAGTCGGCGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2130)
576	SEQ ID NO: 2	TAGTAGTTGGTGGGAG
	(SEQ ID NO: 2)	(SEQ ID NO: 2131)
577	SEQ ID NO: 3	TTCGCGTTAATTCGGTA
	(SEQ ID NO: 3)	(SEQ ID NO: 2132)
578	SEQ ID NO: 3	AATTTGTGTTAATTTGGT
	(SEQ ID NO: 3)	(SEQ ID NO: 2133)
579	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2134)
580	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2135)
581	SEQ ID NO: 3	AGTCGGGAGAGCGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2134)
582	SEQ ID NO: 3	AGTTGGGAGAGTGAAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2135)
583	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2136)
584	SEQ ID NO: 3	GGTTGAAGAGTTGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2137)
585	SEQ ID NO: 3	GGTCGAAGAGTCGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2136)
586	SEQ ID NO: 3	GGTTGAAGAGTTGGGA
	(SEQ ID NO: 3)	(SEQ ID NO: 2137)
587	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2138)
588	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2139)
589	SEQ ID NO: 3	ATGTTAGCGGGTCGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2138)
590	SEQ ID NO: 3	ATGTTAGTGGGTTGAA
	(SEQ ID NO: 3)	(SEQ ID NO: 2139)

TABLE 21
							% of
					Syber	% of	samples
					green	samples	methylated
Genomic	Primer	Primer			detection	methylated	(Syber
SEQ ID	SEQ ID	SEQ ID	Probe SEQ	Syber	Temperatire	(Probe	green
NO:	NO:	NO:	ID NO:	green	° C.	detection)	detection)
20	2223	2224	2225	No		91
24	2226	2227	2228	Yes	85° C.	30	30
13	2229	2230		Yes	81° C.		36
13	2239	2240	2241			47
15	2231	2232	2233	No		40
22	2233	2234		Yes	81° C.		72
22	2236	2237	2238			68

