COMPOSITIONS AND METHODS FOR INHIBITING LPA EXPRESSION

TECHNICAL FIELD

The disclosure relates to oligonucleotides that inhibit apolipoprotein(a) (“LPA”) expression and uses thereof, particularly uses relating to treating diseases, disorders and/or conditions associated with LPA expression.

REFERENCE TO SEQUENCE LISTING

A Sequence Listing is submitted concurrently with the specification as an ASCII formatted text file, with a file name of DRNA_C002WO_ST25.txt, a creation date of Aug. 5, 2021, and a size of 238 kilobytes. The information in the electronic format of the Sequence Listing is part of the specification and is hereby incorporated herein by reference in its entirety.

BACKGROUND

Lipoprotein(a) (Lp(a)) is a heterogeneous low density lipoprotein (LDL)-like particle containing a lipid core and apolipoprotein B (apoB-100) with a unique constituent, apolipoprotein (a) (apo(a)), that is attached to apoB-100 through a disulfide bond. The apo(a) gene (LPA) is expressed predominantly in the liver and expression is restricted to human and non-human primates. Lp(a) levels in humans are genetically defined and do not change significantly with diet, exercise, or other lifestyle changes. LPA varies in length depending upon the number of Kringle KIV2 domains present and its expression is inversely correlated with the number of domains present. Normal Lp(a) levels range from 0.1-25 mg/dl, with about 25% of the population in the United States of America having Lp(a) levels of 30 mg/dl or higher. Analysis of Lp(a) levels in multiple studies have implicated high Lp(a) levels as an independent risk factor for cardiovascular disease, stroke, and other related disorders including atherosclerotic stenosis. In addition, genome-wide association analyses have also implicated LPA as a genetic risk factor for diseases such as atherosclerotic stenosis. When therapeutic lipoprotein apheresis is used to lower both Lp(a) and LDL levels in hyperlipidemic patients, significant reductions of cardiovascular events have been observed.

Therefore, there exists a need for therapeutics and treatments related to these and other LPA-related diseases.

BRIEF SUMMARY OF THE INVENTION

Embodiments of the disclosure relate to compositions and methods for treating a disease, disorder and/or condition related to LPA expression. The disclosure is based, in part, on the discovery and development of oligonucleotides that selectively inhibit and/or reduce LPA expression in the liver. Accordingly, target sequences within LPA mRNA were identified and RNAi oligonucleotides that bind to these target sequences and inhibit LPA mRNA expression were generated. As demonstrated herein, the RNAi oligonucleotides inhibited monkey and human LPA expression in the liver. Without being bound by theory, the RNAi oligonucleotides described herein are useful for treating a disease, disorder or condition associated with LPA expression (e.g., cardiometabolic diseases, atherosclerosis, dyslipidemia, NAFLD and NASH).

Accordingly, in some embodiments, the present disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand and an antisense strand, wherein the sense strand and the antisense strand form a duplex region, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is at least 15 contiguous nucleotides in length.

In any of the foregoing or related embodiments, the sense strand is 15 to 50 nucleotides in length. In some embodiments, the sense strand is 18 to 36 nucleotides in length.

In any of the foregoing or related aspects, the antisense strand is 15 to 30 nucleotides in length.

In any of the foregoing or related aspects, the antisense strand is 22 nucleotides in length and wherein antisense strand and the sense strand form a duplex region of at least 19 nucleotides in length, optionally at least 20 nucleotides in length.

In any of the foregoing or related aspects, the region of complementarity is at least 19 contiguous nucleotides in length, optionally at least 20 nucleotides in length.

In any of the foregoing or related aspects, the 3′ end of the sense strand comprises a stem-loop set forth as S1-L-S2, wherein S1 is complementary to S2, and wherein L forms a loop between S1 and S2 of 3-5 nucleotides in length.

In some aspects, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand of 15 to 50 nucleotides in length and an antisense strand, wherein the sense strand and the antisense strand form a duplex region, wherein the wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is at least 15 contiguous nucleotides in length.

In other aspects, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand of 15 to 50 nucleotides in length and an antisense strand of 15 to 30 nucleotides in length, wherein the sense strand and the antisense strand form a duplex region, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is at least 15 contiguous nucleotides in length.

In yet other aspects, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand of 15 to 50 nucleotides in length and an antisense strand, wherein the sense strand and the antisense strand form a duplex region, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is 19 contiguous nucleotides in length, optionally 20 nucleotides in length.

In further aspects, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand of 18 to 36 nucleotides in length and an antisense strand, wherein the sense strand and the antisense strand form a duplex region, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is 19 contiguous nucleotides in length, optionally 20 nucleotides in length.

In other aspects, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand of 18 to 36 nucleotides in length and an antisense strand of 22 nucleotides in length, wherein the sense strand and the antisense strand form a duplex region, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is 19 contiguous nucleotides in length, optionally 20 nucleotides in length.

In some aspects, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand of 18 to 36 nucleotides in length and an antisense strand of 22 nucleotides in length, wherein the sense strand and the antisense strand form a duplex region, wherein the 3′ end of the sense strand comprises a stem-loop set forth as S1-L-S2, wherein S1 is complementary to S2, and wherein L forms a loop between S1 and S2 of 3-5 nucleotides in length, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is 19 contiguous nucleotides in length, optionally 20 nucleotides in length.

In other aspects, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand of 36 nucleotides in length and an antisense strand of 22 nucleotides in length, wherein the sense strand and the antisense strand form a duplex region, wherein the 3′ end of the sense strand comprises a stem-loop set forth as S1-L-S2, wherein S1 is complementary to S2, and wherein L forms a loop between S1 and S2 of 3-5 nucleotides in length, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is 19 contiguous nucleotides in length, optionally 20 nucleotides in length.

In yet other aspects, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand of 36 nucleotides in length and an antisense strand of 22 nucleotides in length, wherein the sense strand and the antisense strand form a duplex region of at least 19 nucleotides in length, optionally 20 nucleotides in length, wherein the 3′ end of the sense strand comprises a stem-loop set forth as S1-L-S2, wherein S1 is complementary to S2, and wherein L forms a loop between S1 and S2 of 3-5 nucleotides in length, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is 19 contiguous nucleotides in length, optionally 20 nucleotides in length.

In any of the foregoing or related aspects, L is a triloop or a tetraloop. In some embodiments, L is a tetraloop. In some embodiments, the tetraloop comprises the sequence 5′-GAAA-3′.

In any of the foregoing or related embodiments, the S1 and S2 are 1-10 nucleotides in length and have the same length. In some embodiments, S1 and S2 are 1 nucleotide, 2 nucleotides, 3 nucleotides, 4 nucleotides, 5 nucleotides, 6 nucleotides, 7 nucleotides, 8 nucleotides, 9 nucleotides, or 10 nucleotides in length. In some embodiments, S1 and S2 are 6 nucleotides in length. In some embodiments, the stem-loop comprises the sequence 5′-GCAGCCGAAAGGCUGC-3′ (SEQ ID NO: 1197).

In any of the foregoing or related embodiments, the antisense strand comprises a 3′ overhang sequence of one or more nucleotides in length. In some embodiments, the 3′ overhang sequence is 2 nucleotides in length, optionally wherein the 3′ overhang sequence is GG.

In any of the foregoing or related embodiments, the oligonucleotide comprises at least one modified nucleotide. In some embodiments, the modified nucleotide comprises a 2′-modification. In some embodiments, the 2′-modification is a modification selected from 2′-aminoethyl, 2′-fluoro, 2′-O-methyl, 2′-O-methoxyethyl, and 2′-deoxy-2′-fluoro-β-d-arabinonucleic acid. In some embodiments, all nucleotides comprising the oligonucleotide are modified, optionally wherein the modification is a 2′-modification selected from 2′-fluoro and 2′-O-methyl.

In any of the foregoing or related embodiments, the oligonucleotide comprises at least one modified internucleotide linkage. In some embodiments, the at least one modified internucleotide linkage is a phosphorothioate linkage.

In any of the foregoing or related embodiments, the 4′-carbon of the sugar of the 5′-nucleotide of the antisense strand comprises a phosphate analog. In some embodiments, the phosphate analog is oxymethylphosphonate, vinylphosphonate or malonyl phosphonate, optionally wherein the phosphate analog is a 4′-phosphate analog comprising 5′-methoxyphosphonate-4′-oxy.

In any of the foregoing or related embodiments, at least one nucleotide of the oligonucleotide is conjugated to one or more targeting ligands. In some embodiments, each targeting ligand comprises a carbohydrate, amino sugar, cholesterol, polypeptide, or lipid. In some embodiments, each targeting ligand comprises a N-acetylgalactosamine (GalNAc) moiety. In some embodiments, the GalNAc moiety is a monovalent GalNAc moiety, a bivalent GalNAc moiety, a trivalent GalNAc moiety or a tetravalent GalNAc moiety. In some embodiments, up to 4 nucleotides of L of the stem-loop are each conjugated to a monovalent GalNAc moiety.

In any of the foregoing or related embodiments, the sense strand comprises a nucleotide sequence of any one of SEQ ID NOs: 388, 389, 390, 391, 392, 393, 394, 395, 396, 397, 398, 399, 400, 401, 402, and 403.

In any of the foregoing or related embodiments, the antisense strand comprises a nucleotide sequence of any one of SEQ ID NOs: 788, 789, 790, 791, 792, 793, 794, 795, 796, 797, 798, 799, 800, 801, 802, and 803.

In any of the foregoing or related embodiments, the sense strand and antisense strands comprise nucleotide sequences selected from the group consisting of:

- (a) SEQ ID NOs: 393 and 793, respectively;
- (b) SEQ ID NOs: 388 and 788, respectively;
- (c) SEQ ID NOs: 389 and 789, respectively;
- (d) SEQ ID NOs: 390 and 790, respectively;
- (e) SEQ ID NOs: 391 and 791, respectively;
- (f) SEQ ID NOs: 392 and 792, respectively;
- (g) SEQ ID NOs: 394 and 794, respectively;
- (h) SEQ ID NOs: 395 and 795, respectively;
- (i) SEQ ID NOs: 396 and 796, respectively;
- (j) SEQ ID NOs: 397 and 797, respectively;
- (k) SEQ ID NOs: 398 and 798, respectively;
- (l) SEQ ID NOs: 399 and 799, respectively;
- (m) SEQ ID NOs: 400 and 800, respectively;
- (n) SEQ ID NOs: 401 and 801, respectively;
- (o) SEQ ID NOs: 402 and 802, respectively; and
- (p) SEQ ID NOs: 403 and 803, respectively.

In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 393, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 793. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 388, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 788. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 389, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 789. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 390, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 790. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 391, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 791. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 392, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 792. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 394, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 794. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 395, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 795. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 396, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 796. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 397, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 797. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 398, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 798. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 399, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 799. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 400, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 800. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 401, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 801. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 402, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 802. In some embodiments, the sense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 403, wherein the antisense strand comprises a nucleotide sequence as set forth in SEQ ID NO: 803.

In further embodiments, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand and an antisense strand, wherein the sense strand and the antisense strand form a duplex region, wherein all nucleotides comprising the sense strand and antisense strand are modified, wherein the 4′-carbon of the sugar of the 5′-nucleotide of the antisense strand comprises a phosphate analog, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is at least 15 contiguous nucleotides in length.

In other embodiments, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand and an antisense strand, wherein the sense strand and the antisense strand form a duplex region, wherein all nucleotides comprising the sense strand and antisense strand are modified, wherein the 4′-carbon of the sugar of the 5′-nucleotide of the antisense strand comprises a phosphate analog, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is at least 15 contiguous nucleotides in length.

In some embodiments, the disclosure provides an RNAi oligonucleotide for reducing LPA expression, the oligonucleotide comprising a sense strand and an antisense strand, wherein the sense strand and the antisense strand form a duplex region, wherein all nucleotides comprising the sense strand and the antisense strand are modified, wherein the antisense strand and the sense strand comprise one or more 2′-fluoro and 2′-O-methyl modified nucleotides and at least one phosphorothioate linkage, wherein the 4′-carbon of the sugar of the 5′-nucleotide of the antisense strand comprises a phosphate analog, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is at least 15 contiguous nucleotides in length.

In some embodiments, the disclosure provides a method for treating a subject having a disease, disorder or condition associated with LPA expression, the method comprising administering to the subject a therapeutically effective amount of the RNAi oligonucleotide of any one of the preceding claims, or pharmaceutical composition thereof, thereby treating the subject.

In other embodiments, the disclosure provides a pharmaceutical composition comprising a RNAi oligonucleotide described herein, and a pharmaceutically acceptable carrier, delivery agent or excipient.

In other embodiments, the disclosure provides a method of delivering an oligonucleotide to a subject, the method comprising administering a pharmaceutical composition described herein to the subject.

In another embodiments, the disclosure provides a method for reducing LPA expression in a cell, a population of cells or a subject, the method comprising the step of:

- i. contacting the cell or the population of cells with a RNAi oligonucleotide or pharmaceutical composition described herein; or
- ii. administering to the subject a RNAi oligonucleotide or pharmaceutical composition described herein. In some embodiments, reducing LPA expression comprises reducing an amount or level of LPA mRNA, an amount or level of LPA protein, or both. In some embodiments, the subject has a disease, disorder or condition associated with LPA expression. In some embodiments, the disease, disorder, or condition associated with LPA expression is a cardiometabolic disease, optionally atherosclerosis, dyslipidemia, NAFLD and NASH. In some embodiments, the RNAi oligonucleotide, or pharmaceutical composition, is administered in combination with a second composition or therapeutic agent.

In another aspect, the disclosure provides a method for treating a subject having a disease, disorder or condition associated with LPA expression, the method comprising administering to the subject a therapeutically effective amount of an RNAi oligonucleotide comprising a sense strand and an antisense strand, wherein the sense strand and the antisense strand form a duplex region, wherein the antisense strand comprises a region of complementarity to a LPA mRNA target sequence of any one of SEQ ID NOs: 4-387, and wherein the region of complementarity is at least 15 contiguous nucleotides in length.

In other embodiments, the disclosure provides a method for treating a subject having a disease, disorder or condition associated with LPA expression, the method comprising administering to the subject a therapeutically effective amount of an RNAi oligonucleotide comprising a sense strand and an antisense strand, wherein the sense strand and antisense strands comprise nucleotide sequences selected from the group consisting of:

- (a) SEQ ID NOs: 393 and 793, respectively;
- (b) SEQ ID NOs: 388 and 788, respectively;
- (c) SEQ ID NOs: 389 and 789, respectively;
- (d) SEQ ID NOs: 390 and 790, respectively;
- (e) SEQ ID NOs: 391 and 791, respectively;
- (f) SEQ ID NOs: 392 and 792, respectively;
- (g) SEQ ID NOs: 394 and 794, respectively;
- (h) SEQ ID NOs: 395 and 795, respectively;
- (i) SEQ ID NOs: 396 and 796, respectively;
- (j) SEQ ID NOs: 397 and 797, respectively;
- (k) SEQ ID NOs: 398 and 798, respectively;
- (l) SEQ ID NOs: 399 and 799, respectively;
- (m) SEQ ID NOs: 400 and 800, respectively;
- (n) SEQ ID NOs: 401 and 801, respectively;
- (o) SEQ ID NOs: 402 and 802, respectively; and
- (p) SEQ ID NOs: 403 and 803, respectively.

In some embodiments, the disease, disorder, or condition associated with LPA expression is a cardiometabolic disease, optionally atherosclerosis, dyslipidemia, NAFLD and NASH.

In some embodiments, the disclosure provides use of an RNAi oligonucleotide or pharmaceutical composition described herein, in the manufacture of a medicament for the treatment of a disease, disorder or condition associated with LPA expression, optionally for the treatment of a cardiometabolic disease, optionally atherosclerosis, dyslipidemia, NAFLD and NASH.

In some embodiments, the disclosure provides use of an RNAi oligonucleotide or pharmaceutical composition described herein, for use, or adaptable for use, in the treatment of a disease, disorder or condition associated with LPA expression, optionally for the treatment of a cardiometabolic disease, optionally atherosclerosis, dyslipidemia, NAFLD and NASH.

In other embodiments, the disclosure provides a kit comprising an RNAi oligonucleotide described herein, an optional pharmaceutically acceptable carrier, and a package insert comprising instructions for administration to a subject having a disease, disorder or condition associated with LPA expression.

In any of the foregoing or related embodiments, the disease, disorder, or condition associated with LPA expression is a cardiometabolic disease, optionally atherosclerosis, dyslipidemia, NAFLD and NASH.

BRIEF DESCRIPTION OF THE DRAWINGS

FIGS. 1-4 provide graphs depicting the percent (%) of LPA mRNA in HEK293-LPA cells transfected with the indicated DsiRNAs relative to the % of LPA mRNA control mock-treated cells.

FIG. 5 provides a graph depicting the percent (%) of LPA mRNA in HepG2-LPA cells transfected with the indicated DsiRNAs relative to the % of LPA mRNA control mock-treated cells.

FIGS. 6-7 provide graphs depicting the percent (%) of LPA mRNA in HEK293-LPA cells transfected with the indicated DsiRNAs relative to the % of LPA mRNA control mock-treated cells.

FIGS. 8-9 provide graphs depicting the percent (%) of LPA mRNA in liver samples from mice treated with the indicated GalNAc-conjugated LPA oligonucleotides relative to mice treated with phosphate buffered saline (PBS).

FIG. 10 provides a schematic depicting the structure and chemical modification patterns of generic N-Acetylgalactosamine (GalNAc)-conjugated LPA oligonucleotides.

FIGS. 11A-11C provide graphs depicting the percent (%) of LPA mRNA in liver samples from non-human primates (NHPs) treated with the indicated GalNAc-conjugated LPA oligonucleotides relative to NHPs treated with PBS on day 28 (FIG. 11A), day 56 (FIG. 11B) and day 84 (FIG. 11C) following treatment.

FIG. 11D provides a graph depicting the percent (%) of PLG mRNA in liver samples from NHPs treated with the indicated GalNAc-conjugated LPA oligonucleotides relative to NHPs treated with PBS on day 28.

FIG. 12 provides a graph depicting the mean percent (%) of apo(a) protein in serum from NHPs treated with the indicated GalNAc-conjugated LPA oligonucleotides relative to NHPs treated with PBS over time.

DETAILED DESCRIPTION
I. Definitions

As used herein, “about,” as applied to one or more values of interest, refers to a value that is similar to a stated reference value. In certain embodiments, “about” refers to a range of values that fall within 25%, 20%, 19%, 18%1, 17%, 16%, 15%, 14%, 13%, 12%, 11%, 10%, 9%, 8%, 7%, 6%, 5%, 4%, 3%, 2%, 1% or less in either direction (greater than or less than) of the stated reference value unless otherwise stated or otherwise evident from the context (except where such number would exceed 100% of a possible value).

As used herein, “administer,” “administering,” “administration” and the like refers to providing a substance (e.g., an oligonucleotide) to a subject in a manner that is pharmacologically useful (e.g., to treat a condition in the subject).

As used herein, the term “apolipoprotein(a)” and abbreviated as “apo(a)”, refers to the apolipoprotein(a) polypeptide, which is a member of the apolipoprotein class of polypeptides that bind lipids to form lipoproteins. Apo(a) is a polymorphic glycoprotein encoded by the LPA gene in humans. LPA mRNA and apo(a) polypeptide are expressed predominantly in the liver. Lipoprotein(a) (abbreviated as Lp(a)) is a class of lipoprotein formed in the liver and comprises a single copy of apolipoprotein (apo) B-100 (Apo-B100) covalently tethered to apo(a). In humans, apo(a) includes at least 10 subtypes of KIV repeats, composed of 1 copy each of KIV₁, multiple copies of KIV₂, and 1 copy each of KIV₃-KIV₁₀, KV, and an inactive protease-like domain. The presence of apo(a) distinguishes Lp(a) from all other lipoprotein classes (Marcovina et al., (1995) Clin Chem. 41(2):246-55). For the purposes of the disclosure, “apolipoprotein(a)” or “apo(a)” refers to the apo(a) polypeptide from any vertebrate or mammal including, but not limited to, human, mouse, primate, monkey, bovine, chicken, rodent, rat, porcine, ovine and guinea pig. “Apo(a)” also refers to fragments and variants of native apo(a) that maintain at least one in vivo or in vitro activity of a native apo(a). Apo(a) encompasses full-length, unprocessed precursor forms of Apo(a), as well as mature forms resulting from post-translational processing. An exemplary sequence of a human LPA mRNA transcript is publicly available (GenBank Accession No. NM_005577.3) and disclosed herein (SEQ ID NO: 1). An exemplary sequence of cynomolgus monkey LPA mRNA is publicly available (GenBank Accession No. XM_015448517.1) and disclosed herein (SEQ ID NO: 2).

As used herein, “asialoglycoprotein receptor” or “ASGPR” refers to a bipartite C-type lectin formed by a major 48 kDa subunit (ASGPR-1) and minor 40 kDa subunit (ASGPR-2). ASGPR is primarily expressed on the sinusoidal surface of hepatocyte cells and has a major role in binding, internalizing and subsequent clearing of circulating glycoproteins that contain terminal galactose or GalNAc residues (asialoglycoproteins).