TABLE 22
Primers and oligonucleotides according to Example 2
Genomic
SEQ ID NO:	Assay	Primer 1	Primer 2	Probe 1	Probe 2	Blocker
SEQ ID	MSP	CGcacttaaaata	tgttgtgttaCGa	cgtagggtcgtgc
NO: 104		aaaacactaCG	ggtggattC	gggatcg
(Assay 4)		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
		2242	2243	2244
SEQ ID	MSP	CCACCTCGATAAA	AGTAGGCGTGTAA	CGGCGGTTTTTTG
NO: 77		TTAAAAAATAAAC	GGGTTTC	TTCGGGTTGTC
(Assay 1-5)		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
		2245	2246	2247
SEQ ID	MSP	CCCGACTAAAACG	TTTTAGATGAAGT	CGTGTGCGTGGCG
NO: 90		TACCAAC	CGTTATAGAGGTC	GGTTTC
(Assay 1		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
		2248	2249	2250
SEQ ID	MSP	cggttgttgtagg	gcaaaacacacga	Cgcgtgtgtaggt
NO: 4		cgtc	aaacg	cgcgcgt
(Assay 1)		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
		2251	2252	2253
SEQ ID	MSP	AAAATCCTCTCCA	CGCGATTCGTTGT	CGGATTTCGCGGT
NO: 13		ACACGTC	TTATTAG	TAACGCGTAGTT
(Assay 2)		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
		2256	2257	2258
SEQ ID	Heavy-	CCAAAACCTAAAC	GGAAATTTGAGGG	GGCGATCGAGGCG	Red640GCGGGTG	TACAACACCACCA
NO: 15	Metal	TTACAAC	GTAA	TCGT-fluo	GGGAGCGAG-pho	ACAAACCCAAAAA
(Assay 5)		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:	SEQ ID NO:	CACAA-pho
		2259	2260	2261	2262	SEQ ID NO:
						2263
SEQ ID	MSP	CTACCTCCACCGC	AAGCGTTTTTTAG	TACGTCGTTGCGC
NO: 20		GAC	AGCGC	GTTTTTGTGC
(Assay o)		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
		2264	2265	2266
SEQ ID	MSP	TGTTATTTAGACG	ATCTATCCGTCAA	CGTTTTTCGCGGT
NO: 38		TTTACGAATAAGT	TACTTATAAATCG	TTTGGGGAATTC
(Assay 3)		TC	SEQ ID NO:	SEQ ID NO:
		SEQ ID NO:	2268	2269
		2267
SEQ ID	MSP	AcaccCGtaaact	AtttttagCGagt	Cggtaagcgttcg
NO: 3		ccttCG	CGagttttC	aaatcgggt
(Assay 8)		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
		2270	2271	2272
SEQ ID	MSP	Aaatacaaaaacg	Gaggcgtttgaga	GCGgaaCGgCGCG
NO: 29		aaaaaccg	gattttc	tga
(Assay 2)		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
		2273	2274	2275
SEQ ID	MSP	Ggcgagggaagtt	Catttaacaaacc	Ttttaggaaattt
NO: 22		aagaac	gaacga	cggttcgttttac
(Assay o)		SEQ ID NO:	SEQ ID NO:	gtcgg
		2276	2277	SEQ ID NO:
				2278
SEQ ID	MSP	Aaggatttgggat	Ccgccctcctaaa	Cgtaggtagcggc
NO: 115		ttacgatc	actctac	gggggcg
(Assay 1)		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
		2279	2280	2281
SEQ ID	MSP	Aaactccgaaaac	Agtgagtagagtt	CGCGttCGtttCG
NO: 112		taaaaaacg	tagagtcgtgc	tgtattttCGC
(Assay 2-2)		SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
		2282	2283	2284
SEQ ID	HM	Cacaaactatcta	Gattgttgttggt	TCgTCTCTTAAAC	Red640-CCTCAA	ctcaaacacaaaa
NO: 6		taaaaaattaatc	gtttgttatt	CgCTTTCgA-	AATAAACACgAAC	aaattaacatctc
(Assay 5)		tc	SEQ ID NO:	fluo	ATACCC-pho	atctcttaaacca
		SEQ ID NO:	2286	SEQ ID NO:	SEQ ID NO:	ctttcaat-pho
		2285		2287	2288	SEQ ID NO:
						2297
SEQ ID	MSP	Ttaaaactaaacg	Ggaggttagttat	CgtttagCGtttg
NO: 98		accaaaaacg	tttcggagtc	gggaCGtCGattt
(Assay 2)		SEQ ID NO:	SEQ ID NO:	C
		2289	2290	SEQ ID NO:
				2291
SEQ ID	HM	Tttggagaaagag	Aaaatcaaaaatt	Cggaattgtagag	red640-gttttt	Acctcccaccctc
NO: 22		ggat	acacctc	cgtcggtta-	tttttcgcgaacg	cactcaacattc
(Assay 2)		SEQ ID NO:	SEQ ID NO:	fluo	tcg-ph	a-ph
		2292	2293	SEQ ID NO:	SEQ ID NO:	SEQ ID NO:
				2294	2295	2296

TABLE 23
Genomic	Figure		Sensi-	Speci-	Wilcoxon
SEQ ID NO:	number	AUC	tivity	ficity	p-value
SEQ ID NO:	6	0.62	0.29	0.9	0.2664
104 (Assay 4)		(0.41, 0.81)
SEQ ID NO:	5	0.93	0.93	0.9	1e−04
77 (Assay 1-5)		(0.73, 0.99)
SEQ ID NO:	4	0.9	1	0.9	8e−04
90 (Assay 1)		(0.73, 0.99)
SEQ ID NO:	9	0.96	0.93	1	1e−04
13 (Assay 2)		(0.79, 1)
SEQ ID NO:	8	1	1	0.9	0
20 (Assay o)		(0.86,1)
SEQ ID NO:	7	1	1	0.9	0
38 (Assay 3)		(0.86, 1)
SEQ ID NO:	1	0.95	0.93	0.9	2e−04
4 (Assay 1)		(0.79, 1)
SEQ ID NO:	3	0.91	0.93	0.9	4e−04
29 (Assay 2)		(0.73, 0.99)
SEQ ID NO:	12	0.95	0.93	0.9	2e−04
115 (Assay 1)		(0.79, 1)
SEQ ID NO:	10	0.93	0.86	0.9	5e−04
112 (Assay 2-2-5)		(0.73, 0.99)
SEQ ID NO:	11	0.89	0.86	0.9	0.0011
98 (Assay 2)		(0.68, 0.97)
SEQ ID NO:	2	0.99	0.93	0.9	1e−04
22 (Assay o)		(0.8, 1)