As used herein, “attenuate,” “attenuating,” “attenuation” and the like refers to reducing or effectively halting. As a non-limiting example, one or more of the treatments herein may reduce or effectively halt the onset or progression of cardiometabolic diseases including atherosclerosis, dyslipidemia, NAFLD and NASH in a subject. This attenuation may be exemplified by, for example, a decrease in one or more aspects (e.g., symptoms, tissue characteristics, and cellular, inflammatory or immunological activity, etc.) of cardiometabolic diseases including atherosclerosis, dyslipidemia, NAFLD and NASH, no detectable progression (worsening) of one or more aspects of cardiometabolic diseases including atherosclerosis, dyslipidemia, NAFLD and NASH, or no detectable aspects of cardiometabolic diseases including atherosclerosis, dyslipidemia, NAFLD and NASH in a subject when they might otherwise be expected.

As used herein, “complementary” refers to a structural relationship between two nucleotides (e.g., on two opposing nucleic acids or on opposing regions of a single nucleic acid strand) that permits the two nucleotides to form base pairs with one another. For example, a purine nucleotide of one nucleic acid that is complementary to a pyrimidine nucleotide of an opposing nucleic acid may base pair together by forming hydrogen bonds with one another. In some embodiments, complementary nucleotides can base pair in the Watson-Crick manner or in any other manner that allows for the formation of stable duplexes. In some embodiments, two nucleic acids may have regions of multiple nucleotides that are complementary with each other to form regions of complementarity, as described herein.

As used herein, “deoxyribonucleotide” refers to a nucleotide having a hydrogen in place of a hydroxyl at the 2′ position of its pentose sugar when compared with a ribonucleotide. A modified deoxyribonucleotide is a deoxyribonucleotide having one or more modifications or substitutions of atoms other than at the 2′ position, including modifications or substitutions in or of the sugar, phosphate group or base.

As used herein, “double-stranded oligonucleotide” or “ds oligonucleotide” refers to an oligonucleotide that is substantially in a duplex form. In some embodiments, the complementary base-pairing of duplex region(s) of a ds oligonucleotide is formed between antiparallel sequences of nucleotides of covalently separate nucleic acid strands. In some embodiments, complementary base-pairing of duplex region(s) of a ds oligonucleotide is formed between antiparallel sequences of nucleotides of nucleic acid strands that are covalently linked. In some embodiments, complementary base-pairing of duplex region(s) of a ds oligonucleotide is formed from single nucleic acid strand that is folded (e.g., via a hairpin) to provide complementary antiparallel sequences of nucleotides that base pair together. In some embodiments, a ds oligonucleotide comprises two covalently separate nucleic acid strands that are fully duplexed with one another. However, in some embodiments, a ds oligonucleotide comprises two covalently separate nucleic acid strands that are partially duplexed (e.g., having overhangs at one or both ends). In some embodiments, a ds oligonucleotide comprises antiparallel sequence of nucleotides that are partially complementary, and thus, may have one or more mismatches, which may include internal mismatches or end mismatches.

As used herein, “duplex,” in reference to nucleic acids (e.g., oligonucleotides), refers to a structure formed through complementary base pairing of two antiparallel sequences of nucleotides.

As used herein, “excipient” refers to a non-therapeutic agent that may be included in a composition, for example, to provide or contribute to a desired consistency or stabilizing effect.

As used herein, “hepatocyte” or “hepatocytes” refers to cells of the parenchymal tissues of the liver. These cells make up about 70%-85% of the liver's mass and manufacture serum albumin, FBN and the prothrombin group of clotting factors (except for Factors 3 and 4). Markers for hepatocyte lineage cells include, but are not limited to, transthyretin (Ttr), glutamine synthetase (Glul), hepatocyte nuclear factor 1a (Hnf1a) and hepatocyte nuclear factor 4a (Hnf4a). Markers for mature hepatocytes may include, but are not limited to, cytochrome P450 (Cyp3a11), fumarylacetoacetate hydrolase (Fah), glucose 6-phosphate (G6p), albumin (Alb) and OC2-2F8. See, e.g., Huch et al. (2013) Nature 494:247-250.

As used herein, a “hepatotoxic agent” refers to a chemical compound, virus or other substance that is itself toxic to the liver or can be processed to form a metabolite that is toxic to the liver. Hepatotoxic agents may include, but are not limited to, carbon tetrachloride (CCl₄), acetaminophen (paracetamol), vinyl chloride, arsenic, chloroform, nonsteroidal anti-inflammatory drugs (such as aspirin and phenylbutazone).

As used herein, “labile linker” refers to a linker that can be cleaved (e.g., by acidic pH). A “fairly stable linker” refers to a linker that cannot be cleaved.

As used herein, “liver inflammation” or “hepatitis” refers to a physical condition in which the liver becomes swollen, dysfunctional and/or painful, especially as a result of injury or infection, as may be caused by exposure to a hepatotoxic agent. Symptoms may include jaundice (yellowing of the skin or eyes), fatigue, weakness, nausea, vomiting, appetite reduction and weight loss. Liver inflammation, if left untreated, may progress to fibrosis, cirrhosis, liver failure or liver cancer.

As used herein, “liver fibrosis” or “fibrosis of the liver” refers to an excessive accumulation in the liver of extracellular matrix proteins, which could include collagens (I, III, and IV), FBN, undulin, elastin, laminin, hyaluronan and proteoglycans resulting from inflammation and liver cell death. Liver fibrosis, if left untreated, may progress to cirrhosis, liver failure or liver cancer.

As used herein, “loop” refers to a unpaired region of a nucleic acid (e.g., oligonucleotide) that is flanked by two antiparallel regions of the nucleic acid that are sufficiently complementary to one another, such that under appropriate hybridization conditions (e.g., in a phosphate buffer, in a cells), the two antiparallel regions, which flank the unpaired region, hybridize to form a duplex (referred to as a “stem”).

As used herein, “modified internucleotide linkage” refers to an internucleotide linkage having one or more chemical modifications when compared with a reference internucleotide linkage comprising a phosphodiester bond. In some embodiments, a modified nucleotide is a non-naturally occurring linkage. Typically, a modified internucleotide linkage confers one or more desirable properties to a nucleic acid in which the modified internucleotide linkage is present. For example, a modified nucleotide may improve thermal stability, resistance to degradation, nuclease resistance, solubility, bioavailability, bioactivity, reduced immunogenicity, etc.

As used herein, “modified nucleotide” refers to a nucleotide having one or more chemical modifications when compared with a corresponding reference nucleotide selected from: adenine ribonucleotide, guanine ribonucleotide, cytosine ribonucleotide, uracil ribonucleotide, adenine deoxyribonucleotide, guanine deoxyribonucleotide, cytosine deoxyribonucleotide and thymidine deoxyribonucleotide. In some embodiments, a modified nucleotide is a non-naturally occurring nucleotide. In some embodiments, a modified nucleotide has one or more chemical modification in its sugar, nucleobase and/or phosphate group. In some embodiments, a modified nucleotide has one or more chemical moieties conjugated to a corresponding reference nucleotide. Typically, a modified nucleotide confers one or more desirable properties to a nucleic acid in which the modified nucleotide is present. For example, a modified nucleotide may improve thermal stability, resistance to degradation, nuclease resistance, solubility, bioavailability, bioactivity, reduced immunogenicity, etc.

As used herein, “nicked tetraloop structure” refers to a structure of a RNAi oligonucleotide that is characterized by separate sense (passenger) and antisense (guide) strands, in which the sense strand has a region of complementarity with the antisense strand, and in which at least one of the strands, generally the sense strand, has a tetraloop configured to stabilize an adjacent stem region formed within the at least one strand.

As used herein, “oligonucleotide” refers to a short nucleic acid (e.g., less than about 100 nucleotides in length). An oligonucleotide may be single-stranded (ss) or ds. An oligonucleotide may or may not have duplex regions. As a set of non-limiting examples, an oligonucleotide may be, but is not limited to, a small interfering RNA (siRNA), microRNA (miRNA), short hairpin RNA (shRNA), dicer substrate interfering RNA (dsiRNA), antisense oligonucleotide, short siRNA or ss siRNA. In some embodiments, a ds oligonucleotide is an RNAi oligonucleotide.

As used herein, “overhang” refers to terminal non-base pairing nucleotide(s) resulting from one strand or region extending beyond the terminus of a complementary strand with which the one strand or region forms a duplex. In some embodiments, an overhang comprises one or more unpaired nucleotides extending from a duplex region at the 5′ terminus or 3′ terminus of a ds oligonucleotide. In certain embodiments, the overhang is a 3′ or 5′ overhang on the antisense strand or sense strand of a ds oligonucleotides.

As used herein, “phosphate analog” refers to a chemical moiety that mimics the electrostatic and/or steric properties of a phosphate group. In some embodiments, a phosphate analog is positioned at the 5′ terminal nucleotide of an oligonucleotide in place of a 5′-phosphate, which is often susceptible to enzymatic removal. In some embodiments, a 5′ phosphate analog contains a phosphatase-resistant linkage. Examples of phosphate analogs include, but are not limited to, 5′ phosphonates, such as 5′ methylenephosphonate (5′-MP) and 5′-(E)-vinylphosphonate (5′-VP). In some embodiments, an oligonucleotide has a phosphate analog at a 4′-carbon position of the sugar (referred to as a “4′-phosphate analog”) at a 5′-terminal nucleotide. An example of a 4′-phosphate analog is oxymethylphosphonate, in which the oxygen atom of the oxymethyl group is bound to the sugar moiety (e.g., at its 4′-carbon) or analog thereof. See, e.g., US Provisional Patent Application Nos. 62/383,207 (filed on 2 Sep. 2016) and 62/393,401 (filed on 12 Sep. 2016). Other modifications have been developed for the 5′ end of oligonucleotides (see, e.g., Intl. Patent Application No. WO 2011/133871; U.S. Pat. No. 8,927,513; and Prakash et al. (2015) Nucleic Acids Res. 43:2993-3011).

As used herein, “reduced expression” of a gene (e.g., LPA) refers to a decrease in the amount or level of RNA transcript (e.g., LPA mRNA) or protein encoded by the gene and/or a decrease in the amount or level of activity of the gene in a cell, a population of cells, a sample or a subject, when compared to an appropriate reference (e.g., a reference cell, population of cells, sample or subject). For example, the act of contacting a cell with an oligonucleotide herein (e.g., an oligonucleotide comprising an antisense strand having a nucleotide sequence that is complementary to a nucleotide sequence comprising LPA mRNA) may result in a decrease in the amount or level of LPA mRNA, apo(a) protein and/or apo(a) activity (e.g., via inactivation and/or degradation of LPA mRNA by the RNAi pathway) when compared to a cell that is not treated with the ds oligonucleotide. Similarly, and as used herein, “reducing expression” refers to an act that results in reduced expression of a gene (e.g., LPA). As used herein, “reduction of LPA expression” refers to a decrease in the amount or level of LPA mRNA, apo(a) protein and/or apo(a) activity in a cell, a population of cells, a sample or a subject when compared to an appropriate reference (e.g., a reference cell, population of cells, sample, or subject).

As used herein, “region of complementarity” refers to a sequence of nucleotides of a nucleic acid (e.g., a ds oligonucleotide) that is sufficiently complementary to an antiparallel sequence of nucleotides to permit hybridization between the two sequences of nucleotides under appropriate hybridization conditions (e.g., in a phosphate buffer, in a cell, etc.). In some embodiments, an oligonucleotide herein comprises a targeting sequence having a region of complementary to a mRNA target sequence.

As used herein, “ribonucleotide” refers to a nucleotide having a ribose as its pentose sugar, which contains a hydroxyl group at its 2′ position. A modified ribonucleotide is a ribonucleotide having one or more modifications or substitutions of atoms other than at the 2′ position, including modifications or substitutions in or of the ribose, phosphate group or base.

As used herein, “RNAi oligonucleotide” refers to either (a) a ds oligonucleotide having a sense strand (passenger) and antisense strand (guide), in which the antisense strand or part of the antisense strand is used by the Argonaute 2 (Ago2) endonuclease in the cleavage of a target mRNA (e.g., LPA mRNA) or (b) a ss oligonucleotide having a single antisense strand, where that antisense strand (or part of that antisense strand) is used by the Ago2 endonuclease in the cleavage of a target mRNA (e.g., LPA mRNA).

As used herein, “strand” refers to a single, contiguous sequence of nucleotides linked together through internucleotide linkages (e.g., phosphodiester linkages or phosphorothioate linkages). In some embodiments, a strand has two free ends (e.g., a 5′ end and a 3′ end).

As used herein, “subject” means any mammal, including mice, rabbits and humans. In one embodiment, the subject is a human or NHP. Moreover, “individual” or “patient” may be used interchangeably with “subject.”

As used herein, “synthetic” refers to a nucleic acid or other molecule that is artificially synthesized (e.g., using a machine (e.g., a solid-state nucleic acid synthesizer)) or that is otherwise not derived from a natural source (e.g., a cell or organism) that normally produces the molecule.

As used herein, “targeting ligand” refers to a molecule (e.g., a carbohydrate, amino sugar, cholesterol, polypeptide or lipid) that selectively binds to a cognate molecule (e.g., a receptor) of a tissue or cell of interest and that is conjugatable to another substance for purposes of targeting the other substance to the tissue or cell of interest. For example, in some embodiments, a targeting ligand may be conjugated to an oligonucleotide for purposes of targeting the oligonucleotide to a specific tissue or cell of interest. In some embodiments, a targeting ligand selectively binds to a cell surface receptor. Accordingly, in some embodiments, a targeting ligand when conjugated to an oligonucleotide facilitates delivery of the oligonucleotide into a particular cell through selective binding to a receptor expressed on the surface of the cell and endosomal internalization by the cell of the complex comprising the oligonucleotide, targeting ligand and receptor. In some embodiments, a targeting ligand is conjugated to an oligonucleotide via a linker that is cleaved following or during cellular internalization such that the oligonucleotide is released from the targeting ligand in the cell.

As used herein, “tetraloop” refers to a loop that increases stability of an adjacent duplex formed by hybridization of flanking sequences of nucleotides. The increase in stability is detectable as an increase in melting temperature (T_m) of an adjacent stem duplex that is higher than the T_mof the adjacent stem duplex expected, on average, from a set of loops of comparable length consisting of randomly selected sequences of nucleotides. For example, a tetraloop can confer a T_mof at least about 50° C., at least about 55° C., at least about 56° C., at least about 58° C., at least about 60° C., at least about 65° C. or at least about 75° C. in 10 mM NaHPO₄to a hairpin comprising a duplex of at least 2 base pairs (bp) in length. In some embodiments, a tetraloop may stabilize a bp in an adjacent stem duplex by stacking interactions. In addition, interactions among the nucleotides in a tetraloop include, but are not limited to, non-Watson-Crick base pairing, stacking interactions, hydrogen bonding and contact interactions (Cheong et al. (1990) NATURE 346:680-82; Heus & Pardi (1991) SCIENCE 253:191-94). In some embodiments, a tetraloop comprises or consists of 3 to 6 nucleotides and is typically 4 to 5 nucleotides. In certain embodiments, a tetraloop comprises or consists of 3, 4, 5 or 6 nucleotides, which may or may not be modified (e.g., which may or may not be conjugated to a targeting moiety). In one embodiment, a tetraloop consists of 4 nucleotides.

Any nucleotide may be used in the tetraloop and standard IUPAC-IUB symbols for such nucleotides may be used as described in Cornish-Bowden (1985) Nucleic Acids Res. 13:3021-3030. For example, the letter “N” may be used to mean that any base may be in that position, the letter “R” may be used to show that A (adenine) or G (guanine) may be in that position, and “B” may be used to show that C (cytosine), G (guanine), T (thymine) or U (uracil) may be in that position. Examples of tetraloops include the UNCG family of tetraloops (e.g., UUCG), the GNRA family of tetraloops (e.g., GAAA), and the CUUG tetraloop (Woese et al. (1990) Proc. Natl. Acad. Sci. USA 87:8467-8471; Antao et al. (1991) Nucleic Acids Res. 19:5901-5905). Examples of DNA tetraloops include the d(GNNA) family of tetraloops (e.g., d(GTTA), the d(GNRA)) family of tetraloops, the d(GNAB) family of tetraloops, the d(CNNG) family of tetraloops, and the d(TNCG) family of tetraloops (e.g., d(TTCG)). See, e.g., Nakano et al. (2002) Biochem. 41:4281-14292; Shinji et al. (2000) Nippon Kagakkai Koen Yokoshu 78:731. In some embodiments, the tetraloop is contained within a nicked tetraloop structure.

As used herein, “treat” or “treating” refers to the act of providing care to a subject in need thereof, for example, by administering a therapeutic agent (e.g., an oligonucleotide herein) to the subject, for purposes of improving the health and/or well-being of the subject with respect to an existing condition (e.g., a disease, disorder) or to prevent or decrease the likelihood of the occurrence of a condition. In some embodiments, treatment involves reducing the frequency or severity of at least one sign, symptom or contributing factor of a condition (e.g., disease, disorder) experienced by a subject.

II. Oligonucleotide Inhibitors of LPA Expression

The disclosure provides, inter alia, oligonucleotides that inhibit LPA expression. In some embodiments, an oligonucleotide that inhibits LPA expression herein is targeted to an LPA mRNA.

i. LPA Target Sequences

In some embodiments, the oligonucleotide is targeted to a target sequence comprising an LPA mRNA. In some embodiments, the oligonucleotide, or a portion, fragment or strand thereof (e.g., an antisense strand or a guide strand of a ds oligonucleotide) binds or anneals to a target sequence comprising an LPA mRNA, thereby inhibiting LPA expression. In some embodiments, the oligonucleotide is targeted to an LPA target sequence for the purpose of inhibiting LPA expression in vivo. In some embodiments, the amount or extent of inhibition of LPA expression by an oligonucleotide targeted to an LPA target sequence correlates with the potency of the oligonucleotide. In some embodiments, the amount or extent of inhibition of LPA expression by an oligonucleotide targeted to an LPA target sequence correlates with the amount or extent of therapeutic benefit in a subject or patient having a disease, disorder or condition associated with the expression of LPA treated with the oligonucleotide.

Through examination and analysis of the nucleotide sequence of LPA mRNAs encoding apo(a), including mRNAs of multiple different species (e.g., human, cynomolgus monkey, and rhesus monkey; see, e.g., Example 1) and as a result of in vitro and in vivo testing (see, e.g., Example 2 and Example 3), it has been discovered that certain nucleotide sequences of LPA mRNA are more amenable than others to oligonucleotide-based inhibition of LPA expression and are thus useful as target sequences for the oligonucleotides herein. In some embodiments, a sense strand of an oligonucleotide (e.g., a ds oligonucleotide) described herein (e.g., in Table 5) comprises an LPA target sequence. In some embodiments, a portion or region of the sense strand of a ds oligonucleotide described herein (e.g., in Table 5) comprises an LPA target sequence. In some embodiments, an LPA target sequence comprises, or consists of, a sequence of any one of SEQ ID Nos: 4-387.

ii. LPA Targeting Sequences

In some embodiments, the oligonucleotides herein have regions of complementarity to LPA mRNA (e.g., within a target sequence of LPA mRNA) for purposes of targeting the LPA mRNA in cells and inhibiting LPA expression. In some embodiments, the oligonucleotides herein comprise an LPA targeting sequence (e.g., an antisense strand or a guide strand of a ds oligonucleotide) having a region of complementarity that binds or anneals to an LPA target sequence by complementary (Watson-Crick) base pairing. The targeting sequence or region of complementarity is generally of a suitable length and base content to enable binding or annealing of the oligonucleotide (or a strand thereof) to an LPA mRNA for purposes of inhibiting its expression. In some embodiments, the targeting sequence or region of complementarity is at least about 12, at least about 13, at least about 14, at least about 15, at least about 16, at least about 17, at least about 18, at least about 19, at least about 20, at least about 21, at least about 22, at least about 23, at least about 24, at least about 25, at least about 26, at least about 27, at least about 28, at least about 29 or at least about 30 nucleotides in length. In some embodiments, the targeting sequence or region of complementarity is about 12 to about 30 (e.g., 12 to 30, 12 to 22, 15 to 25, 17 to 21, 18 to 27, 19 to 27, or 15 to 30) nucleotides in length. In some embodiments, the targeting sequence or region of complementarity is about 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29 or 30 nucleotides in length. In some embodiments, the targeting sequence or region of complementarity is 18 nucleotides in length. In some embodiments, the targeting sequence or region of complementarity is 19 nucleotides in length. In some embodiments, the targeting sequence or region of complementarity is 20 nucleotides in length. In some embodiments, the targeting sequence or region of complementarity is 21 nucleotides in length. In some embodiments, the targeting sequence or region of complementarity is 22 nucleotides in length. In some embodiments, the targeting sequence or region of complementarity is 23 nucleotides in length. In some embodiments, the targeting sequence or region of complementarity is 24 nucleotides in length.

In some embodiments, an oligonucleotide herein comprises a targeting sequence or a region of complementarity (e.g., an antisense strand or a guide strand of a double-stranded oligonucleotide) that is fully complementary to an LPA target sequence. In some embodiments, the targeting sequence or region of complementarity is partially complementary to an LPA target sequence. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity that is fully complementary to a sequence of any one of SEQ ID NOs: 4-387. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity that is partially complementary to a sequence of any one of SEQ ID NOs: 4-387.

In some embodiments, the oligonucleotide herein comprises a targeting sequence or region of complementarity that is complementary to a contiguous sequence of nucleotides comprising an LPA mRNA, wherein the contiguous sequence of nucleotides is about 12 to about 30 nucleotides in length (e.g., 12 to 30, 12 to 28, 12 to 26, 12 to 24, 12 to 20, 12 to 18, 12 to 16, 14 to 22, 16 to 20, 18 to 20 or 18 to 19 nucleotides in length). In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity that is complementary to a contiguous sequence of nucleotides comprising an LPA mRNA, wherein the contiguous sequence of nucleotides is 10, 11, 12, 13, 14, 15, 16, 17, 18, 19 or 20 nucleotides in length. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity that is complementary to a contiguous sequence of nucleotides comprising an LPA mRNA, wherein the contiguous sequence of nucleotides is 19 nucleotides in length. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity that is complementary to a contiguous sequence of nucleotides comprising an LPA mRNA, wherein the contiguous sequence of nucleotides is 20 nucleotides in length. In some embodiments, the oligonucleotide comprises a targeting sequence or a region of complementarity that is complementary to a contiguous sequence of nucleotides of any one of SEQ ID NOs: 4-387, optionally wherein the contiguous sequence of nucleotides is 19 nucleotides in length.

In some embodiments, a targeting sequence or region of complementarity of an oligonucleotide that is complementary to contiguous nucleotides of a sequence as set forth in any one of SEQ ID NOs: 4-387 and spans the entire length of an antisense strand. In some embodiments, a region of complementarity of an oligonucleotide that is complementary to contiguous nucleotides of a sequence as set forth in any one of SEQ ID NOs: 4-387 and spans a portion of the entire length of an antisense strand. In some embodiments, an oligonucleotide herein comprises a region of complementarity (e.g., on an antisense strand of a ds oligonucleotide) that is at least partially (e.g., fully) complementary to a contiguous stretch of nucleotides spanning nucleotides 1-20 of a sequence as set forth in any one of SEQ ID NOs: 4-387.

In some embodiments, an oligonucleotide herein comprises a targeting sequence or region of complementarity having one or more base pair (bp) mismatches with the corresponding LPA target sequence. In some embodiments, the targeting sequence or region of complementarity may have up to about 1, up to about 2, up to about 3, up to about 4, up to about 5, etc. mismatches with the corresponding LPA target sequence provided that the ability of the targeting sequence or region of complementarity to bind or anneal to the LPA mRNA under appropriate hybridization conditions and/or the ability of the oligonucleotide to reduce or inhibit LPA expression is maintained. Alternatively, in some embodiments, the targeting sequence or region of complementarity comprises no more than 1, no more than 2, no more than 3, no more than 4, or no more than 5 mismatches with the corresponding LPA target sequence provided that the ability of the targeting sequence or region of complementarity to bind or anneal to the LPA mRNA under appropriate hybridization conditions and/or the ability of the oligonucleotide to reduce or inhibit LPA expression is maintained. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity having 1 mismatch with the corresponding target sequence. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity having 2 mismatches with the corresponding target sequence. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity having 3 mismatches with the corresponding target sequence. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity having 4 mismatches with the corresponding target sequence. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity having 5 mismatches with the corresponding target sequence. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity more than one mismatch (e.g., 2, 3, 4, 5 or more mismatches) with the corresponding target sequence, wherein at least 2 (e.g., all) of the mismatches are positioned consecutively (e.g., 2, 3, 4, 5 or more mismatches in a row), or wherein the mismatches are interspersed in any position throughout the targeting sequence or region of complementarity. In some embodiments, the oligonucleotide comprises a targeting sequence or region of complementarity more than one mismatch (e.g., 2, 3, 4, 5 or more mismatches) with the corresponding target sequence, wherein at least 2 (e.g., all) of the mismatches are positioned consecutively (e.g., 2, 3, 4, 5 or more mismatches in a row), or wherein at least one or more non-mismatched base pair is located between the mismatches, or a combination thereof.

iii. Types of Oligonucleotides

A variety of oligonucleotide types and/or structures are useful for targeting LPA mRNA in the methods herein including, but not limited to, RNAi oligonucleotides, antisense oligonucleotides, miRNAs, etc. Any of the oligonucleotide types described herein or elsewhere are contemplated for use as a framework to incorporate an LPA mRNA targeting sequence herein for the purposes of inhibiting LPA expression.

In some embodiments, the oligonucleotides herein inhibit LPA expression by engaging with RNA interference (RNAi) pathways upstream or downstream of Dicer involvement. For example, RNAi oligonucleotides have been developed with each strand having sizes of about 19-25 nucleotides with at least one 3′ overhang of 1 to 5 nucleotides (see, e.g., U.S. Pat. No. 8,372,968). Longer oligonucleotides also have been developed that are processed by Dicer to generate active RNAi products (see, e.g., U.S. Pat. No. 8,883,996). Further work produced extended ds oligonucleotides where at least one end of at least one strand is extended beyond a duplex targeting region, including structures where one of the strands includes a thermodynamically-stabilizing tetraloop structure (see, e.g., U.S. Pat. Nos. 8,513,207 and 8,927,705, as well as Intl. Patent Application Publication No. WO 2010/033225). Such structures may include ss extensions (on one or both sides of the molecule) as well as ds extensions.

In some embodiments, the oligonucleotides herein engage with the RNAi pathway downstream of the involvement of Dicer (e.g., Dicer cleavage). In some embodiments, the oligonucleotide has an overhang (e.g., of 1, 2, or 3 nucleotides in length) in the 3′ end of the sense strand. In some embodiments, the oligonucleotide (e.g., siRNA) comprises a 21-nucleotide guide strand that is antisense to a target mRNA (e.g., LPA mRNA) and a complementary passenger strand, in which both strands anneal to form a 19-bp duplex and 2 nucleotide overhangs at either or both 3′ ends. Longer oligonucleotide designs also are contemplated including oligonucleotides having a guide strand of 23 nucleotides and a passenger strand of 21 nucleotides, where there is a blunt end on the right side of the molecule (3′ end of passenger strand/5′ end of guide strand) and a two nucleotide 3′-guide strand overhang on the left side of the molecule (5′ end of the passenger strand/3′ end of the guide strand). In such molecules, there is a21 bp duplex region. See, e.g., U.S. Pat. Nos. 9,012,138; 9,012,621 and 9,193,753.

In some embodiments, the oligonucleotides herein comprise sense and antisense strands that are both in the range of about 17 to 26 (e.g., 17 to 26, 20 to 25 or 21-23) nucleotides in length. In some embodiments, an oligonucleotide herein comprises a sense and antisense strand that are both in the range of about 19-22 nucleotides in length. In some embodiments, the sense and antisense strands are of equal length. In some embodiments, an oligonucleotide comprises sense and antisense strands, such that there is a 3′-overhang on either the sense strand or the antisense strand, or both the sense and antisense strand. In some embodiments, for oligonucleotides that have sense and antisense strands that are both in the range of about 21-23 nucleotides in length, a 3′ overhang on the sense, antisense, or both sense and antisense strands is 1 or 2 nucleotides in length. In some embodiments, the oligonucleotide has a guide strand of 22 nucleotides and a passenger strand of 20 nucleotides, where there is a blunt end on the right side of the molecule (3′ end of passenger strand/5′ end of guide strand) and a 2 nucleotide 3′-guide strand overhang on the left side of the molecule (5′ end of the passenger strand/3′ end of the guide strand). In such molecules, there is a 20 bp duplex region.

Other oligonucleotide designs for use with the compositions and methods herein include: 16-mer siRNAs (see, e.g., NUCLEIC ACIDS IN CHEMISTRY AND BIOLOGY, Blackburn (ed.), Royal Society of Chemistry, 2006), shRNAs (e.g., having 19 bp or shorter stems; see, e.g., Moore et al. (2010) METHODS MOL. BIOL. 629:141-58), blunt siRNAs (e.g., of 19 bps in length; see, e.g., Kraynack & Baker (2006) RNA 12:163-76), asymmetrical siRNAs (aiRNA; see, e.g., Sun et al. (2008) NAT. BIOTECHNOL. 26:1379-82), asymmetric shorter-duplex siRNA (see, e.g., Chang et al. (2009) MOL. THER. 17:725-32), fork siRNAs (see, e.g., Hohjoh (2004) FEBS LETT. 557:193-198), ss siRNAs (Elsner (2012) NAT. BIOTECHNOL. 30:1063), dumbbell-shaped circular siRNAs (see, e.g., Abe et al. (2007) J. AM. CHEM. SOC. 129:15108-09), and small internally segmented interfering RNA (siRNA; see, e.g., Bramsen et al. (2007) NUCLEIC ACIDS RES. 35:5886-97). Further non-limiting examples of an oligonucleotide structures that may be used in some embodiments to reduce or inhibit the expression of LPA are microRNA (miRNA), short hairpin RNA (shRNA) and short siRNA (see, e.g., Hamilton et al. (2002) EMBO J. 21:4671-79; see also, US Patent Application Publication No. 2009/0099115).

Still, in some embodiments, an oligonucleotide for reducing or inhibiting LPA expression herein is single-stranded (ss). Such structures may include but are not limited to ss RNAi molecules. Recent efforts have demonstrated the activity of ss RNAi molecules (see, e.g., Matsui et al. (2016) Mol. Ther. 24:946-955). However, in some embodiments, oligonucleotides herein are antisense oligonucleotides (ASOs). An antisense oligonucleotide is a ss oligonucleotide that has a nucleobase sequence which, when written or depicted in the 5′ to 3′ direction, comprises the reverse complement of a targeted segment of a particular nucleic acid and is suitably modified (e.g., as a gapmer) so as to induce RNaseH-mediated cleavage of its target RNA in cells or (e.g., as a mixmer) so as to inhibit translation of the target mRNA in cells. ASOs for use herein may be modified in any suitable manner known in the art including, for example, as shown in U.S. Pat. No. 9,567,587 (including, e.g., length, sugar moieties of the nucleobase (pyrimidine, purine), and alterations of the heterocyclic portion of the nucleobase). Further, ASOs have been used for decades to reduce expression of specific target genes (see, e.g., Bennett et al. (2017) Annu. Rev. Pharmacol. 57:81-105).

iv. Double-Stranded Oligonucleotides

The disclosure provides double-stranded (ds) oligonucleotides for targeting LPA mRNA and inhibiting LPA expression (e.g., via the RNAi pathway) comprising a sense strand (also referred to herein as a passenger strand) and an antisense strand (also referred to herein as a guide strand). In some embodiments, the sense strand and antisense strand are separate strands and are not covalently linked. In some embodiments, the sense strand and antisense strand are covalently linked.

In some embodiments, the sense strand has a first region (R1) and a second region (R2), wherein R2 comprises a first subregion (S1), a tetraloop (L) or triloop (triL), and a second subregion (S2), wherein L or triL is located between S1 and S2, and wherein S1 and S2 form a second duplex (D2). D2 may have various lengths. In some embodiments, D2 is about 1-6 bp in length. In some embodiments, D2 is 2-6, 3-6, 4-6, 5-6, 1-5, 2-5, 3-5 or 4-5 bp in length. In some embodiments, D2 is 1, 2, 3, 4, 5 or 6 bp in length. In some embodiments, D2 is 6 bp in length.

In some embodiments, R1 of the sense strand and the antisense strand form a first duplex (D1). In some embodiments, D1 is at least about 15 (e.g., at least 15, at least 16, at least 17, at least 18, at least 19, at least 20 or at least 21) nucleotides in length. In some embodiments, D1 is in the range of about 12 to 30 nucleotides in length (e.g., 12 to 30, 12 to 27, 15 to 22, 18 to 22, 18 to 25, 18 to 27, 18 to 30 or 21 to 30 nucleotides in length). In some embodiments, D1 is at least 12 nucleotides in length (e.g., at least 12, at least 15, at least 20, at least 25, or at least 30 nucleotides in length). In some embodiments, D1 is 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29 or 30 nucleotides in length. In some embodiments, D1 is 20 nucleotides in length. In some embodiments, D1 comprising sense strand and antisense strand does not span the entire length of the sense strand and/or antisense strand. In some embodiments, D1 comprising the sense strand and antisense strand spans the entire length of either the sense strand or antisense strand or both. In certain embodiments, D1 comprising the sense strand and antisense strand spans the entire length of both the sense strand and the antisense strand.

In some embodiments, a ds oligonucleotide herein comprises a sense strand having a sequence of any one of SEQ ID NOs: 388-403 and an antisense strand comprising a complementary sequence selected from SEQ ID NOs: 788-803, as is arranged Table 3. In some embodiments, the sense strand comprises the sequence of SEQ ID NO: 393 and the antisense strand comprises the sequence of SEQ ID NO: 793.

It should be appreciated that, in some embodiments, sequences presented in the Sequence Listing may be referred to in describing the structure of an oligonucleotide (e.g., a ds oligonucleotide) or other nucleic acid. In such embodiments, the actual oligonucleotide or other nucleic acid may have one or more alternative nucleotides (e.g., an RNA counterpart of a DNA nucleotide or a DNA counterpart of an RNA nucleotide) and/or one or more modified nucleotides and/or one or more modified internucleotide linkages and/or one or more other modification when compared with the specified sequence while retaining essentially same or similar complementary properties as the specified sequence.

In some embodiments, a ds oligonucleotide herein comprises a 25-nucleotide sense strand and a 27-nucleotide antisense strand that when acted upon by a Dicer enzyme results in an antisense strand that is incorporated into the mature RISC. In some embodiments, the sense strand of the ds oligonucleotide is longer than 27 nucleotides (e.g., 28, 29, 30, 31, 32, 33, 34, 35, 36, 37, 38, 39 or 40 nucleotides). In some embodiments, the sense strand of the ds oligonucleotide is longer than 25 nucleotides (e.g., 26, 27, 28, 29 or 30 nucleotides).

In some embodiments, the ds oligonucleotides herein have one 5′ end that is thermodynamically less stable when compared to the other 5′ end. In some embodiments, an asymmetric ds oligonucleotide is provided that comprises a blunt end at the 3′ end of a sense strand and a 3′-overhang at the 3′ end of an antisense strand. In some embodiments, the 3′-overhang on the antisense strand is about 1-8 nucleotides in length (e.g., 1, 2, 3, 4, 5, 6, 7 or 8 nucleotides in length). Typically, a ds oligonucleotide for RNAi has a two-nucleotide overhang on the 3′ end of the antisense (guide) strand. However, other overhangs are possible. In some embodiments, an overhang is a 3′-overhang comprising a length of between 1 and 6 nucleotides, optionally 1 to 5, 1 to 4, 1 to 3, 1 to 2, 2 to 6, 2 to 5, 2 to 4, 2 to 3, 3 to 6, 3 to 5, 3 to 4, 4 to 6, 4 to 5, 5 to 6 nucleotides, or 1, 2, 3, 4, 5 or 6 nucleotides. However, in some embodiments, the overhang is a 5′-overhang comprising a length of between 1 and 6 nucleotides, optionally 1 to 5, 1 to 4, 1 to 3, 1 to 2, 2 to 6, 2 to 5, 2 to 4, 2 to 3, 3 to 6, 3 to 5, 3 to 4, 4 to 6, 4 to 5, 5 to 6 nucleotides, or 1, 2, 3, 4, 5 or 6 nucleotides.

In some embodiments, two terminal nucleotides on the 3′ end of an antisense strand are modified. In some embodiments, the two terminal nucleotides on the 3′ end of the antisense strand are complementary with the target mRNA (e.g., LPA mRNA). In some embodiments, the two terminal nucleotides on the 3′ end of the antisense strand are not complementary with the target mRNA. In some embodiments, two terminal nucleotides on each 3′ end of an oligonucleotide in the nicked tetraloop structure are GG. Typically, one or both of the two terminal GG nucleotides on each 3′ end of a ds oligonucleotide is not complementary with the target mRNA.

In some embodiments, there is one or more (e.g., 1, 2, 3, 4 or 5) mismatch(s) between a sense and antisense strand. If there is more than one mismatch between a sense and antisense strand, they may be positioned consecutively (e.g., 2, 3 or more in a row), or interspersed throughout the region of complementarity. In some embodiments, the 3′ end of the sense strand contains one or more mismatches. In one embodiment, two mismatches are incorporated at the 3′ end of the sense strand. In some embodiments, base mismatches, or destabilization of segments at the 3′ end of the sense strand of the oligonucleotide improves or increases the potency of the ds oligonucleotide.

a. Antisense Strands

In some embodiments, an oligonucleotide (e.g., ads oligonucleotide) disclosed herein for targeting LPA mRNA and inhibiting LPA expression comprises an antisense strand comprising or consisting of a sequence as set forth in any one of SEQ ID NOs: 404-803. In some embodiments, an oligonucleotide herein comprises an antisense strand comprising or consisting of at least about 12 (e.g., at least 12, at least 13, at least 14, at least 15, at least 16, at least 17, at least 18, at least 19, at least 20, at least 21, at least 22 or at least 23) contiguous nucleotides of a sequence as set forth in any one of SEQ ID NOs: 404-803.

In some embodiments, an oligonucleotide (e.g., a ds oligonucleotide) herein comprises an antisense strand of up to about 40 nucleotides in length (e.g., up to 40, up to 35, up to 30, up to 27, up to 25, up to 21, up to 19, up to 17 or up to 12 nucleotides in length). In some embodiments, an oligonucleotide may have an antisense strand of at least about 12 nucleotides in length (e.g., at least 12, at least 15, at least 19, at least 21, at least 22, at least 25, at least 27, at least 30, at least 35 or at least 38 nucleotides in length). In some embodiments, an oligonucleotide may have an antisense strand in a range of about 12 to about 40 (e.g., 12 to 40, 12 to 36, 12 to 32, 12 to 28, 15 to 40, 15 to 36, 15 to 32, 15 to 28, 17 to 22, 17 to 25, 19 to 27, 19 to 30, 20 to 40, 22 to 40, 25 to 40 or 32 to 40) nucleotides in length. In some embodiments, an oligonucleotide may have an antisense strand of 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 or 40 nucleotides in length.

In some embodiments, an antisense strand of an oligonucleotide is referred to as a “guide strand.” For example, an antisense strand that engages with RNA-induced silencing complex (RISC) and binds to an Argonaute protein such as Ago2, or engages with or binds to one or more similar factors, and directs silencing of a target gene, the antisense strand is referred to as a guide strand. In some embodiments, a sense strand complementary to a guide strand is referred to as a “passenger strand.”

b. Sense Strands

In some embodiments, an oligonucleotide (e.g., a ds oligonucleotide) herein for targeting LPA mRNA and inhibiting LPA expression comprises or consists of a sense strand sequence as set forth in in any one of SEQ ID NOs: 4-403. In some embodiments, an oligonucleotide has a sense strand that comprises or consists of at least about 12 (e.g., at least 13, at least 14, at least 15, at least 16, at least 17, at least 18, at least 19, at least 20, at least 21, at least 22 or at least 23) contiguous nucleotides of a sequence as set forth in in any one of SEQ ID NOs: 4-403.

In some embodiments, an oligonucleotide (e.g., a ds oligonucleotide) herein comprises a sense strand (or passenger strand) of up to about 40 nucleotides in length (e.g., up to 40, up to 36, up to 30, up to 27, up to 25, up to 21, up to 19, up to 17 or up to 12 nucleotides in length). In some embodiments, an oligonucleotide may have a sense strand of at least about 12 nucleotides in length (e.g., at least 12, at least 15, at least 19, at least 21, at least 25, at least 27, at least 30, at least 36 or at least 38 nucleotides in length). In some embodiments, an oligonucleotide may have a sense strand in a range of about 12 to about 40 (e.g., 12 to 40, 12 to 36, 12 to 32, 12 to 28, 15 to 40, 15 to 36, 15 to 32, 15 to 28, 17 to 21, 17 to 25, 19 to 27, 19 to 30, 20 to 40, 22 to 40, 25 to 40 or 32 to 40) nucleotides in length. In some embodiments, an oligonucleotide may have a sense strand of 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 or 40 nucleotides in length.