TABLE 24
Assay performance in Other cancer vs. Breast cancer detection
Genomic	Figure		Sensi-	Speci-	Wilcoxon
SEQ ID NO:	Number	AUC	tivity	ficity	p-value
SEQ ID NO:	16	0.75	0.67	0.88	8e−04
104 (Assay 4)		(0.6, 0.86)
SEQ ID NO:	17	0.44	0	0.88	0.516
77 (Assay 1-5)		(0.29, 0.59)
SEQ ID NO:	13	0.8	0.54	o.88	4e−04
90 (Assay 1)		(0.65, 0.9)
SEQ ID NO:	15	0.66	0.29	0.92	0.1239
13 (Assay 2)		(0.49, 0.81)
SEQ ID NO:	18	0.65	0.25	0.88	0.0852
20 (Assay o)		(0,49, 0.78)
SEQ ID NO:	14	0.79	0.54	0.88	4e−04
38 (Assay 3)		(0.65, 0.9)

TABLE 25
Patient samples according to Example 1
Sub Diagnosis                # used
Early sporadic breast cancer 259
IDCT1N0postET+               24
IDCT1N0postER−               25
IDCT1N0preER+                24
IDCT1N0preER−                24
IDCT1N12postER+              27
IDCT1N12postER−              24
IDCT1N12preER+               24
IDCT1N12preER−               24
ILC caucasian ER+ T1N0       16
ILC caucasian ER+ T1N12      8
DCIS caucasian ER+/−         39
genetic breast cancer        23
BRCA1                        23
Benign breast conditions     84
fibroadenoma                 45
fibrocystic disease          6
ductal hyperplasia           3
normal breast epithelium     12
normal breast tissue         18
Other cancers                75
colon                        13
lung                         19
endometrial                  16
ovarian                      16
others                       11
Lymphocyte controls          34
age group old                13
age group young              13
male controls                8
Total                        475

TABLE 26
		Sense	Antisense	Sense	Antisense
		methyl-	methyl-	unmethyl-	unmethyl-
		ated	ated	ated	ated
	Genomic	converted	converted	converted	converted
	SEQ ID	SEQ ID	SEQ ID	SEQ ID	SEQ ID
Gene	NO:	NO:	NO:	NO:	NO:
Genomic	4	499	500	735	736
region
Genomic	7	505	506	741	742
region
Genomic	9	509	510	745	746
region
ORPHAN	11	513	514	749	750
NUCLEAR
RECEPTOR
NR5A2
Genomic	14	519	520	755	756
region
Genomic	16	523	524	759	760
region
Genomic	17	525	526	761	762
region
Genomic	19	529	530	765	766
region
PRDM6	20	531	532	767	768
DKK3	24	539	540	775	776
GIRK2	27	545	546	781	782
Genomic	28	547	548	783	784
region
Genomic	29	549	550	785	786
region
Genomic	36	563	564	799	800
region
GS1	40	571	572	807	808
SEQ ID	42	575	576	811	812
NO: 42
DDX51	43	577	578	813	814
Genomic	46	583	584	819	820
region
Genomic	48	587	588	823	824
region
BCL11B	50	591	592	827	828
Genomic	51	593	594	829	830
region
MGC34831	52	595	596	831	832
CDKN2A	57	605	606	841	842
APC	65	621	622	857	858
SERPINB5	68	627	628	863	864
CASP8	71	633	634	869	870
SNCG	73	637	638	873	874
ESR1	75	641	642	877	878
FABP3	77	645	646	881	882
PGR	83	657	658	893	894
TP73	86	663	664	899	900
RARB	88	667	668	903	904
MLH1	89	669	670	905	906
ESR2	91	673	674	909	910
TERT	92	675	676	911	912
TGFBR2	93	677	678	913	914
S100A7	96	683	684	919	920
DAPK1	98	687	688	923	924
MCT1	101	693	694	929	930
SASH1	102	695	696	931	932
SOD2	105	701	702	937	938
NME1	107	705	706	941	942
RARA	108	707	708	943	944
GJB2	111	713	714	949	950
HS3ST2	113	717	718	953	954
SLC19A1	116	723	724	959	960
Genomic	117	725	726	961	962
region