In some embodiments, a sense strand comprises a stem-loop structure at its 3′ end. In some embodiments, a sense strand comprises a stem-loop structure at its 5′ end. In some embodiments, a stem is a duplex of 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13 or 14 bp in length. In some embodiments, a stem-loop provides the oligonucleotide protection against degradation (e.g., enzymatic degradation) and facilitates or improves targeting and/or delivery to a target cell, tissue, or organ (e.g, the liver), or both. For example, in some embodiments, the loop of a stem-loop provides nucleotides comprising one or more modifications that facilitate, improve, or increase targeting to a target mRNA (e.g., an LPA mRNA), inhibition of target gene expression (e.g., LPA expression), and/or delivery to a target cell, tissue, or organ (e.g., the liver), or both. In some embodiments, the stem-loop itself or modification(s) to the stem-loop do not substantially affect the inherent gene expression inhibition activity of the oligonucleotide, but facilitates, improves, or increases stability (e.g., provides protection against degradation) and/or delivery of the oligonucleotide to a target cell, tissue, or organ (e.g., the liver). In certain embodiments, an oligonucleotide comprises a sense strand comprising (e.g., at its 3′ end) a stem-loop set forth as: S1-L-S2, in which S1 is complementary to S2, and in which L forms a single-stranded loop between S1 and S2 of up to about 10 nucleotides in length (e.g., 3, 4, 5, 6, 7, 8, 9 or 10 nucleotides in length). In some embodiments, the loop (L) is 4 nucleotides in length. FIG. 10 depicts a non-limiting example of such an oligonucleotide. In some embodiments, a loop (L) of a stem-loop having the structure S1-L-S2 as described above is a tetraloop (e.g., within a nicked tetraloop structure). In some embodiments, the tetraloop comprises ribonucleotides, deoxyribonucleotides, modified nucleotides, delivery ligands, and combinations thereof.

v. Oligonucleotide Modifications

a. Sugar Modifications

In some embodiments, a modified sugar (also referred herein to a sugar analog) includes a modified deoxyribose or ribose moiety in which, for example, one or more modifications occur at the 2′, 3′, 4′ and/or 5′ carbon position of the sugar. In some embodiments, a modified sugar may also include non-natural alternative carbon structures such as those present in locked nucleic acids (“LNA”; see, e.g., Koshkin et al. (1998) TETRAHEDON 54:3607-30), unlocked nucleic acids (“UNA”; see, e.g., Snead et al. (2013) MOL. THER-NUCL. ACIDS 2:e103) and bridged nucleic acids (“BNA”; see, e.g., Imanishi & Obika (2002) CHEM COMMUN. (CAMB) 21:1653-59).

In some embodiments, a nucleotide modification in a sugar comprises a 2′-modification. In some embodiments, a 2′-modification may be 2′-O-propargyl, 2′-O-propylamin, 2′-amino, 2′-ethyl, 2′-fluoro (2′-F), 2′-aminoethyl (EA), 2′-O-methyl (2′-OMe), 2′-O-methoxyethyl (2′-MOE), 2′-O-[2-(methylamino)-2-oxoethyl] (2′-O-NMA) or 2′-deoxy-2′-fluoro-β-d-arabinonucleic acid (2′-FANA). In some embodiments, the modification is 2′-F, 2′-OMe or 2′-MOE. In some embodiments, a modification in a sugar comprises a modification of the sugar ring, which may comprise modification of one or more carbons of the sugar ring. For example, a modification of a sugar of a nucleotide may comprise a 2′-oxygen of a sugar is linked to a 1′-carbon or 4′-carbon of the sugar, or a 2′-oxygen is linked to the 1′-carbon or 4′-carbon via an ethylene or methylene bridge. In some embodiments, a modified nucleotide has an acyclic sugar that lacks a 2′-carbon to 3′-carbon bond. In some embodiments, a modified nucleotide has a thiol group, e.g., in the 4′ position of the sugar.

In some embodiments, the oligonucleotide described herein comprises at least about 1 modified nucleotide (e.g., at least 1, at least 5, at least 10, at least 15, at least 20, at least 25, at least 30, at least 35, at least 40, at least 45, at least 50, at least 55, at least 60, or more). In some embodiments, the sense strand of the oligonucleotide comprises at least about 1 modified nucleotide (e.g., at least 1, at least 5, at least 10, at least 15, at least 20, at least 25, at least 30, at least 35, or more). In some embodiments, the antisense strand of the oligonucleotide comprises at least about 1 modified nucleotide (e.g., at least 1, at least 5, at least 10, at least 15, at least 20, or more).

In some embodiments, all the nucleotides of the sense strand of the oligonucleotide are modified. In some embodiments, all the nucleotides of the antisense strand of the oligonucleotide are modified. In some embodiments, all the nucleotides of the oligonucleotide (i.e., both the sense strand and the antisense strand) are modified. In some embodiments, the modified nucleotide comprises a 2′-modification (e.g., a 2′-F or 2′-OMe, 2′-MOE, and 2′-deoxy-2′-fluoro-β-d-arabinonucleic acid). In some embodiments, the modified nucleotide comprises a 2′-modification (e.g., a 2′-F or 2′-OMe)

The disclosure provides oligonucleotides having different modification patterns. In some embodiments, the modified oligonucleotides comprise a sense strand sequence having a modification pattern as set forth in any one of Tables 3 and 4 (as well as FIG. 10) and an antisense strand having a modification pattern as set forth in any one of Tables 3 and 4 (as well as FIG. 10). In some embodiments, for these oligonucleotides, one or more of positions 8, 9, 10 or 11 of the sense strand is modified with a 2′—F group. In other embodiments, for these oligonucleotides, the sugar moiety at each of nucleotides at positions 1-7 and 12-20 in the sense strand is modified with a 2′-OMe.

In some embodiments, the antisense strand has 3 nucleotides that are modified at the 2′-position of the sugar moiety with a 2′-F. In some embodiments, the sugar moiety at positions 2, 5 and 14 and optionally up to 3 of the nucleotides at positions 1, 3, 7 and 10 of the antisense strand are modified with a 2′-F. In other embodiments, the sugar moiety at each of the positions at positions 2, 5 and 14 of the antisense strand is modified with the 2′-F. In other embodiments, the sugar moiety at each of the positions at positions 1, 2, 5 and 14 of the antisense strand is modified with the 2′-F. In still other embodiments, the sugar moiety at each of the positions at positions 1, 2, 3, 5, 7 and 14 of the antisense strand is modified with the 2′-F. In yet another embodiment, the sugar moiety at each of the positions at positions 1, 2, 3, 5, 10 and 14 of the antisense strand is modified with the 2′-F. In another embodiment, the sugar moiety at each of the positions at positions 2, 3, 5, 7, 10 and 14 of the antisense strand is modified with the 2′-F.

b. 5′ Terminal Phosphates

In some embodiments, 5′-terminal phosphate groups of an RNAi oligonucleotide enhance the interaction with Ago2. However, oligonucleotides comprising a 5′-phosphate group may be susceptible to degradation via phosphatases or other enzymes, which can limit their bioavailability in vivo. In some embodiments, an oligonucleotide (e.g., a ds oligonucleotide) herein includes analogs of 5′ phosphates that are resistant to such degradation. In some embodiments, the phosphate analog is oxymethylphosphonate, vinylphosphonate or malonyl phosphonate, or a combination thereof. In certain embodiments, the 3′ end of an oligonucleotide strand is attached to chemical moiety that mimics the electrostatic and steric properties of a natural 5′-phosphate group (“phosphate mimic”).

In some embodiments, an oligonucleotide has a phosphate analog at a 4′-carbon position of the sugar (referred to as a “4′-phosphate analog”). See, e.g., Intl. Patent Application Publication No. WO 2018/045317. In some embodiments, an oligonucleotide herein comprises a 4′-phosphate analog at a 5′-terminal nucleotide. In some embodiments, a phosphate analog is an oxymethylphosphonate, in which the oxygen atom of the oxymethyl group is bound to the sugar moiety (e.g., at its 4′-carbon) or analog thereof. In other embodiments, a4′-phosphate analog is a thiomethylphosphonate or an aminomethylphosphonate, in which the sulfur atom of the thiomethyl group or the nitrogen atom of the amino methyl group is bound to the 4′-carbon of the sugar moiety or analog thereof. In certain embodiments, a 4′-phosphate analog is an oxymethylphosphonate. In some embodiments, an oxymethylphosphonate is represented by the formula —O—CH₂—PO(OH)₂or —O—CH₂—PO(OR)₂, in which R is independently selected from H, CH₃, an alkyl group, CH₂CH₂CN, CH₂OCOC(CH₃)₃, CH₂OCH₂CH₂Si(CH₃)₃or a protecting group. In certain embodiments, the alkyl group is CH₂CH₃. More typically, R is independently selected from H, CH₃or CH₂CH₃.

c. Modified Intranucleoside Linkages

In some embodiments, an oligonucleotide comprises a modified internucleoside linkage. In some embodiments, phosphate modifications or substitutions result in an oligonucleotide that comprises at least about 1 (e.g., at least 1, at least 2, at least 3 or at least 5) modified internucleotide linkage. In some embodiments, any one of the oligonucleotides disclosed herein comprises about 1 to about 10 (e.g., 1 to 10, 2 to 8, 4 to 6, 3 to 10, 5 to 10, 1 to 5, 1 to 3 or 1 to 2) modified internucleotide linkages. In some embodiments, any one of the oligonucleotides disclosed herein comprises 1, 2, 3, 4, 5, 6, 7, 8, 9 or 10 modified internucleotide linkages.

A modified internucleotide linkage may be a phosphorodithioate linkage, a phosphorothioate linkage, a phosphotriester linkage, a thionoalkylphosphonate linkage, a thionalkylphosphotriester linkage, a phosphoramidite linkage, a phosphonate linkage or a boranophosphate linkage. In some embodiments, at least one modified internucleotide linkage of any one of the oligonucleotides as disclosed herein is a phosphorothioate linkage.

In some embodiments, the oligonucleotide described herein has a phosphorothioate linkage between one or more of positions 1 and 2 of the sense strand, positions 1 and 2 of the antisense strand, positions 2 and 3 of the antisense strand, positions 3 and 4 of the antisense strand, positions 20 and 21 of the antisense strand, and positions 21 and 22 of the antisense strand. In some embodiments, the oligonucleotide described herein has a phosphorothioate linkage between each of positions 1 and 2 of the sense strand, positions 1 and 2 of the antisense strand, positions 2 and 3 of the antisense strand, positions 20 and 21 of the antisense strand, and positions 21 and 22 of the antisense strand.

d. Base Modifications

In some embodiments, oligonucleotides herein have one or more modified nucleobases. In some embodiments, modified nucleobases (also referred to herein as base analogs) are linked at the 1′ position of a nucleotide sugar moiety. In certain embodiments, a modified nucleobase is a nitrogenous base. In certain embodiments, a modified nucleobase does not contain nitrogen atom. See, e.g., US Patent Application Publication No. 2008/0274462. In some embodiments, a modified nucleotide comprises a universal base. However, in certain embodiments, a modified nucleotide does not contain a nucleobase (abasic).

In some embodiments, a universal base is a heterocyclic moiety located at the 1′ position of a nucleotide sugar moiety in a modified nucleotide, or the equivalent position in a nucleotide sugar moiety substitution, that, when present in a duplex, can be positioned opposite more than one type of base without substantially altering structure of the duplex. In some embodiments, compared to a reference single-stranded nucleic acid (e.g., oligonucleotide) that is fully complementary to a target nucleic acid, a single-stranded nucleic acid containing a universal base forms a duplex with the target nucleic acid that has a lower T_mthan a duplex formed with the complementary nucleic acid. However, in some embodiments, when compared to a reference single-stranded nucleic acid in which the universal base has been replaced with a base to generate a single mismatch, the single-stranded nucleic acid containing the universal base forms a duplex with the target nucleic acid that has a higher T_mthan a duplex formed with the nucleic acid comprising the mismatched base.

Non-limiting examples of universal-binding nucleotides include, but are not limited to, inosine, 1-β-D-ribofuranosyl-5-nitroindole and/or 1-β-D-ribofuranosyl-3-nitropyrrole (see, US Patent Application Publication No. 2007/0254362; Van Aerschot et al. (1995) NUCLEIC ACIDS RES. 23:4363-70; Loakes et al. (1995) NUCLEIC ACIDS RES. 23:2361-66; and Loakes & Brown (1994) NUCLEIC ACIDS RES. 22:4039-43).

e. Reversible Modifications

While certain modifications to protect an oligonucleotide from the in vivo environment before reaching target cells can be made, they can reduce the potency or activity of the oligonucleotide once it reaches the cytosol of the target cell. Reversible modifications can be made such that the molecule retains desirable properties outside of the cell, which are then removed upon entering the cytosolic environment of the cell. Reversible modification can be removed, for example, by the action of an intracellular enzyme or by the chemical conditions inside of a cell (e.g., through reduction by intracellular glutathione).

In some embodiments, a reversibly modified nucleotide comprises a glutathione-sensitive moiety. Typically, nucleic acid molecules have been chemically modified with cyclic disulfide moieties to mask the negative charge created by the internucleotide diphosphate linkages and improve cellular uptake and nuclease resistance. See US Patent Application Publication No. 2011/0294869, Intl. Patent Application Publication Nos. WO 2014/088920 and WO 2015/188197, and Meade et al. (2014) NAT. BIOTECHNOL. 32:1256-63. This reversible modification of the internucleotide diphosphate linkages is designed to be cleaved intracellularly by the reducing environment of the cytosol (e.g. glutathione). Earlier examples include neutralizing phosphotriester modifications that were reported to be cleavable inside cells (see, Dellinger et al. (2003) J. AM. CHEM. SOC. 125:940-50).

In some embodiments, such a reversible modification allows protection during in vivo administration (e.g., transit through the blood and/or lysosomal/endosomal compartments of a cell) where the oligonucleotide will be exposed to nucleases and other harsh environmental conditions (e.g., pH). When released into the cytosol of a cell where the levels of glutathione are higher compared to extracellular space, the modification is reversed, and the result is a cleaved oligonucleotide. Using reversible, glutathione-sensitive moieties, it is possible to introduce sterically larger chemical groups into the oligonucleotide of interest when compared to the options available using irreversible chemical modifications. This is because these larger chemical groups will be removed in the cytosol and, therefore, should not interfere with the biological activity of the oligonucleotides inside the cytosol of a cell. As a result, these larger chemical groups can be engineered to confer various advantages to the nucleotide or oligonucleotide, such as nuclease resistance, lipophilicity, charge, thermal stability, specificity and reduced immunogenicity. In some embodiments, the structure of the glutathione-sensitive moiety can be engineered to modify the kinetics of its release.

In some embodiments, a glutathione-sensitive moiety is attached to the sugar of the nucleotide. In some embodiments, a glutathione-sensitive moiety is attached to the 2′-carbon of the sugar of a modified nucleotide. In some embodiments, the glutathione-sensitive moiety is located at the 5′-carbon of a sugar, particularly when the modified nucleotide is the 5′-terminal nucleotide of the oligonucleotide. In some embodiments, the glutathione-sensitive moiety is located at the 3′-carbon of sugar, particularly when the modified nucleotide is the 3′-terminal nucleotide of the oligonucleotide. In some embodiments, the glutathione-sensitive moiety comprises a sulfonyl group. See, e.g., U.S. Provisional Patent Application No. 62/378,635, entitled Compositions Comprising Reversibly Modified Oligonucleotides and Uses Thereof, which was filed on Aug. 23, 2016.

vi. Targeting Ligands

In some embodiments, it is desirable to target the oligonucleotides of the disclosure to one or more cells or one or more organs. Such a strategy can help to avoid undesirable effects in other organs or avoid undue loss of the oligonucleotide to cells, tissue or organs that would not benefit from the oligonucleotide. Accordingly, in some embodiments, oligonucleotides disclosed herein are modified to facilitate targeting and/or delivery to a tissue, cell or organ (e.g., to facilitate delivery of the oligonucleotide to the liver). In certain embodiments, oligonucleotides disclosed herein are modified to facilitate delivery of the oligonucleotide to the hepatocytes of the liver. In some embodiments, an oligonucleotide comprises at least one nucleotide (e.g., 1, 2, 3, 4, 5, 6 or more nucleotides) conjugated to one or more targeting ligand(s).

In some embodiments, the targeting ligand comprises a carbohydrate, amino sugar, cholesterol, peptide, polypeptide, protein or part of a protein (e.g., an antibody or antibody fragment), or lipid. In some embodiments, the targeting ligand is an aptamer. For example, a targeting ligand may be an RGD peptide that is used to target tumor vasculature or glioma cells, CREKA peptide to target tumor vasculature or stoma, transferring, lactoferrin, or an aptamer to target transferrin receptors expressed on CNS vasculature, or an anti-EGFR antibody to target EGFR on glioma cells. In certain embodiments, the targeting ligand is one or more GalNAc moieties.

In some embodiments, 1 or more (e.g., 1, 2, 3, 4, 5 or 6) nucleotides of an oligonucleotide are each conjugated to a separate targeting ligand. In some embodiments, 2 to 4 nucleotides of an oligonucleotide are each conjugated to a separate targeting ligand. In some embodiments, targeting ligands are conjugated to 2 to 4 nucleotides at either ends of the sense or antisense strand (e.g., targeting ligands are conjugated to a 2 to 4 nucleotide overhang or extension on the 5′ or 3′ end of the sense or antisense strand) such that the targeting ligands resemble bristles of a toothbrush and the oligonucleotide resembles a toothbrush. For example, an oligonucleotide may comprise a stem-loop at either the 5′ or 3′ end of the sense strand and 1, 2, 3 or 4 nucleotides of the loop of the stem may be individually conjugated to a targeting ligand. In some embodiments, an oligonucleotide (e.g., a ds oligonucleotide) provided by the disclosure comprises a stem-loop at the 3′ end of the sense strand, wherein the loop of the stem-loop comprises a triloop or a tetraloop, and wherein the 3 or 4 nucleotides comprising the triloop or tetraloop, respectfully, are individually conjugated to a targeting ligand.

GalNAc is a high affinity ligand for the ASGPR, which is primarily expressed on the sinusoidal surface of hepatocyte cells and has a major role in binding, internalizing and subsequent clearing circulating glycoproteins that contain terminal galactose or GalNAc residues (asialoglycoproteins). Conjugation (either indirect or direct) of GalNAc moieties to oligonucleotides of the instant disclosure can be used to target these oligonucleotides to the ASGPR expressed on cells. In some embodiments, an oligonucleotide of the instant disclosure is conjugated to at least one or more GalNAc moieties, wherein the GalNAc moieties target the oligonucleotide to an ASGPR expressed on human liver cells (e.g. human hepatocytes). In some embodiments, the GalNAc moiety target the oligonucleotide to the liver.

In some embodiments, an oligonucleotide of the instant disclosure is conjugated directly or indirectly to a monovalent GalNAc. In some embodiments, the oligonucleotide is conjugated directly or indirectly to more than one monovalent GalNAc (i.e., is conjugated to 2, 3 or 4 monovalent GalNAc moieties, and is typically conjugated to 3 or 4 monovalent GalNAc moieties). In some embodiments, an oligonucleotide is conjugated to one or more bivalent GalNAc, trivalent GalNAc or tetravalent GalNAc moieties.

In some embodiments, 1 or more (e.g., 1, 2, 3, 4, 5 or 6) nucleotides of an oligonucleotide are each conjugated to a GalNAc moiety. In some embodiments, 2 to 4 nucleotides of a tetraloop are each conjugated to a separate GalNAc. In some embodiments, 1 to 3 nucleotides of a triloop are each conjugated to a separate GalNAc. In some embodiments, targeting ligands are conjugated to 2 to 4 nucleotides at either ends of the sense or antisense strand (e.g., ligands are conjugated to a 2 to 4 nucleotide overhang or extension on the 5′ or 3′ end of the sense or antisense strand) such that the GalNAc moieties resemble bristles of a toothbrush and the oligonucleotide resembles a toothbrush. In some embodiments, GalNAc moieties are conjugated to a nucleotide of the sense strand. For example, 4 GalNAc moieties can be conjugated to nucleotides in the tetraloop of the sense strand where each GalNAc moiety is conjugated to 1 nucleotide.

In some embodiments, an oligonucleotide herein comprises a monovalent GalNAc attached to a guanine nucleotide referred to as [ademG-GalNAc] or 2′-aminodiethoxymethanol-Guanine-GalNAc, as depicted below:

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In some embodiments, an oligonucleotide herein comprises a monovalent GalNAc attached to an adenine nucleotide, referred to as [ademA-GalNAc] or 2′-aminodiethoxymethanol-Adenine-GalNAc, as depicted below:

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An example of such conjugation is shown below for a loop comprising from 5′ to 3′ the nucleotide sequence GAAA (L=linker, X=heteroatom) stem attachment points are shown. Such a loop may be present, for example, at positions 27-30 of the sense strand listed in Table 5 and as shown in FIG. 3. In the chemical formula,

embedded image

is used to describe an attachment point to the oligonucleotide strand.

embedded image

Appropriate methods or chemistry (e.g., click chemistry) can be used to link a targeting ligand to a nucleotide. In some embodiments, a targeting ligand is conjugated to a nucleotide using a click linker. In some embodiments, an acetal-based linker is used to conjugate a targeting ligand to a nucleotide of any one of the oligonucleotides described herein. Acetal-based linkers are disclosed, for example, in Intl. Patent Application Publication No. WO 2016/100401. In some embodiments, the linker is a labile linker. However, in other embodiments, the linker is stable. An example is shown below for a loop comprising from 5′ to 3′ the nucleotides GAAA, in which GalNAc moieties are attached to nucleotides of the loop using an acetal linker. Such a loop may be present, for example, at positions 27-30 of the any one of the sense strand listed in Tables 3 or 4 and as shown in FIG. 10. In the chemical formula,

embedded image

is an attachment point to the oligonucleotide strand.

embedded image

As mentioned, various appropriate methods or chemistry synthetic techniques (e.g., click chemistry) can be used to link a targeting ligand to a nucleotide. In some embodiments, a targeting ligand is conjugated to a nucleotide using a click linker. In some embodiments, an acetal-based linker is used to conjugate a targeting ligand to a nucleotide of any one of the oligonucleotides described herein. Acetal-based linkers are disclosed, for example, in Intl. Patent Application Publication No. WO 2016/100401. In some embodiments, the linker is a labile linker. However, in other embodiments, the linker is a stable linker.

In some embodiments, a duplex extension (e.g., of up to 3, 4, 5 or 6 bp in length) is provided between a targeting ligand (e.g., a GalNAc moiety) and a ds oligonucleotide. In some embodiments, the oligonucleotides herein do not have a GalNAc conjugated thereto.

III. Formulations

Various formulations have been developed to facilitate oligonucleotide use. For example, oligonucleotides can be delivered to a subject or a cellular environment using a formulation that minimizes degradation, facilitates delivery and/or uptake, or provides another beneficial property to the oligonucleotides in the formulation. In some embodiments, an oligonucleotide is formulated in buffer solutions such as phosphate buffered saline solutions, liposomes, micellar structures and capsids.

Formulations of oligonucleotides with cationic lipids can be used to facilitate transfection of the oligonucleotides into cells. For example, cationic lipids, such as lipofectin, cationic glycerol derivatives, and polycationic molecules (e.g., polylysine, can be used. Suitable lipids include Oligofectamine, Lipofectamine (Life Technologies), NC388 (Ribozyme Pharmaceuticals, Inc., Boulder, Colo.), or FuGene 6 (Roche) all of which can be used according to the manufacturer's instructions.

Accordingly, in some embodiments, a formulation comprises a lipid nanoparticle. In some embodiments, an excipient comprises a liposome, a lipid, a lipid complex, a microsphere, a microparticle, a nanosphere or a nanoparticle, or may be otherwise formulated for administration to the cells, tissues, organs, or body of a subject in need thereof (see, e.g., Remington: THE SCIENCE AND PRACTICE OF PHARMACY, 22nd edition, Pharmaceutical Press, 2013).

In some embodiments, the formulations herein comprise an excipient. In some embodiments, an excipient confers to a composition improved stability, improved absorption, improved solubility and/or therapeutic enhancement of the active ingredient. In some embodiments, an excipient is a buffering agent (e.g., sodium citrate, sodium phosphate, a tris base, or sodium hydroxide) or a vehicle (e.g., a buffered solution, petrolatum, dimethyl sulfoxide or mineral oil). In some embodiments, an oligonucleotide is lyophilized for extending its shelf-life and then made into a solution before use (e.g., administration to a subject). Accordingly, an excipient in a composition comprising any one of the oligonucleotides described herein may be a lyoprotectant (e.g., mannitol, lactose, polyethylene glycol or polyvinylpyrrolidone) or a collapse temperature modifier (e.g., dextran, Ficoll™ or gelatin).

In some embodiments, a pharmaceutical composition is formulated to be compatible with its intended route of administration. Examples of routes of administration include parenteral (e.g., intravenous, intramuscular, intraperitoneal, intradermal, subcutaneous), oral (e.g., inhalation), transdermal (e.g., topical), transmucosal and rectal administration.

Pharmaceutical compositions suitable for injectable use include sterile aqueous solutions (where water soluble) or dispersions and sterile powders for the extemporaneous preparation of sterile injectable solutions or dispersion. For intravenous administration, suitable carriers include physiological saline, bacteriostatic water, Cremophor EL™ (BASF, Parsippany, N.J.) or phosphate buffered saline (PBS). The carrier can be a solvent or dispersion medium containing, for example, water, ethanol, polyol (e.g., glycerol, propylene glycol, and liquid polyethylene glycol, and the like), and suitable mixtures thereof. In many cases, it will be preferable to include isotonic agents, for example, sugars, polyalcohols such as mannitol, sorbitol, sodium chloride in the composition. Sterile injectable solutions can be prepared by incorporating the oligonucleotides in a required amount in a selected solvent with one or a combination of ingredients enumerated above, as required, followed by filtered sterilization.

In some embodiments, a composition may contain at least about 0.1% of the therapeutic agent or more, although the percentage of the active ingredient(s) may be between about 1% to about 80% or more of the weight or volume of the total composition. Factors such as solubility, bioavailability, biological half-life, route of administration, product shelf life, as well as other pharmacological considerations will be contemplated by one skilled in the art of preparing such pharmaceutical formulations, and as such, a variety of dosages and treatment regimens may be desirable.

Even though several embodiments are directed to liver-targeted delivery of any of the oligonucleotides herein, targeting of other tissues is also contemplated.

IV. Methods of Use

i. Reducing LPA Expression in Cells

The disclosure provides methods for contacting or delivering to a cell or population of cells an effective amount any of the oligonucleotides (e.g., a ds oligonucleotide) herein for purposes of reducing LPA expression. In some embodiments, a reduction of LPA expression is determined by measuring a reduction in the amount or level of LPA mRNA, apo(a) protein, or apo(a) activity in a cell. The methods can include the steps described herein, and these maybe be, but not necessarily, carried out in the sequence as described. Other sequences, however, also are conceivable. Moreover, individual or multiple steps bay be carried out either in parallel and/or overlapping in time and/or individually or in multiply repeated steps. Furthermore, the methods may include additional, unspecified steps.

Methods herein are useful in any appropriate cell type. In some embodiments, a cell is any cell that expresses mRNA (e.g., hepatocytes, macrophages, monocyte-derived cells, prostate cancer cells, cells of the brain, endocrine tissue, bone marrow, lymph nodes, lung, gall bladder, liver, duodenum, small intestine, pancreas, kidney, gastrointestinal tract, bladder, adipose and soft tissue and skin). In some embodiments, the cell is a primary cell obtained from a subject. In some embodiments, the primary cell has undergone a limited number of passages such that the cell substantially maintains is natural phenotypic properties. In some embodiments, a cell to which the oligonucleotide is delivered is ex vivo or in vitro (i.e., can be delivered to a cell in culture or to an organism in which the cell resides).

In some embodiments, the oligonucleotides herein are delivered to a cell or population of cells using a nucleic acid delivery method known in the art including, but not limited to, injection of a solution containing the oligonucleotide, bombardment by particles covered by the oligonucleotide, exposing the cell or population of cells to a solution containing the oligonucleotide, or electroporation of cell membranes in the presence of the oligonucleotide. Other methods known in the art for delivering oligonucleotides to cells may be used, such as lipid-mediated carrier transport, chemical-mediated transport, and cationic liposome transfection such as calcium phosphate, and others.

In some embodiments, reduction of LPA expression is determined by an assay or technique that evaluates one or more molecules, properties or characteristics of a cell or population of cells associated with LPA expression (e.g., using an LPA expression biomarker) or by an assay or technique that evaluates molecules that are directly indicative of LPA expression in a cell or population of cells (e.g., LPA mRNA or apo(a) protein). In some embodiments, the extent to which an oligonucleotide herein reduces LPA expression is evaluated by comparing LPA expression in a cell or population of cells contacted with the oligonucleotide to a control cell or population of cells (e.g., a cell or population of cells not contacted with the oligonucleotide or contacted with a control oligonucleotide). In some embodiments, a control amount or level of LPA expression in a control cell or population of cells is predetermined, such that the control amount or level need not be measured in every instance the assay or technique is performed. The predetermined level or value can take a variety of forms. In some embodiments, a predetermined level or value can be single cut-off value, such as a median or mean.

In some embodiments, contacting or delivering an oligonucleotide (e.g., a ds oligonucleotide) herein to a cell or a population of cells results in a reduction in LPA expression. In some embodiments, the reduction in LPA expression is relative to a control amount or level of LPA expression in cell or population of cells not contacted with the oligonucleotide or contacted with a control oligonucleotide. In some embodiments, the reduction in LPA expression is about 1% or lower, about 5% or lower, about 10% or lower, about 15% or lower, about 20% or lower, about 25% or lower, about 30% or lower, about 35% or lower, about 40% or lower, about 45% or lower, about 50% or lower, about 55% or lower, about 60% or lower, about 70% or lower, about 80% or lower, or about 90% or lower relative to a control amount or level of LPA expression. In some embodiments, the control amount or level of LPA expression is an amount or level of LPA mRNA and/or apo(a) protein in a cell or population of cells that has not been contacted with an oligonucleotide herein. In some embodiments, the effect of delivery of an oligonucleotide to a cell or population of cells according to a method herein is assessed after any finite period or amount of time (e.g., minutes, hours, days, weeks, months). For example, in some embodiments, LPA expression is determined in a cell or population of cells at least about 4 hours, about 8 hours, about 12 hours, about 18 hours, about 24 hours; or at least about 1 day, about 2 days, about 3 days, about 4 days, about 5 days, about 6 days, about 7 days, about 8 days, about 9 days, about 10 days, about 11 days, about 12 days, about 13 days, about 14 days, about 21 days, about 28 days, about 35 days, about 42 days, about 49 days, about 56 days, about 63 days, about 70 days, about 77 days, or about 84 days or more after contacting or delivering the oligonucleotide to the cell or population of cells. In some embodiments, LPA expression is determined in a cell or population of cells at least about 1 month, about 2 months, about 3 months, about 4 months, about 5 months, or about 6 months or more after contacting or delivering the oligonucleotide to the cell or population of cells.

In some embodiments, an oligonucleotide is delivered in the form of a transgene that is engineered to express in a cell the oligonucleotide or strands comprising the oligonucleotide (e.g., its sense and antisense strands). In some embodiments, an oligonucleotide is delivered using a transgene engineered to express any oligonucleotide disclosed herein. Transgenes may be delivered using viral vectors (e.g., adenovirus, retrovirus, vaccinia virus, poxvirus, adeno-associated virus or herpes simplex virus) or non-viral vectors (e.g., plasmids or synthetic mRNAs). In some embodiments, transgenes can be injected directly to a subject.

ii. Medical Use

The disclosure also provides oligonucleotides for use, or adaptable for use, to treat a subject (e.g., a human having a disease, disorder or condition associated with LPA expression) that would benefit from reducing LPA expression. In some embodiments, the disclosure provides oligonucleotides for use, or adapted for use, to treat a subject having a disease, disorder or condition associated with expression of LPA. The disclosure also provides oligonucleotides for use, or adaptable for use, in the manufacture of a medicament or pharmaceutical composition for treating a disease, disorder or condition associated with LPA expression. In some embodiments, the oligonucleotides for use, or adaptable for use, target LPA mRNA and reduce LPA expression (e.g., via the RNAi pathway). In some embodiments, the oligonucleotides for use, or adaptable for use, target LPA mRNA and reduce the amount or level of LPA mRNA, apo(a) protein and/or apo (a) activity.

In addition, in some embodiments of the methods herein, a subject having a disease, disorder or condition associated with LPA expression or is predisposed to the same is selected for treatment with an oligonucleotide (e.g., a ds oligonucleotide) herein. In some embodiments, the method comprises selecting an individual having a marker (e.g., a biomarker) for a disease, disorder or condition associated with LPA expression, or predisposed to the same, such as, but not limited to, LPA mRNA, apo(a) protein, lipoprotein(a), or a combination thereof. Likewise, and as detailed below, some embodiments of the methods provided by the disclosure include steps such as measuring or obtaining a baseline value for a marker of LPA expression (e.g., lipoprotein(a)), and then comparing such obtained value to one or more other baseline values or values obtained after the subject is administered the oligonucleotide to assess the effectiveness of treatment.

iii. Methods of Treatment

The disclosure also provides methods of treating a subject having, suspected of having, or at risk of developing a disease, disorder or condition associated with LPA expression with an oligonucleotide herein. In some embodiments, the disclosure provides methods of treating or attenuating the onset or progression of a disease, disorder or condition associated with LPA expression using the oligonucleotides herein. In other embodiments, the disclosure provides methods to achieve one or more therapeutic benefits in a subject having a disease, disorder or condition associated with LPA expression using the oligonucleotides herein. In some embodiments of the methods herein, the subject is treated by administering a therapeutically effective amount of any one or more of the oligonucleotides herein. In some embodiments, treatment comprises reducing LPA expression. In some embodiments, the subject is treated therapeutically. In some embodiments, the subject is treated prophylactically.

In some embodiments of the methods herein, an oligonucleotide herein, or a pharmaceutical composition comprising the oligonucleotide, is administered to a subject having a disease, disorder or condition associated with LPA expression such that LPA expression is reduced in the subject, thereby treating the subject. In some embodiments, an amount or level of LPA mRNA is reduced in the subject. In some embodiments, an amount or level of apo(a) protein is reduced in the subject. In some embodiments, an amount or level of lipoprotein(a) is reduced in the subject. In some embodiments, an amount or level of apo(a) activity is reduced in the subject. In some embodiments, an amount or level of triglyceride (TG) (e.g., one or more TG(s) or total TGs) is reduced in the subject. In some embodiments, an amount or level of cholesterol (e.g., total cholesterol, LDL cholesterol, and/or HDL cholesterol) is reduced in the subject. In some embodiments, an amount or level of low-density lipoprotein (LDL) cholesterol is reduced in the subject. In some embodiments, an amount or activity of OxPL is reduced or altered in the subject. In some embodiments, an amount or activity of LDL-C is reduced or altered in the subject. In some embodiments, an amount or activity of apoB-100 is reduced or altered in the subject. In some embodiments, any combination of the following is reduced or altered in the subject: LPA expression, an amount or level of LPA mRNA, an amount or level of apo(a) protein, an amount or level of apo(a) activity, an amount or level of TG, an amount or level of cholesterol, an amount or activity of OxPL, an amount or activity of LDL-C, and/or an amount or activity of apoB-100.

Lipoprotein(a) levels range widely in human adults with plasma levels ranging from <0.1 mg/dL to >200 mg/dL, thus exhibiting up to three orders of magnitude difference among individuals (Schmidt et al., (2016) J Lipid Res. 57(8):1339-1359). Lipoprotein(a) levels <30 mg/dl are considered optimal in the United States and Canada (Anderson et al., (2016) CAN J CARDIOL 32:1263-82). The European Atherosclerosis Society (EAS) has proposed <50 mg/dL as optimal, and lipoprotein(a) levels >60 mg/dl are used as a cutoff for the reimbursement of apheresis in Germany and the United Kingdom (Tsimikas (2017) J AM COLL CARDIOL. 69(6):692-711). In some embodiments, a subject selected for treatment or treated with an oligonucleotide herein is identified or determined to have an amount or level of lipoprotein(a) of about 30 mg/dL or greater. In some embodiments, a subject selected for treatment or treated with an oligonucleotide herein is identified or determined to have an amount or level of lipoprotein(a) of >30 mg/dL. In some embodiments, a subject selected for treatment or treated with an oligonucleotide herein is identified or determined to have an amount or level of lipoprotein(a) of about 50 mg/dL or greater. In some embodiments, a subject selected for treatment or treated with an oligonucleotide herein is identified or determined to have an amount or level of lipoprotein(a) of about 60 mg/dL or greater. In some embodiments, a subject selected for treatment or treated with an oligonucleotide herein is identified or determined to have an amount or level of lipoprotein(a) in the range of 30 mg/dL to 300 mg/dL.

Generally, a normal or desirable TG range for a human patient is <150 mg/dL of blood, with <100 being considered ideal. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of TG of ≥150 mg/dL. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of TG in the range of 150 to 199 mg/dL, which is considered borderline high TG levels. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of TG in the range of 200 to 499 mg/dL, which is considered high TG levels. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of TG in the range of 500 mg/dL or higher (i.e., ≥500 mg/dL), which is considered very high TG levels. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of TG which is ≥150 mg/dL, ≥200 mg/dL or ≥500 mg/dL. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount of level of TG of 200 to 499 mg/dL, or 500 mg/dL or higher. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of TG which is ≥200 mg/dL.

In some embodiments of the methods herein, an oligonucleotide herein, or a pharmaceutical composition comprising the oligonucleotide, is administered to a subject having a disease, disorder or condition associated with LPA expression such that an amount or level of cholesterol (e.g., total cholesterol, LDL cholesterol, and/or HDL cholesterol) is reduced in the subject by at least about 30%, about 35%, about 40%, about 45%, about 50%, about 55%, about 60%, about 65%, about 70%, about 75%, about 80%, about 85%, about 90%, about 95%, about 99% or greater than 99% when compared to the amount or level of cholesterol prior to administration of the oligonucleotide or pharmaceutical composition. In some embodiments, an amount or level of cholesterol is reduced in the subject by at least about 30%, about 35%, about 40%, about 45%, about 50%, about 55%, about 60%, about 65%, about 70%, about 75%, about 80%, about 85%, about 90%, about 95%, about 99% or greater than 99% when compared to an amount or level of cholesterol in a subject (e.g., a reference or control subject) not receiving the oligonucleotide or pharmaceutical composition or receiving a control oligonucleotide, pharmaceutical composition or treatment.

Generally, a normal or desirable cholesterol range (total cholesterol) for an adult human patient is <200 mg/dL of blood. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of cholesterol of ≥200 mg/dL. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of cholesterol in the range of 200 to 239 mg/dL, which is considered borderline high cholesterol levels. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of cholesterol in the range of 240 mg/dL and higher (i.e., ≥240 mg/dL), which is considered high cholesterol levels. In some embodiments, the patient selected from treatment or treated is identified or determined to have an amount or level of cholesterol of 200 to 239 mg/dL, or 240 mg/dL or higher. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of cholesterol which is ≥200 mg/dL or ≥240 mg/dL or higher.

Generally, a normal or desirable LDL cholesterol range for an adult human patient is <100 mg/dL of blood. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of cholesterol of ≥100 mg/dL. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of LDL cholesterol in the range of 100 to 129 mg/dL, which is considered above optimal. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of LDL cholesterol in the range of 130 to 159 mg/dL, which is considered borderline high levels. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of LDL cholesterol in the range of 160 to 189 mg/dL, which is considered high LDL cholesterol levels. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of LDL cholesterol in the range of 190 mg/dL and higher (i.e., ≥190 mg/dL), which is considered very high LDL cholesterol levels. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of LDL cholesterol which is ≥100 mg/dL, ≥130 mg/dL, ≥160 mg/dL, or ≥190 mg/dL or higher, preferably ≥160 mg/dL, or ≥190 mg/dL or higher. In some embodiments, the patient selected for treatment or treated is identified or determined to have an amount or level of LDL cholesterol of 100 to 129 mg/dL, 130 to 159 mg/dL, 160 to 189 mg/dL, or 190 mg/dL and higher.

Suitable methods for determining LPA expression, an amount or level of LPA mRNA, an amount or level of apo(a) protein, an amount or level of apo(a) activity, an amount or level of lipoprotein(a), and/or an amount or level of OxPL, LDL-C, apoB-100, TG and/or LDL cholesterol in the subject, or in a sample from the subject, are known in the art. Further, the Examples set forth herein illustrate exemplary methods for determining LPA expression.

In some embodiments, LPA expression, the amount or level of LPA mRNA, apo(a) protein, apo(a) activity, OxPL, LDL-C, apoB-100, TG, LDL cholesterol, or any combination thereof, is reduced in a cell (e.g., a hepatocyte), a population or a group of cells (e.g., an organoid), an organ (e.g., liver), blood or a fraction thereof (e.g., plasma), a tissue (e.g., liver tissue), a sample (e.g., a liver biopsy sample), or any other biological material obtained or isolated from the subject. In some embodiments, LPA expression, the amount or level of LPA mRNA, apo(a) protein, apo(a) activity, OxPL, LDL-C, apoB-100, TG, LDL cholesterol, or any combination thereof, is reduced in more than one type of cell (e.g., a hepatocyte and one or more other type(s) of cell), more than one groups of cells, more than one organ (e.g., liver and one or more other organ(s)), more than one fraction of blood (e.g., plasma and one or more other blood fraction(s)), more than one type of tissue (e.g., liver tissue and one or more other type(s) of tissue), more than one type of sample (e.g., a liver biopsy sample and one or more other type(s) of biopsy sample) obtained or isolated from the subject.

Examples of a disease, disorder or condition associated with LPA expression include, but are not limited to, Berger's disease, peripheral artery disease, coronary artery disease, metabolic syndrome, acute coronary syndrome, aortic valve stenosis, aortic valve regurgitation, aortic dissection, retinal artery occlusion, cerebrovascular disease, mesenteric ischemia, superior mesenteric artery occlusion, renal artery stenosis, stable/unstable angina, acute coronary syndrome, heterozygous or homozygous familial hypercholesterolemia, hyperapobetalipoproteinemia, cerebrovascular atherosclerosis, cerebrovascular disease, and venous thrombosis, or a combination thereof.