	TABLE 21
	BC vs. Benign		BC vs. Other cancer
SEQ ID		p-value		p-value
NO:	Accuracy	(corrected)	Accuracy	(corrected)
4	0.77	2.49E−20	0.55	1.00E+00
7	0.84	5.86E−28	0.61	1.57E−01
9	0.64	2.80E−05	0.56	1.00E+00
11	0.69	1.03E−12	0.56	1.00E+00
14	0.60	8.55E−06	0.48	1.00E+00
16	0.75	2.69E−16	0.58	4.89E−01
17	0.64	6.32E−06	0.61	4.41E−01
19	0.60	6.64E−05	0.55	3.37E−01
20	0.56	3.84E−02	0.60	4.26E−01
24	0.61	1.05E−08	0.48	1.00E+00
27	0.80	4.30E−27	0.62	7.44E−02
28	0.60	6.52E−03	0.59	9.95E−02
29	0.69	2.23E−13	0.59	4.16E−01
36	0.58	2.17E−02	0.54	1.00E+00
40	0.61	1.73E−04	0.54	1.00E+00
42	0.75	5.03E−15	0.63	1.65E−01
43	0.73	1.93E−13	0.54	1.00E+00
46	0.82	3.46E−30	0.54	3.63E−01
48	0.73	4.18E−11	0.69	5.18E−02
50	0.63	4.27E−10	0.47	1.00E+00
51	0.73	9.83E−20	0.55	1.00E+00
52	0.69	2.04E−05	0.48	1.00E+00
57	0.67	7.94E−14	0.49	1.00E+00
65	0.73	4.18E−16	0.58	1.00E+00
68	0.70	7.48E−10	0.67	1.98E−01
71	0.61	8.85E−06	0.53	1.00E+00
73	0.68	1.01E−10	0.57	1.00E+00
75	0.69	2.35E−06	0.60	1.00E+00
77	0.69	8.14E−12	0.50	1.00E+00
83	0.64	1.47E−04	0.65	8.17E−02
86	0.63	4.12E−03	0.48	1.00E+00
88	0.60	5.10E−08	0.58	1.00E+00
89	0.54	1.10E−04	0.56	1.00E+00
91	0.55	7.72E−05	0.40	2.15E−01
92	0.66	1.26E−03	0.55	1.00E+00
93	0.62	7.19E−08	0.61	1.00E+00
96	0.69	7.22E−11	0.57	1.00E+00
98	0.68	1.08E−04	0.60	1.00E+00
101	0.72	8.66E−08	0.71	5.95E−01
102	0.66	−4.41E−07	0.55	1.00E+00
105	0.67	2.49E−07	0.59	1.00E+00
107	0.58	9.74E−05	0.59	1.28E−01
108	0.62	6.51E−06	0.44	1.00E+00
111	0.68	5.59E−14	0.54	6.62E−01
113	0.85	2.66E−31	0.75	6.54E−01
116	0.65	1.52E−08	0.46	1.00E+00
117	0.86	1.32E−37	0.54	1.00E+00

Claims

1. A method for detecting breast cell proliferative disorders in a human subject, comprising: determining the CpG methylation status of LMX1A (SEQ ID NO: 38) in a sample from the subject containing breast cells, breast fluid or breast tissue; andcomparing the CpG methylation status in the sample with CpG methylation from a normal subject not having a breast cell proliferative disorder, wherein a difference in the CpG methylation status is indicative of a breast cell proliferative disorder.