Because of their high specificity, the oligonucleotides herein specifically target mRNAs of target genes of cells, tissues, or organs (e.g., liver). In preventing disease, the target gene may be one which is required for initiation or maintenance of the disease or which has been identified as being associated with a higher risk of contracting the disease. In treating disease, the oligonucleotide can be brought into contact with the cells or tissue exhibiting or responsible for mediating the disease. For example, an oligonucleotide substantially identical to all or part of a wild-type (i.e., native) or mutated gene associated with a disorder or condition associated with LPA expression may be brought into contact with or introduced into a cell or tissue type of interest such as a hepatocyte or other liver cell.

In some embodiments, the target gene may be a target gene from any mammal, such as a human. Any gene may be silenced according to the method described herein.

Methods described herein are typically involve administering to a subject a therapeutically effective amount of an oligonucleotide herein, that is, an amount capable of producing a desirable therapeutic result. A therapeutically acceptable amount may be an amount that can therapeutically treat a disease or disorder. The appropriate dosage for any one subject will depend on certain factors, including the subject's size, body surface area, age, the particular composition to be administered, the active ingredient(s) in the composition, time and route of administration, general health, and other drugs being administered concurrently.

In some embodiments, a subject is administered any one of the compositions herein either enterally (e.g., orally, by gastric feeding tube, by duodenal feeding tube, via gastrostomy or rectally), parenterally (e.g., subcutaneous injection, intravenous injection or infusion, intra-arterial injection or infusion, intraosseous infusion, intramuscular injection, intracerebral injection, intracerebroventricular injection, intrathecal), topically (e.g., epicutaneous, inhalational, via eye drops, or through a mucous membrane), or by direct injection into a target organ (e.g., the liver of a subject). Typically, oligonucleotides herein are administered intravenously or subcutaneously.

As a non-limiting set of examples, the oligonucleotides herein would typically be administered quarterly (once every three months), bi-monthly (once every two months), monthly or weekly. For example, the oligonucleotides may be administered every week or at intervals of two, or three weeks. Alternatively, the oligonucleotides may be administered daily. In some embodiments, a subject is administered one or more loading doses of the oligonucleotide followed by one or more maintenance doses of the oligonucleotide.

In some embodiments, the subject to be treated is a human or non-human primate or other mammalian subject. Other exemplary subjects include domesticated animals such as dogs and cats; livestock such as horses, cattle, pigs, sheep, goats, and chickens; and animals such as mice, rats, guinea pigs, and hamsters.

V. Kits

In some embodiments, the disclosure provides a kit comprising an oligonucleotide herein, and instructions for use. In some embodiments, the kit comprises an oligonucleotide herein, and a package insert containing instructions for use of the kit and/or any component thereof. In some embodiments, the kit comprises, in a suitable container, an oligonucleotide herein, one or more controls, and various buffers, reagents, enzymes and other standard ingredients well known in the art. In some embodiments, the container comprises at least one vial, well, test tube, flask, bottle, syringe or other container means, into which the oligonucleotide is placed, and in some instances, suitably aliquoted. In some embodiments where an additional component is provided, the kit contains additional containers into which this component is placed. The kits can also include a means for containing the oligonucleotide and any other reagent in close confinement for commercial sale. Such containers may include injection or blow-molded plastic containers into which the desired vials are retained. Containers and/or kits can include labeling with instructions for use and/or warnings.

In some embodiments, a kit comprises an oligonucleotide herein, and a pharmaceutically acceptable carrier, or a pharmaceutical composition comprising the oligonucleotide and instructions for treating or delaying progression of a disease, disorder or condition associated with LPA expression in a subject in need thereof.

EXAMPLES

While the disclosure has been described with reference to the specific embodiments set forth in the following Examples, it should be understood by those skilled in the art that various changes may be made, and equivalents may be substituted without departing from the true spirit and scope of the disclosure. Further, the following Examples are offered by way of illustration and are not intended to limit the scope of the disclosure in any manner. In addition, modifications may be made to adapt to a situation, material, composition of matter, process, process step or steps, to the objective, spirit and scope of the disclosure. All such modifications are intended to be within the scope of the disclosure. Standard techniques well known in the art or the techniques specifically described below are utilized.

Example 1: Preparation of Double-Stranded RNAi Oligonucleotides
Oligonucleotide Synthesis and Purification

The ds RNAi oligonucleotides described in the foregoing Examples are chemically synthesized using methods described herein. Generally, ds RNAi oligonucleotides are synthesized using solid phase oligonucleotide synthesis methods as described for 19-23mer siRNAs (see, e.g., Scaringe et al. (1990) NUCLEIC ACIDS RES. 18:5433-41 and Usman et al. (1987) J. AM. CHEM. SOC. 109:7845-45; see also, U.S. Pat. Nos. 5,804,683; 5,831,071; 5,998,203; 6,008,400; 6,111,086; 6,117,657; 6,353,098; 6,362,323; 6,437,117 and 6,469,158).

Individual RNA strands are synthesized and HPLC purified according to standard methods (Integrated DNA Technologies; Coralville, IA). For example, RNA oligonucleotides are synthesized using solid phase phosphoramidite chemistry, deprotected and desalted on NAP-5 columns (Amersham Pharmacia Biotech; Piscataway, NJ) using standard techniques (Damha & Olgivie (1993) METHODS MOL. BIOL. 20:81-114; Wincott et al. (1995) NUCLEIC ACIDS RES. 23:2677-84). The oligomers are purified using ion-exchange high performance liquid chromatography (IE-HPLC) on an Amersham Source 15Q column (1.0 cm×25 cm; Amersham Pharmacia Biotech) using a 15 min step-linear gradient. The gradient varies from 90:10 Buffers A:B to 52:48 Buffers A:B, where Buffer A is 100 mM Tris pH 8.5 and Buffer B is 100 mM Tris pH 8.5, 1 M NaCl. Samples are monitored at 260 nm and peaks corresponding to the full-length oligonucleotide species are collected, pooled, desalted on NAP-5 columns, and lyophilized.

The purity of each oligomer is determined by capillary electrophoresis (CE) on a Beckman PACE 5000 (Beckman Coulter, Inc.; Fullerton, CA). The CE capillaries have a 100 μm inner diameter and contain ssDNA 100R Gel (Beckman-Coulter). Typically, about 0.6 nmole of oligonucleotide is injected into a capillary, is run in an electric field of 444 V/cm and is detected by UV absorbance at 260 nm. Denaturing Tris-Borate-7 M-urea running buffer is purchased from Beckman-Coulter. Oligoribonucleotides are obtained that are at least 90% pure as assessed by CE for use in experiments described below. Compound identity is verified by matrix-assisted laser desorption ionization time-of-flight (MALDI-TOF) mass spectroscopy on a Voyager DE™ Biospectometry Work Station (Applied Biosystems; Foster City, CA) following the manufacturer's recommended protocol. Relative molecular masses of all oligomers are obtained, often within 0.2% of expected molecular mass.

Preparation of Duplexes

ssRNA oligomers are resuspended (e.g., at 100 μM concentration) in duplex buffer consisting of 100 mM potassium acetate, 30 mM HEPES, pH 7.5. Complementary sense and antisense strands are mixed in equal molar amounts to yield a final solution of, for example, 50 μM duplex. Samples are heated to 100° C. for 5′ in RNA buffer (IDT) and are allowed to cool to room temperature before use. The ds RNA oligonucleotides are stored at −20° C. ss RNA oligomers are stored lyophilized or in nuclease-free water at −80° C.

Example 2: RNAi Oligonucleotide Inhibition of LPA Expression In Vitro

LPA mRNA Target Sequence Identification

To identify RNAi oligonucleotide inhibitors of LPA expression, a computer-based algorithm was used to computationally identify LPA mRNA target sequences suitable for assaying inhibition of LPA expression by the RNAi pathway. The algorithm provides RNAi oligonucleotide guide (antisense) strand sequences each having a region of complementarity to a suitable LPA target sequence of human LPA mRNA (e.g., SEQ ID NO: 1; Table 1). Some of the guide strand sequences identified by the algorithm are also complementary to the corresponding LPA target sequence of monkey LPA mRNA (SEQ ID NO: 2; Table 1). RNAi oligonucleotides (formatted as DsiRNA oligonucleotides) were generated (Table 2), each with a unique guide strand having a region of complementarity to an LPA target sequence identified by the algorithm. The passenger (sense) strands of the DsiRNAs provided in Table 2 comprise a unique human LPA mRNA target sequence identified by the algorithm.

TABLE 1

Sequences of Human and NHP (Monkey) mRNA

Species
GenBank Ref Seq #
SEQ ID NO:

Human (Hs)
NM_005577.3
1

Cynomolgus monkey (Mf)
XM_015448517.1
2

Rhesus monkey
XM_028847001.1
3

TABLE 2

DsiRNAs Targeting Human LPA mRNA and

Controls Evaluated in Cells

SEQ

SEQ

SEQ

ID
Guide
ID
Target
ID

Passenger (Sense)
NO:
(Antisense)
NO:
Sequence
NO:

Dsi

RNA

LPA-
CUGAGCAAAGCCAUGUGGU
4
UCCUGUACCACAUG
404
CUGAGCAAAG
804

125
ACAGGA

GCUUUGCUCAGGU

CCAUGUGGU

LPA-
AGCAAAGCCAUGUGGUCCA
5
CAAUCUUGGACCAC
405
AGCAAAGCCA
805

128
AGAUTG

AUGGCUUUGCUCA

UGUGGUCCA

LPA-
AAGCCAUGUGGUCCAGGAU
6
GUAGCUAUCCUGGA
406
AAGCCAUGUG
806

132
AGCUAC

CCACAUGGCUUUG

GUCCAGGAU

LPA-
AGCCAUGUGGUCCAGGAUU
7
GGUAGUAAUCCUGG
407
AGCCAUGUGG
807

133
ACUACC

ACCACAUGGCUUU

UCCAGGAUU

LPA-
GCCAUGUGGUCCAGGAUUG
8
UGGUAUCAAUCCUG
408
GCCAUGUGGU
808

134
AUACCA

GACCACAUGGCUU

CCAGGAUUG

LPA-
CCAUGUGGUCCAGGAUUGC
9
AUGGUUGCAAUCCU
409
CCAUGUGGUC
809

135
AACCAT

GGACCACAUGGCU

CAGGAUUGC

LPA-
CAUGUGGUCCAGGAUUGCU
10
CAUGGUAGCAAUCC
410
CAUGUGGUCC
810

136
ACCATG

UGGACCACAUGGC

AGGAUUGCU

LPA-
AUGUGGUCCAGGAUUGCUA
11
CCAUGUUAGCAAUC
411
AUGUGGUCCA
811

137
ACAUGG

CUGGACCACAUGG

GGAUUGCUA

LPA-
UGUGGUCCAGGAUUGCUAC
12
ACCAUUGUAGCAAU
412
UGUGGUCCAG
812

138
AAUGGT

CCUGGACCACAUG

GAUUGCUAC

LPA-
GGUGAUGGACAGAGUUAUC
13
UGCCUUGAUAACUC
413
GGUGAUGGAC
813

160
AAGGCA

UGUCCAUCACCAU

AGAGUUAUC

LPA-
UCCACCACUGUCACAGGAA
14
AGGUCUUUCCUGUG
414
UCCACCACUG
814

190
AGACCT

ACAGUGGUGGAGU

UCACAGGAA

LPA-
CCACCACUGUCACAGGAAG
15
CAGGUUCUUCCUGU
415
CCACCACUGU
815

191
AACCTG

GACAGUGGUGGAG

CACAGGAAG

LPA-
CUGUCACAGGAAGGACCUG
16
GCUUGUCAGGUCCU
416
CUGUCACAGG
816

197
ACAAGC

UCCUGUGACAGUG

AAGGACCUG

LPA-
GGAAGGACCUGCCAAGCUU
17
AUGACUAAGCUUGG
417
GGAAGGACCU
817

205
AGUCAT

CAGGUCCUUCCUG

GCCAAGCUU

LPA-
GAAGGACCUGCCAAGCUUG
18
GAUGAUCAAGCUUG
418
GAAGGACCUG
818

206
AUCATC

GCAGGUCCUUCCU

CCAAGCUUG

LPA-
AGGACCUGCCAAGCUUGGU
19
UAGAUUACCAAGCU
419
AGGACCUGCC
819

208
AAUCTA

UGGCAGGUCCUUC

AAGCUUGGU

LPA-
GGACCUGCCAAGCUUGGUC
20
AUAGAUGACCAAGC
420
GGACCUGCCA
820

209
AUCUAT

UUGGCAGGUCCUU

AGCUUGGUC

LPA-
GACCUGCCAAGCUUGGUCA
21
CAUAGUUGACCAAG
421
GACCUGCCAA
821

210
ACUATG

CUUGGCAGGUCCU

GCUUGGUCA

LPA-
ACCUGCCAAGCUUGGUCAU
22
UCAUAUAUGACCAA
422
ACCUGCCAAG
822

211
AUAUGA

GCUUGGCAGGUCC

CUUGGUCAU

LPA-
CCUGCCAAGCUUGGUCAUC
23
GUCAUUGAUGACCA
423
CCUGCCAAGC
823

212
AAUGAC

AGCUUGGCAGGUC

UUGGUCAUC

LPA-
AGCUUGGUCAUCUAUGACA
24
AUGUGUUGUCAUAG
424
AGCUUGGUCA
824

219
ACACAT

AUGACCAAGCUUG

UCUAUGACA

LPA-
GUCAUCUAUGACACCACAU
25
AUGUUUAUGUGGUG
425
GUCAUCUAUG
825

225
AAACAT

UCAUAGAUGACCA

ACACCACAU

LPA-
CACAGAAAACUACCCAAAU
26
GCCAGUAUUUGGGU
426
CACAGAAAAC
826

258
ACUGGC

AGUUUUCUGUGGU

UACCCAAAU

LPA-
AGAAAACUACCCAAAUGCU
27
CAAGCUAGCAUUUG
427
AGAAAACUAC
827

261
AGCUTG

GGUAGUUUUCUGU

CCAAAUGCU

LPA-
AAAACUACCCAAAUGCUGG
28
AUCAAUCCAGCAUU
428
AAAACUACCC
828

263
AUUGAT

UGGGUAGUUUUCU

AAAUGCUGG

LPA-
ACCCAAAUGCUGGCUUGAU
29
UUCAUUAUCAAGCC
429
ACCCAAAUGC
829

269
AAUGAA

AGCAUUUGGGUAG

UGGCUUGAU

LPA-
CCCAAAUGCUGGCUUGAUC
30
GUUCAUGAUCAAGC
430
CCCAAAUGCU
830

270
AUGAAC

CAGCAUUUGGGUA

GGCUUGAUC

LPA-
GAACUACUGCAGGAAUCCA
31
AGCAUUUGGAUUCC
431
GAACUACUGC
831

291
AAUGCT

UGCAGUAGUUCAU

AGGAAUCCA

LPA-
UACUGCAGGAAUCCAGAUG
32
CCACAUCAUCUGGA
432
UACUGCAGGA
832

295
AUGUGG

UUCCUGCAGUAGU

AUCCAGAUG

LPA-
ACUGCAGGAAUCCAGAUGC
33
GCCACUGCAUCUGG
433
ACUGCAGGAA
833

296
AGUGGC

AUUCCUGCAGUAG

UCCAGAUGC

LPA-
UGCAGGAAUCCAGAUGCUG
34
CUGCCUCAGCAUCU
434
UGCAGGAAUC
834

298
AGGCAG

GGAUUCCUGCAGU

CAGAUGCUG

LPA-
AGGUGGGAGUACUGCAACC
35
GCGUCUGGUUGCAG
435
AGGUGGGAGU
835

355
AGACGC

UACUCCCACCUGA

ACUGCAACC

LPA-
AAUGCUCAGACGCAGAAGG
36
GCAGUUCCUUCUGC
436
AAUGCUCAGA
836

380
AACUGC

GUCUGAGCAUUGC

CGCAGAAGG

LPA-
GACUGUUACCCCGGUUCCA
37
UAGGCUUGGAACCG
437
GACUGUUACC
837

417
AGCCTA

GGGUAACAGUCGG

CCGGUUCCA

LPA-
ACUGUUACCCCGGUUCCAA
38
CUAGGUUUGGAACC
438
ACUGUUACCC
838

418
ACCUAG

GGGGUAACAGUCG

CGGUUCCAA

LPA-
CUGUUACCCCGGUUCCAAG
39
UCUAGUCUUGGAAC
439
CUGUUACCCC
839

419
ACUAGA

CGGGGUAACAGUC

GGUUCCAAG

LPA-
UGUUACCCCGGUUCCAAGC
40
CUCUAUGCUUGGAA
440
UGUUACCCCG
840

420
AUAGAG

CCGGGGUAACAGU

GUUCCAAGC

LPA-
GUUACCCCGGUUCCAAGCC
41
CCUCUUGGCUUGGA
441
GUUACCCCGG
841

421
AAGAGG

ACCGGGGUAACAG

UUCCAAGCC

LPA-
UUACCCCGGUUCCAAGCCU
42
GCCUCUAGGCUUGG
442
UUACCCCGGU
842

422
AGAGGC

AACCGGGGUAACA

UCCAAGCCU

LPA-
UACCCCGGUUCCAAGCCUA
43
AGCCUUUAGGCUUG
443
UACCCCGGUU
843

423
AAGGCT

GAACCGGGGUAAC

CCAAGCCUA

LPA-
GUGCUACCAUGGUAAUGGA
44
ACUCUUUCCAUUAC
444
GUGCUACCAU
844

492
AAGAGT

CAUGGUAGCACUC

GGUAAUGGA

LPA-
UGCUACCAUGGUAAUGGAC
45
AACUCUGUCCAUUA
445
UGCUACCAUG
845

493
AGAGTT

CCAUGGUAGCACU

GUAAUGGAC

LPA-
GCUACCAUGGUAAUGGACA
46
UAACUUUGUCCAUU
446
GCUACCAUGG
846

494
AAGUTA

ACCAUGGUAGCAC

UAAUGGACA

LPA-
CUACCAUGGUAAUGGACAG
47
AUAACUCUGUCCAU
447
CUACCAUGGU
847

495
AGUUAT

UACCAUGGUAGCA

AAUGGACAG

LPA-
UACCAUGGUAAUGGACAGA
48
GAUAAUUCUGUCCA
448
UACCAUGGUA
848

496
AUUATC

UUACCAUGGUAGC

AUGGACAGA

LPA-
ACCAUGGUAAUGGACAGAG
49
CGAUAUCUCUGUCC
449
ACCAUGGUAA
849

497
AUAUCG

AUUACCAUGGUAG

UGGACAGAG

LPA-
CCAUGGUAAUGGACAGAGU
50
UCGAUUACUCUGUC
450
CCAUGGUAAU
850

498
AAUCGA

CAUUACCAUGGUA

GGACAGAGU

LPA-
CAUGGUAAUGGACAGAGUU
51
CUCGAUAACUCUGU
451
CAUGGUAAUG
851

499
AUCGAG

CCAUUACCAUGGU

GACAGAGUU

LPA-
AUGGUAAUGGACAGAGUUA
52
CCUCGUUAACUCUG
452
AUGGUAAUGG
852

500
ACGAGG

UCCAUUACCAUGG

ACAGAGUUA

LPA-
UGGUAAUGGACAGAGUUAU
53
GCCUCUAUAACUCU
453
UGGUAAUGGA
853

501
AGAGGC

GUCCAUUACCAUG

CAGAGUUAU

LPA-
GGUAAUGGACAGAGUUAUC
54
UGCCUUGAUAACUC
454
GGUAAUGGAC
854

502
AAGGCA

UGUCCAUUACCAU

AGAGUUAUC

LPA-
GUAAUGGACAGAGUUAUCG
55
GUGCCUCGAUAACU
455
GUAAUGGACA
855

503
AGGCAC

CUGUCCAUUACCA

GAGUUAUCG

LPA-
GGCACAUACUCCACCACUG
56
CUGUGUCAGUGGUG
456
GGCACAUACU
856

523
ACACAG

GAGUAUGUGCCUC

CCACCACUG

LPA-
CUUGGUCAUCUAUGACACC
57
GAGUGUGGUGUCAU
457
CUUGGUCAUC
857

563
ACACTC

AGAUGACCAAGCU

UAUGACACC

LPA-
GUCAUCUAUGACACCACAC
58
AUGCGUGUGUGGUG
458
GUCAUCUAUG
858

567
ACGCAT

UCAUAGAUGACCA

ACACCACAC

LPA-
UCAUCUAUGACACCACACU
59
UAUGCUAGUGUGGU
459
UCAUCUAUGA
859

568
AGCATA

GUCAUAGAUGACC

CACCACACU

LPA-
CAUCUAUGACACCACACUC
60
CUAUGUGAGUGUGG
460
CAUCUAUGAC
860

569
ACAUAG

UGUCAUAGAUGAC

ACCACACUC

LPA-
GCACAUACUCCACCACUGU
61
CCAGUUACAGUGGU
461
GCACAUACUC
861

1208
AACUGG

GGAGUAUGUGCCU

CACCACUGU

LPA-
AGCCCCUUAUUGUUAUACG
62
AUCCCUCGUAUAAC
462
AGCCCCUUAU
862

2715
AGGGAT

AAUAAGGGGCUGC

UGUUAUACG

LPA-
GCCCCUUAUUGUUAUACGA
63
GAUCCUUCGUAUAA
463
GCCCCUUAUU
863

2716
AGGATC

CAAUAAGGGGCUG

GUUAUACGA

LPA-
CCAAGCCUAGAGGCUCCUU
64
GUUCAUAAGGAGCC
464
CCAAGCCUAG
864

2827
AUGAAC

UCUAGGCUUGGAA

AGGCUCCUU

LPA-
AGGCUCCUUCUGAACAAGC
65
GUUGGUGCUUGUUC
465
AGGCUCCUUC
865

2837
ACCAAC

AGAAGGAGCCUCU

UGAACAAGC

LPA-
AUGGACAGAGUUAUCAAGG
66
UAUGUUCCUUGAUA
466
AUGGACAGAG
866

2900
AACATA

ACUCUGUCCAUUU

UUAUCAAGG

LPA-
UGGACAGAGUUAUCAAGGC
67
GUAUGUGCCUUGAU
467
UGGACAGAGU
867

2901
ACAUAC

AACUCUGUCCAUU

UAUCAAGGC

LPA-
GGACAGAGUUAUCAAGGCA
68
AGUAUUUGCCUUGA
468
GGACAGAGUU
868

2902
AAUACT

UAACUCUGUCCAU

AUCAAGGCA

LPA-
GACAGAGUUAUCAAGGCAC
69
AAGUAUGUGCCUUG
469
GACAGAGUUA
869

2903
AUACTT

AUAACUCUGUCCA

UCAAGGCAC

LPA-
ACAGAGUUAUCAAGGCACA
70
GAAGUUUGUGCCUU
470
ACAGAGUUAU
870

2904
AACUTC

GAUAACUCUGUCC

CAAGGCACA

LPA-
CAGAGUUAUCAAGGCACAU
71
UGAAGUAUGUGCCU
471
CAGAGUUAUC
871

2905
ACUUCA

UGAUAACUCUGUC

AAGGCACAU

LPA-
UACCCAAAUGCUGGCUUGA
72
UCUUGUUCAAGCCA
472
UACCCAAAUG
872

3004
ACAAGA

GCAUUUGGGUAGU

CUGGCUUGA

LPA-
CCAAAUGCUGGCUUGAUCA
73
AGUUCUUGAUCAAG
473
CCAAAUGCUG
873

3007
AGAACT

CCAGCAUUUGGGU

GCUUGAUCA

LPA-
UCAAGAACUACUGCCGAAA
74
UCUGGUUUUCGGCA
474
UCAAGAACUA
874

3023
ACCAGA

GUAGUUCUUGAUC

CUGCCGAAA

LPA-
CAAGAACUACUGCCGAAAU
75
AUCUGUAUUUCGGC
475
CAAGAACUAC
875

3024
ACAGAT

AGUAGUUCUUGAU

UGCCGAAAU

LPA-
AAGAACUACUGCCGAAAUC
76
GAUCUUGAUUUCGG
476
AAGAACUACU
876

3025
AAGATC

CAGUAGUUCUUGA

GCCGAAAUC

LPA-
GAACUACUGCCGAAAUCCA
77
AGGAUUUGGAUUUC
477
GAACUACUGC
877

3027
AAUCCT

GGCAGUAGUUCUU

CGAAAUCCA

LPA-
CUACUGCCGAAAUCCAGAU
78
CACAGUAUCUGGAU
478
CUACUGCCGA
878

3030
ACUGTG

UUCGGCAGUAGUU

AAUCCAGAU

LPA-
UGUGGCAGCCCCUUGGUGU
79
UGUAUUACACCAAG
479
UGUGGCAGCC
879

3051
AAUACA

GGGCUGCCACAGG

CCUUGGUGU

LPA-
GUGGCAGCCCCUUGGUGUU
80
UUGUAUAACACCAA
480
GUGGCAGCCC
880

3052
AUACAA

GGGGCUGCCACAG

CUUGGUGUU

LPA-
UGGCAGCCCCUUGGUGUUA
81
GUUGUUUAACACCA
481
UGGCAGCCCC
881

3053
AACAAC

AGGGGCUGCCACA

UUGGUGUUA

LPA-
GGCAGCCCCUUGGUGUUAU
82
UGUUGUAUAACACC
482
GGCAGCCCCU
882

3054
ACAACA

AAGGGGCUGCCAC

UGGUGUUAU

LPA-
GCAGCCCCUUGGUGUUAUA
83
CUGUUUUAUAACAC
483
GCAGCCCCUU
883

3055
AAACAG

CAAGGGGCUGCCA

GGUGUUAUA

LPA-
CAGCCCCUUGGUGUUAUAC
84
UCUGUUGUAUAACA
484
CAGCCCCUUG
884

3056
AACAGA

CCAAGGGGCUGCC

GUGUUAUAC

LPA-
AGCCCCUUGGUGUUAUACA
85
AUCUGUUGUAUAAC
485
AGCCCCUUGG
885

3057
ACAGAT

ACCAAGGGGCUGC

UGUUAUACA

LPA-
GCCCCUUGGUGUUAUACAA
86
GAUCUUUUGUAUAA
486
GCCCCUUGGU
886

3058
AAGATC

CACCAAGGGGCUG

GUUAUACAA

LPA-
CCCCUUGGUGUUAUACAAC
87
GGAUCUGUUGUAUA
487
CCCCUUGGUG
887

3059
AGAUCC

ACACCAAGGGGCU

UUAUACAAC

LPA-
GGUGGGAGUACUGCAACCU
88
CGUGUUAGGUUGCA
488
GGUGGGAGUA
888

3092
AACACG

GUACUCCCACCUG

CUGCAACCU

LPA-
GUGGGAGUACUGCAACCUG
89
UCGUGUCAGGUUGC
489
GUGGGAGUAC
889

3093
ACACGA

AGUACUCCCACCU

UGCAACCUG

LPA-
GGAGUACUGCAACCUGACA
90
GCAUCUUGUCAGGU
490
GGAGUACUGC
890

3096
AGAUGC

UGCAGUACUCCCA

AACCUGACA

LPA-
GAGUACUGCAACCUGACAC
91
AGCAUUGUGUCAGG
491
GAGUACUGCA
891

3097
AAUGCT

UUGCAGUACUCCC

ACCUGACAC

LPA-
GUACUGCAACCUGACACGA
92
UGAGCUUCGUGUCA
492
GUACUGCAAC
892

3099
AGCUCA

GGUUGCAGUACUC

CUGACACGA

LPA-
UACUGCAACCUGACACGAU
93
CUGAGUAUCGUGUC
493
UACUGCAACC
893

3100
ACUCAG

AGGUUGCAGUACU

UGACACGAU

LPA-
ACUGCAACCUGACACGAUG
94
UCUGAUCAUCGUGU
494
ACUGCAACCU
894

3101
AUCAGA

CAGGUUGCAGUAC

GACACGAUG

LPA-
CUGCAACCUGACACGAUGC
95
AUCUGUGCAUCGUG
495
CUGCAACCUG
895

3102
ACAGAT

UCAGGUUGCAGUA

ACACGAUGC

LPA-
UGCAACCUGACACGAUGCU
96
CAUCUUAGCAUCGU
496
UGCAACCUGA
896

3103
AAGATG

GUCAGGUUGCAGU

CACGAUGCU

LPA-
CAACCUGACACGAUGCUCA
97
UGCAUUUGAGCAUC
497
CAACCUGACA
897

3105
AAUGCA

GUGUCAGGUUGCA

CGAUGCUCA

LPA-
ACCUGACACGAUGCUCAGA
98
UCUGCUUCUGAGCA
498
ACCUGACACG
898

3107
AGCAGA

UCGUGUCAGGUUG

AUGCUCAGA

LPA-
CCUGACACGAUGCUCAGAU
99
UUCUGUAUCUGAGC
499
CCUGACACGA
899

3108
ACAGAA

AUCGUGUCAGGUU

UGCUCAGAU

LPA-
CUGACACGAUGCUCAGAUG
100
AUUCUUCAUCUGAG
500
CUGACACGAU
900

3109
AAGAAT

CAUCGUGUCAGGU

GCUCAGAUG

LPA-
UGACACGAUGCUCAGAUGC
101
CAUUCUGCAUCUGA
501
UGACACGAUG
901

3110
AGAATG

GCAUCGUGUCAGG

CUCAGAUGC

LPA-
GACACGAUGCUCAGAUGCA
102
CCAUUUUGCAUCUG
502
GACACGAUGC
902

3111
AAAUGG

AGCAUCGUGUCAG

UCAGAUGCA

LPA-
ACACGAUGCUCAGAUGCAG
103
UCCAUUCUGCAUCU
503
ACACGAUGCU
903

3112
AAUGGA

GAGCAUCGUGUCA

CAGAUGCAG

LPA-
CACGAUGCUCAGAUGCAGA
104
GUCCAUUCUGCAUC
504
CACGAUGCUC
904

3113
AUGGAC

UGAGCAUCGUGUC

AGAUGCAGA

LPA-
UGCUACUACCAUUAUGGAC
105
AACUCUGUCCAUAA
505
UGCUACUACC
905

3229
AGAGTT

UGGUAGUAGCAGU

AUUAUGGAC

LPA-
GCUACUACCAUUAUGGACA
106
UAACUUUGUCCAUA
506
GCUACUACCA
906

3230
AAGUTA

AUGGUAGUAGCAG

UUAUGGACA

LPA-
CUACUACCAUUAUGGACAG
107
GUAACUCUGUCCAU
507
CUACUACCAU
907

3231
AGUUAC

AAUGGUAGUAGCA

UAUGGACAG

LPA-
UACUACCAUUAUGGACAGA
108
GGUAAUUCUGUCCA
508
UACUACCAUU
908

3232
AUUACC

UAAUGGUAGUAGC

AUGGACAGA

LPA-
ACUACCAUUAUGGACAGAG
109
CGGUAUCUCUGUCC
509
ACUACCAUUA
909

3233
AUACCG

AUAAUGGUAGUAG

UGGACAGAG

LPA-
CUACCAUUAUGGACAGAGU
110
UCGGUUACUCUGUC
510
CUACCAUUAU
910

3234
AACCGA

CAUAAUGGUAGUA

GGACAGAGU

LPA-
UACCAUUAUGGACAGAGUU
111
CUCGGUAACUCUGU
511
UACCAUUAUG
911

3235
ACCGAG

CCAUAAUGGUAGU

GACAGAGUU

LPA-
ACCAUUAUGGACAGAGUUA
112
CCUCGUUAACUCUG
512
ACCAUUAUGG
912

3236
ACGAGG

UCCAUAAUGGUAG

ACAGAGUUA

LPA-
GAGGCACAUACUCCACCAC
113
GUGACUGUGGUGGA
513
GAGGCACAUA
913

3257
AGUCAC

GUAUGUGCCUCGG

CUCCACCAC

LPA-
CUCCACCACUGUCACAGGA
114
AGUUCUUCCUGUGA
514
CUCCACCACU
914

3267
AGAACT

CAGUGGUGGAGUA

GUCACAGGA

LPA-
ACAGGAAGAACUUGCCAAG
115
ACCAAUCUUGGCAA
515
ACAGGAAGAA
915

3280
AUUGGT

GUUCUUCCUGUGA

CUUGCCAAG

LPA-
CAGGAAGAACUUGCCAAGC
116
GACCAUGCUUGGCA
516
CAGGAAGAAC
916

3281
AUGGTC

AGUUCUUCCUGUG

UUGCCAAGC

LPA-
AGGAAGAACUUGCCAAGCU
117
UGACCUAGCUUGGC
517
AGGAAGAACU
917

3282
AGGUCA

AAGUUCUUCCUGU

UGCCAAGCU

LPA-
GGAAGAACUUGCCAAGCUU
118
AUGACUAAGCUUGG
518
GGAAGAACUU
918

3283
AGUCAT

CAAGUUCUUCCUG

GCCAAGCUU

LPA-
GAAGAACUUGCCAAGCUUG
119
GAUGAUCAAGCUUG
519
GAAGAACUUG
919

3284
AUCATC

GCAAGUUCUUCCU

CCAAGCUUG

LPA-
AAGAACUUGCCAAGCUUGG
120
AGAUGUCCAAGCUU
520
AAGAACUUGC
920

3285
ACAUCT

GGCAAGUUCUUCC

CAAGCUUGG

LPA-
AGAACUUGCCAAGCUUGGU
121
UAGAUUACCAAGCU
521
AGAACUUGCC
921

3286
AAUCTA

UGGCAAGUUCUUC

AAGCUUGGU

LPA-
GAACUUGCCAAGCUUGGUC
122
AUAGAUGACCAAGC
522
GAACUUGCCA
922

3287
AUCUAT

UUGGCAAGUUCUU

AGCUUGGUC

LPA-
AACUUGCCAAGCUUGGUCA
123
CAUAGUUGACCAAG
523
AACUUGCCAA
923

3288
ACUATG

CUUGGCAAGUUCU

GCUUGGUCA

LPA-
ACUUGCCAAGCUUGGUCAU
124
UCAUAUAUGACCAA
524
ACUUGCCAAG
924

3289
AUAUGA

GCUUGGCAAGUUC

CUUGGUCAU

LPA-
CUUGCCAAGCUUGGUCAUC
125
GUCAUUGAUGACCA
525
CUUGCCAAGC
925

3290
AAUGAC

AGCUUGGCAAGUU

UUGGUCAUC

LPA-
UUGCCAAGCUUGGUCAUCU
126
UGUCAUAGAUGACC
526
UUGCCAAGCU
926

3291
AUGACA

AAGCUUGGCAAGU

UGGUCAUCU

LPA-
UGCCAAGCUUGGUCAUCUA
127
GUGUCUUAGAUGAC
527
UGCCAAGCUU
927

3292
AGACAC

CAAGCUUGGCAAG

GGUCAUCUA

LPA-
GCUUGGUCAUCUAUGACAC
128
GGUGUUGUGUCAUA
528
GCUUGGUCAU
928

3298
AACACC

GAUGACCAAGCUU

CUAUGACAC

LPA-
UUGGUCAUCUAUGACACCA
129
CUGGUUUGGUGUCA
529
UUGGUCAUCU
929

3300
AACCAG

UAGAUGACCAAGC

AUGACACCA

LPA-
UGGUCAUCUAUGACACCAC
130
GCUGGUGUGGUGUC
530
UGGUCAUCUA
930

3301
ACCAGC

AUAGAUGACCAAG

UGACACCAC

LPA-
GUCAUCUAUGACACCACAC
131
AUGCUUGUGUGGUG
531
GUCAUCUAUG
931

3303
AAGCAT

UCAUAGAUGACCA

ACACCACAC

LPA-
CAUCUAUGACACCACACCA
132
CUAUGUUGGUGUGG
532
CAUCUAUGAC
932

3305
ACAUAG

UGUCAUAGAUGAC

ACCACACCA

LPA-
AUCUAUGACACCACACCAG
133
ACUAUUCUGGUGUG
533