2. The method according to claim 1, comprising contacting genomic DNA isolated from a biological sample obtained from the subject, with at least one reagent that distinguishes between methylated and non-methylated CpG dinucleotides within one or more of the target nucleic acids.

3. A method for detecting breast cell proliferative disorders in human a subject, comprising: i) obtaining, from the subject, a biological sample containing genomic DNA from breast cells, breast fluid or breast tissue;ii) contacting the genomic DNA, or a fragment thereof, with at least one reagent or for distinguishing between methylated and non-methylated CpG dinucleotide sequences;iii) amplifying at least one target sequence of the DNA by means of at least one primer pair, wherein the sequences are reverse complementary, identical, or hybridize under stringent or highly stringent conditions to an at least 16-base-pair long segment of a base sequence selected from the group consisting SEQ ID NOS: 38, 567, 568, 803, 804, and sequences complementary thereto;iv) determining the CpG methylation status of SEQ ID NO: 38, or an average, or a value reflecting an average methylation status of a plurality of target CpG dinucleotide sequences within SEQ ID NO:38; andv) comparing the CpG methylation status in the sample with CpG methylation from a normal subject not having a breast cell proliferative disorder, wherein a difference in the CpG methylation status is indicative of a breast cell proliferative disorder.

4. The method of claim 3, wherein the reagent of ii) is selected from the group consisting of bisulfite, hydrogen sulfite, disulfite, and combinations thereof.

5. The method of claim 3, wherein the biological sample is selected form the group consisting of nipple aspirate fluid, lymphatic fluid, ductal lavage fluid, fine needle aspirate, blood plasma, blood serum, whole blood, isolated blood cells, and cells isolated from the blood.

6. The method of claim 3, comprising use of at least one nucleic acid molecule or peptide nucleic acid (PNA) molecule comprising, in each case a contiguous sequence at least 9 nucleotides in length that is complementary to, or hybridizes under moderately stringent or stringent conditions to a sequence selected from the group consisting of SEQ ID NOS: 38, 567, 568, 803, and 804.

7. The method of claim 3, wherein amplifying in iii) comprises use of at least one method selected from the group consisting of: use of a heat-resistant DNA polymerase as the amplification enzyme; use of a polymerase lacking 5′-3′ exonuclease activity; use of a polymerase chain reaction (PCR); generation of a amplificate nucleic acid molecule carrying a detectable label; and combinations thereof.

8. The method of claim 3, wherein amplifying in iii) comprises use of methylation specific primers.

9. The method according to claim 3, further comprising in iii) the use of at least one nucleic acid molecule or peptide nucleic acid molecule comprising in each case a contiguous sequence at least 9 nucleotides in length that is complementary to, or hybridizes under moderately stringent or stringent conditions to a sequence selected from the group consisting of SEQ ID NOS: 38, 567, 568, 803, 804 and complements thereof, wherein said nucleic acid molecule or peptide nucleic acid molecule suppresses amplification of the nucleic acid to which it is hybridized.

10. The method according to claim 3, wherein determining in iv) comprises hybridization of at least one nucleic acid molecule or peptide nucleic acid molecule in each case comprising a contiguous sequence at least 9 nucleotides in length that is complementary to, or hybridizes under moderately stringent or stringent conditions to a sequence selected from the group consisting of SEQ ID NOS: 38, 567, 568, 803, 804, and complements thereof.

11. The method of claim 3, wherein determining in iv), comprises sequencing of the amplificate.