AUCUAUGACA
933

3306
AAUAGT

GUGUCAUAGAUGA

CCACACCAG

LPA-
CUAUGACACCACACCAGCA
134
CGACUUUGCUGGUG
534
CUAUGACACC
934

3308
AAGUCG

UGGUGUCAUAGAU

ACACCAGCA

LPA-
GUCGGACCCCAGAAAACUA
135
UUUGGUUAGUUUUC
535
GUCGGACCCC
935

3329
ACCAAA

UGGGGUCCGACUA

AGAAAACUA

LPA-
UCGGACCCCAGAAAACUAC
136
AUUUGUGUAGUUUU
536
UCGGACCCCA
936

3330
ACAAAT

CUGGGGUCCGACU

GAAAACUAC

LPA-
GAAAACUACCCAAAUGCUG
137
UCAGGUCAGCAUUU
537
GAAAACUACC
937

3340
ACCUGA

GGGUAGUUUUCUG

CAAAUGCUG

LPA-
GCUGAGAUUCGCCCUUGGU
138
UGUAAUACCAAGGG
538
GCUGAGAUUC
938

3391
AUUACA

CGAAUCUCAGCAU

GCCCUUGGU

LPA-
CUGAGAUUCGCCCUUGGUG
139
GUGUAUCACCAAGG
539
CUGAGAUUCG
939

3392
AUACAC

GCGAAUCUCAGCA

CCCUUGGUG

LPA-
GAGAUUCGCCCUUGGUGUU
140
UGGUGUAACACCAA
540
GAGAUUCGCC
940

3394
ACACCA

GGGCGAAUCUCAG

CUUGGUGUU

LPA-
AGAUUCGCCCUUGGUGUUA
141
AUGGUUUAACACCA
541
AGAUUCGCCC
941

3395
AACCAT

AGGGCGAAUCUCA

UUGGUGUUA

LPA-
UUCGCCCUUGGUGUUACAC
142
UCCAUUGUGUAACA
542
UUCGCCCUUG
942

3398
AAUGGA

CCAAGGGCGAAUC

GUGUUACAC

LPA-
CUUGGUGUUACACCAUGGA
143
CUGGGUUCCAUGGU
543
CUUGGUGUUA
943

3404
ACCCAG

GUAACACCAAGGG

CACCAUGGA

LPA-
UUGGUGUUACACCAUGGAU
144
ACUGGUAUCCAUGG
544
UUGGUGUUAC
944

3405
ACCAGT

UGUAACACCAAGG

ACCAUGGAU

LPA-
UGGUGUUACACCAUGGAUC
145
CACUGUGAUCCAUG
545
UGGUGUUACA
945

3406
ACAGTG

GUGUAACACCAAG

CCAUGGAUC

LPA-
GGUGUUACACCAUGGAUCC
146
ACACUUGGAUCCAU
546
GGUGUUACAC
946

3407
AAGUGT

GGUGUAACACCAA

CAUGGAUCC

LPA-
UGUUACACCAUGGAUCCCA
147
UGACAUUGGGAUCC
547
UGUUACACCA
947

3409
AUGUCA

AUGGUGUAACACC

UGGAUCCCA

LPA-
GAAUCAAGUGUCCUUGCAA
148
UGAGAUUUGCAAGG
548
GAAUCAAGUG
948

3472
AUCUCA

ACACUUGAUUCUG

UCCUUGCAA

LPA-
AAUCAAGUGUCCUUGCAAC
149
GUGAGUGUUGCAAG
549
AAUCAAGUGU
949

3473
ACUCAC

GACACUUGAUUCU

CCUUGCAAC

LPA-
AUCAAGUGUCCUUGCAACU
150
CGUGAUAGUUGCAA
550
AUCAAGUGUC
950

3474
AUCACG

GGACACUUGAUUC

CUUGCAACU

LPA-
AUGGACAGAGUUAUCGAGG
151
AAUGAUCCUCGAUA
551
AUGGACAGAG
951

3584
AUCATT

ACUCUGUCCAUCA

UUAUCGAGG

LPA-
UGGACAGAGUUAUCGAGGC
152
GAAUGUGCCUCGAU
552
UGGACAGAGU
952

3585
ACAUTC

AACUCUGUCCAUC

UAUCGAGGC

LPA-
ACACCACACUGGCAUCAGA
153
UUGUCUUCUGAUGC
553
ACACCACACU
953

3655
AGACAA

CAGUGUGGUGUCA

GGCAUCAGA

LPA-
UUGGUGUUAUACCAUGGAU
154
AUUGGUAUCCAUGG
554
UUGGUGUUAU
954

3747
ACCAAT

UAUAACACCAAGG

ACCAUGGAU

LPA-
UGGUGUUAUACCAUGGAUC
155
CAUUGUGAUCCAUG
555
UGGUGUUAUA
955

3748
ACAATG

GUAUAACACCAAG

CCAUGGAUC

LPA-
GGUGUUAUACCAUGGAUCC
156
ACAUUUGGAUCCAU
556
GGUGUUAUAC
956

3749
AAAUGT

GGUAUAACACCAA

CAUGGAUCC

LPA-
GUGUUAUACCAUGGAUCCC
157
GACAUUGGGAUCCA
557
GUGUUAUACC
957

3750
AAUGTC

UGGUAUAACACCA

AUGGAUCCC

LPA-
UCAGAUGGGAGUACUGCAA
158
GUCAGUUUGCAGUA
558
UCAGAUGGGA
958

3773
ACUGAC

CUCCCAUCUGACA

GUACUGCAA

LPA-
GAUGGGAGUACUGCAACCU
159
UGUGUUAGGUUGCA
559
GAUGGGAGUA
959

3776
AACACA

GUACUCCCAUCUG

CUGCAACCU

LPA-
AUGGGAGUACUGCAACCUG
160
UUGUGUCAGGUUGC
560
AUGGGAGUAC
960

3777
ACACAA

AGUACUCCCAUCU

UGCAACCUG

LPA-
UGGGAGUACUGCAACCUGA
161
AUUGUUUCAGGUUG
561
UGGGAGUACU
961

3778
AACAAT

CAGUACUCCCAUC

GCAACCUGA

LPA-
GGGAGUACUGCAACCUGAC
162
CAUUGUGUCAGGUU
562
GGGAGUACUG
962

3779
ACAATG

GCAGUACUCCCAU

CAACCUGAC

LPA-
GGCUGUUUCUGAACAAGCA
163
CGUUGUUGCUUGUU
563
GGCUGUUUCU
963

3840
ACAACG

CAGAAACAGCCGU

GAACAAGCA

LPA-
GUUUCUGAACAAGCACCAA
164
GCUCCUUUGGUGCU
564
GUUUCUGAAC
964

3844
AGGAGC

UGUUCAGAAACAG

AAGCACCAA

LPA-
CUCCACCACUGUUACAGGA
165
UGUCCUUCCUGUAA
565
CUCCACCACU
965

3927
AGGACA

CAGUGGUGGAGAA

GUUACAGGA

LPA-
UCCACCACUGUUACAGGAA
166
AUGUCUUUCCUGUA
566
UCCACCACUG
966

3928
AGACAT

ACAGUGGUGGAGA

UUACAGGAA

LPA-
CCACCACUGUUACAGGAAG
167
CAUGUUCUUCCUGU
567
CCACCACUGU
967

3929
AACATG

AACAGUGGUGGAG

UACAGGAAG

LPA-
GACACCACACUGGCAUCAG
168
GGUUCUCUGAUGCC
568
GACACCACAC
968

3972
AGAACC

AGUGUGGUGUCAU

UGGCAUCAG

LPA-
ACACCACACUGGCAUCAGA
169
UGGUUUUCUGAUGC
569
ACACCACACU
969

3973
AAACCA

CAGUGUGGUGUCA

GGCAUCAGA

LPA-
AGAAUACUACCCAAAUGGU
170
CAGGCUACCAUUUG
570
AGAAUACUAC
970

3999
AGCCTG

GGUAGUAUUCUGU

CCAAAUGGU

LPA-
GAAUACUACCCAAAUGGUG
171
UCAGGUCACCAUUU
571
GAAUACUACC
971

4000
ACCUGA

GGGUAGUAUUCUG

CAAAUGGUG

LPA-
AAUACUACCCAAAUGGUGG
172
GUCAGUCCACCAUU
572
AAUACUACCC
972

4001
ACUGAC

UGGGUAGUAUUCU

AAAUGGUGG

LPA-
UCCUUCUGAAGAAGCACCA
173
UUCAGUUGGUGCUU
573
UCCUUCUGAA
973

4185
ACUGAA

CUUCAGAAGGAAG

GAAGCACCA

LPA-
CCUUCUGAAGAAGCACCAA
174
UUUCAUUUGGUGCU
574
CCUUCUGAAG
974

4186
AUGAAA

UCUUCAGAAGGAA

AAGCACCAA

LPA-
CUUCUGAAGAAGCACCAAC
175
UUUUCUGUUGGUGC
575
CUUCUGAAGA
975

4187
AGAAAA

UUCUUCAGAAGGA

AGCACCAAC

LPA-
UUCUGAAGAAGCACCAACU
176
GUUUUUAGUUGGUG
576
UUCUGAAGAA
976

4188
AAAAAC

CUUCUUCAGAAGG

GCACCAACU

LPA-
UCUGAAGAAGCACCAACUG
177
UGUUUUCAGUUGGU
577
UCUGAAGAAG
977

4189
AAAACA

GCUUCUUCAGAAG

CACCAACUG

LPA-
CUGAAGAAGCACCAACUGA
178
CUGUUUUCAGUUGG
578
CUGAAGAAGC
978

4190
AAACAG

UGCUUCUUCAGAA

ACCAACUGA

LPA-
UGAAGAAGCACCAACUGAA
179
GCUGUUUUCAGUUG
579
UGAAGAAGCA
979

4191
AACAGC

GUGCUUCUUCAGA

CCAACUGAA

LPA-
GAAGAAGCACCAACUGAAA
180
UGCUGUUUUCAGUU
580
GAAGAAGCAC
980

4192
ACAGCA

GGUGCUUCUUCAG

CAACUGAAA

LPA-
AAGAAGCACCAACUGAAAA
181
GUGCUUUUUUCAGU
581
AAGAAGCACC
981

4193
AAGCAC

UGGUGCUUCUUCA

AACUGAAAA

LPA-
AGAAGCACCAACUGAAAAC
182
AGUGCUGUUUUCAG
582
AGAAGCACCA
982

4194
AGCACT

UUGGUGCUUCUUC

ACUGAAAAC

LPA-
GAAGCACCAACUGAAAACA
183
CAGUGUUGUUUUCA
583
GAAGCACCAA
983

4195
ACACTG

GUUGGUGCUUCUU

CUGAAAACA

LPA-
AAGCACCAACUGAAAACAG
184
CCAGUUCUGUUUUC
584
AAGCACCAAC
984

4196
AACUGG

AGUUGGUGCUUCU

UGAAAACAG

LPA-
AGGUGAUGGACAGAGUUAU
185
GCCUCUAUAACUCU
585
AGGUGAUGGA
985

4239
AGAGGC

GUCCAUCACCUCG

CAGAGUUAU

LPA-
CUCCACCACUAUCACAGGA
186
UGUUCUUCCUGUGA
586
CUCCACCACU
986

4269
AGAACA

UAGUGGUGGAGAG

AUCACAGGA

LPA-
UCCACCACUAUCACAGGAA
187
AUGUUUUUCCUGUG
587
UCCACCACUA
987

4270
AAACAT

AUAGUGGUGGAGA

UCACAGGAA

LPA-
CCACCACUAUCACAGGAAG
188
CAUGUUCUUCCUGU
588
CCACCACUAU
988

4271
AACATG

GAUAGUGGUGGAG

CACAGGAAG

LPA-
CACCACUAUCACAGGAAGA
189
ACAUGUUCUUCCUG
589
CACCACUAUC
989

4272
ACAUGT

UGAUAGUGGUGGA

ACAGGAAGA

LPA-
ACCACUAUCACAGGAAGAA
190
GACAUUUUCUUCCU
590
ACCACUAUCA
990

4273
AAUGTC

GUGAUAGUGGUGG

CAGGAAGAA

LPA-
CCACUAUCACAGGAAGAAC
191
UGACAUGUUCUUCC
591
CCACUAUCAC
991

4274
AUGUCA

UGUGAUAGUGGUG

AGGAAGAAC

LPA-
CACUAUCACAGGAAGAACA
192
CUGACUUGUUCUUC
592
CACUAUCACA
992

4275
AGUCAG

CUGUGAUAGUGGU

GGAAGAACA

LPA-
ACUAUCACAGGAAGAACAU
193
ACUGAUAUGUUCUU
593
ACUAUCACAG
993

4276
AUCAGT

CCUGUGAUAGUGG

GAAGAACAU

LPA-
CUAUCACAGGAAGAACAUG
194
GACUGUCAUGUUCU
594
CUAUCACAGG
994

4277
ACAGTC

UCCUGUGAUAGUG

AAGAACAUG

LPA-
UAUCACAGGAAGAACAUGU
195
AGACUUACAUGUUC
595
UAUCACAGGA
995

4278
AAGUCT

UUCCUGUGAUAGU

AGAACAUGU

LPA-
AUCACAGGAAGAACAUGUC
196
AAGACUGACAUGUU
596
AUCACAGGAA
996

4279
AGUCTT

CUUCCUGUGAUAG

GAACAUGUC

LPA-
UCACAGGAAGAACAUGUCA
197
CAAGAUUGACAUGU
597
UCACAGGAAG
997

4280
AUCUTG

UCUUCCUGUGAUA

AACAUGUCA

LPA-
CACAGGAAGAACAUGUCAG
198
CCAAGUCUGACAUG
598
CACAGGAAGA
998

4281
ACUUGG

UUCUUCCUGUGAU

ACAUGUCAG

LPA-
ACAGGAAGAACAUGUCAGU
199
ACCAAUACUGACAU
599
ACAGGAAGAA
999

4282
AUUGGT

GUUCUUCCUGUGA

CAUGUCAGU

LPA-
GGAAGAACAUGUCAGUCUU
200
ACGACUAAGACUGA
600
GGAAGAACAU
1000

4285
AGUCGT

CAUGUUCUUCCUG

GUCAGUCUU

LPA-
GAAGAACAUGUCAGUCUUG
201
GACGAUCAAGACUG
601
GAAGAACAUG
1001

4286
AUCGTC

ACAUGUUCUUCCU

UCAGUCUUG

LPA-
AAGAACAUGUCAGUCUUGG
202
AGACGUCCAAGACU
602
AAGAACAUGU
1002

4287
ACGUCT

GACAUGUUCUUCC

CAGUCUUGG

LPA-
AGAACAUGUCAGUCUUGGU
203
UAGACUACCAAGAC
603
AGAACAUGUC
1003

4288
AGUCTA

UGACAUGUUCUUC

AGUCUUGGU

LPA-
GGCAUCGGAGGAUCCCAUU
204
UAGUAUAAUGGGAU
604
GGCAUCGGAG
1004

4325
AUACTA

CCUCCGAUGCCAA

GAUCCCAUU

LPA-
ACUAUCCAAAUGCUGGCCU
205
CUGGUUAGGCCAGC
605
ACUAUCCAAA
1005

4346
AACCAG

AUUUGGAUAGUAU

UGCUGGCCU

LPA-
GCACAGAGGCUCCUUCUGA
206
GCUUGUUCAGAAGG
606
GCACAGAGGC
1006

4517
ACAAGC

AGCCUCUGUGCUU

UCCUUCUGA

LPA-
UCCUUCUGAACAAGCACCA
207
CUCAGUUGGUGCUU
607
UCCUUCUGAA
1007

4527
ACUGAG

GUUCAGAAGGAGC

CAAGCACCA

LPA-
CCUUCUGAACAAGCACCAC
208
UCUCAUGUGGUGCU
608
CCUUCUGAAC
1008

4528
AUGAGA

UGUUCAGAAGGAG

AAGCACCAC

LPA-
CUUCUGAACAAGCACCACC
209
UUCUCUGGUGGUGC
609
CUUCUGAACA
1009

4529
AGAGAA

UUGUUCAGAAGGA

AGCACCACC

LPA-
UUCUGAACAAGCACCACCU
210
UUUCUUAGGUGGUG
610
UUCUGAACAA
1010

4530
AAGAAA

CUUGUUCAGAAGG

GCACCACCU

LPA-
UCUGAACAAGCACCACCUG
211
UUUUCUCAGGUGGU
611
UCUGAACAAG
1011

4531
AGAAAA

GCUUGUUCAGAAG

CACCACCUG

LPA-
CUGAACAAGCACCACCUGA
212
CUUUUUUCAGGUGG
612
CUGAACAAGC
1012

4532
AAAAAG

UGCUUGUUCAGAA

ACCACCUGA

LPA-
UGAACAAGCACCACCUGAG
213
GCUUUUCUCAGGUG
613
UGAACAAGCA
1013

4533
AAAAGC

GUGCUUGUUCAGA

CCACCUGAG

LPA-
GAACAAGCACCACCUGAGA
214
GGCUUUUCUCAGGU
614
GAACAAGCAC
1014

4531
AAAGCC

GGUGCUUGUUCAG

CACCUGAGA

LPA-
AACAAGCACCACCUGAGAA
215
GGGCUUUUCUCAGG
615
AACAAGCACC
1015

4535
AAGCCC

UGGUGCUUGUUCA

ACCUGAGAA

LPA-
CAAGCACCACCUGAGAAAA
216
CAGGGUUUUUCUCA
616
CAAGCACCAC
1016

4537
ACCCTG

GGUGGUGCUUGUU

CUGAGAAAA

LPA-
AAGCACCACCUGAGAAAAG
217
ACAGGUCUUUUCUC
617
AAGCACCACC
1017

4538
ACCUGT

AGGUGGUGCUUGU

UGAGAAAAG

LPA-
AGCACCACCUGAGAAAAGC
218
CACAGUGCUUUUCU
618
AGCACCACCU
1018

4539
ACUGTG

CAGGUGGUGCUUG

GAGAAAAGC

LPA-
CUGAGAAAAGCCCUGUGGU
219
UCCUGUACCACAGG
619
CUGAGAAAAG
1019

4547
ACAGGA

GCUUUUCUCAGGU

CCCUGUGGU

LPA-
GCCCUGUGGUCCAGGAUUG
220
UGGUAUCAAUCCUG
620
GCCCUGUGGU
1020

4556
AUACCA

GACCACAGGGCUU

CCAGGAUUG

LPA-
CUGUGGUCCAGGAUUGCUA
221
CCAUGUUAGCAAUC
621
CUGUGGUCCA
1021

4559
ACAUGG

CUGGACCACAGGG

GGAUUGCUA

LPA-
CUCCACCACUGUCACAGGA
222
GGUCCUUCCUGUGA
622
CUCCACCACU
1022

4611
AGGACC

CAGUGGUGGAGGA

GUCACAGGA

LPA-
UCCACCACUGUCACAGGAA
223
AGGUCUUUCCUGUG
623
UCCACCACUG
1023

4612
AGACCT

ACAGUGGUGGAGG

UCACAGGAA

LPA-
UCUUGGUCAUCUAUGAUAC
224
AGUGUUGUAUCAUA
624
UCUUGGUCAU
1024

4642
AACACT

GAUGACCAAGAUU

CUAUGAUAC

LPA-
CUUGGUCAUCUAUGAUACC
225
CAGUGUGGUAUCAU
625
CUUGGUCAUC
1025

4643
ACACTG

AGAUGACCAAGAU

UAUGAUACC

LPA-
UUGGUCAUCUAUGAUACCA
226
CCAGUUUGGUAUCA
626
UUGGUCAUCU
1026

4644
AACUGG

UAGAUGACCAAGA

AUGAUACCA

LPA-
UGGUCAUCUAUGAUACCAC
227
GCCAGUGUGGUAUC
627
UGGUCAUCUA
1027

4645
ACUGGC

AUAGAUGACCAAG

UGAUACCAC

LPA-
GGUCAUCUAUGAUACCACA
228
UGCCAUUGUGGUAU
628
GGUCAUCUAU
1028

4646
AUGGCA

CAUAGAUGACCAA

GAUACCACA

LPA-
GUCAUCUAUGAUACCACAC
229
AUGCCUGUGUGGUA
629
GUCAUCUAUG
1029

4647
AGGCAT

UCAUAGAUGACCA

AUACCACAC

LPA-
UCAUCUAUGAUACCACACU
230
GAUGCUAGUGUGGU
630
UCAUCUAUGA
1030

4648
AGCATC

AUCAUAGAUGACC

UACCACACU

LPA-
CAUCUAUGAUACCACACUG
231
UGAUGUCAGUGUGG
631
CAUCUAUGAU
1031

4649
ACAUCA

UAUCAUAGAUGAC

ACCACACUG

LPA-
AUCUAUGAUACCACACUGG
232
CUGAUUCCAGUGUG
632
AUCUAUGAUA
1032

4650
AAUCAG

GUAUCAUAGAUGA

CCACACUGG

LPA-
UCUAUGAUACCACACUGGC
233
UCUGAUGCCAGUGU
633
UCUAUGAUAC
1033

4651
AUCAGA

GGUAUCAUAGAUG

CACACUGGC

LPA-
CUAUGAUACCACACUGGCA
234
CUCUGUUGCCAGUG
634
CUAUGAUACC
1034

4652
ACAGAG

UGGUAUCAUAGAU

ACACUGGCA

LPA-
UGAUACCACACUGGCAUCA
235
GUCCUUUGAUGCCA
635
UGAUACCACA
1035

4655
AAGGAC

GUGUGGUAUCAUA

CUGGCAUCA

LPA-
AUACCACACUGGCAUCAGA
236
GGGUCUUCUGAUGC
636
AUACCACACU
1036

4657
AGACCC

CAGUGUGGUAUCA

GGCAUCAGA

LPA-
AGAGGACCCCAGAAAACUA
237
UUUGGUUAGUUUUC
637
AGAGGACCCC
1037

4673
ACCAAA

UGGGGUCCUCUGA

AGAAAACUA

LPA-
GAGGACCCCAGAAAACUAC
238
AUUUGUGUAGUUUU
638
GAGGACCCCA
1038

4674
ACAAAT

CUGGGGUCCUCUG

GAAAACUAC

LPA-
AGAACUACUGCAGGAAUCC
239
GAAUCUGGAUUCCU
639
AGAACUACUG
1039

4712
AGAUTC

GCAGUAGUUCUCG

CAGGAAUCC

LPA-
ACUACUGCAGGAAUCCAGA
240
CCAGAUUCUGGAUU
640
ACUACUGCAG
1040

4715
AUCUGG

CCUGCAGUAGUUC

GAAUCCAGA

LPA-
UACUGCAGGAAUCCAGAUU
241
UCCCAUAAUCUGGA
641
UACUGCAGGA
1041

4717
AUGGGA

UUCCUGCAGUAGU

AUCCAGAUU

LPA-
ACUGCAGGAAUCCAGAUUC
242
UUCCCUGAAUCUGG
642
ACUGCAGGAA
1042

4718
AGGGAA

AUUCCUGCAGUAG

UCCAGAUUC

LPA-
CUGCAGGAAUCCAGAUUCU
243
UUUCCUAGAAUCUG
643
CUGCAGGAAU
1043

4719
AGGAAA

GAUUCCUGCAGUA

CCAGAUUCU

LPA-
UGCAGGAAUCCAGAUUCUG
244
GUUUCUCAGAAUCU
644
UGCAGGAAUC
1044

4720
AGAAAC

GGAUUCCUGCAGU

CAGAUUCUG

LPA-
GCAGGAAUCCAGAUUCUGG
245
UGUUUUCCAGAAUC
645
GCAGGAAUCC
1045

4721
AAAACA

UGGAUUCCUGCAG

AGAUUCUGG

LPA-
GGAAUCCAGAUUCUGGGAA
246
GGUUGUUUCCCAGA
646
GGAAUCCAGA
1046

4724
ACAACC

AUCUGGAUUCCUG

UUCUGGGAA

LPA-
GGGAAACAACCCUGGUGUU
247
UUGUGUAACACCAG
647
GGGAAACAAC
1047

4738
ACACAA

GGUUGUUUCCCAG

CCUGGUGUU

LPA-
GGAAACAACCCUGGUGUUA
248
GUUGUUUAACACCA
648
GGAAACAACC
1048

4739
AACAAC

GGGUUGUUUCCCA

CUGGUGUUA

LPA-
UGUGUGAGGUGGGAGUACU
249
GAUUGUAGUACUCC
649
UGUGUGAGGU
1049

4771
ACAATC

CACCUCACACACG

GGGAGUACU

LPA-
GUGUGAGGUGGGAGUACUG
250
AGAUUUCAGUACUC
650
GUGUGAGGUG
1050

4772
AAAUCT

CCACCUCACACAC

GGAGUACUG

LPA-
GUGAGGUGGGAGUACUGCA
251
UCAGAUUGCAGUAC
651
GUGAGGUGGG
1051

4774
AUCUGA

UCCCACCUCACAC

AGUACUGCA

LPA-
UGAGGUGGGAGUACUGCAA
252
GUCAGUUUGCAGUA
652
UGAGGUGGGA
1052

4775
ACUGAC

CUCCCACCUCACA

GUACUGCAA

LPA-
CUGACACAAUGCUCAGAAA
253
AUUCUUUUUCUGAG
653
CUGACACAAU
1053

4795
AAGAAT

CAUUGUGUCAGAU

GCUCAGAAA

LPA-
UGACACAAUGCUCAGAAAC
254
GAUUCUGUUUCUGA
654
UGACACAAUG
1054

4796
AGAATC

GCAUUGUGUCAGA

CUCAGAAAC

LPA-
GACACAAUGCUCAGAAACA
255
UGAUUUUGUUUCUG
655
GACACAAUGC
1055

4797
AAAUCA

AGCAUUGUGUCAG

UCAGAAACA

LPA-
ACACAAUGCUCAGAAACAG
256
CUGAUUCUGUUUCU
656
ACACAAUGCU
1056

4798
AAUCAG

GAGCAUUGUGUCA

CAGAAACAG

LPA-
CACAAUGCUCAGAAACAGA
257
CCUGAUUCUGUUUC
657
CACAAUGCUC
1057

4799
AUCAGG

UGAGCAUUGUGUC

AGAAACAGA

LPA-
ACAAUGCUCAGAAACAGAA
258
ACCUGUUUCUGUUU
658
ACAAUGCUCA
1058

4800
ACAGGT

CUGAGCAUUGUGU

GAAACAGAA

LPA-
CAAUGCUCAGAAACAGAAU
259
CACCUUAUUCUGUU
659
CAAUGCUCAG
1059

4801
AAGGTG

UCUGAGCAUUGUG

AAACAGAAU

LPA-
AAUGCUCAGAAACAGAAUC
260
ACACCUGAUUCUGU
660
AAUGCUCAGA
1060

4802
AGGUGT

UUCUGAGCAUUGU

AACAGAAUC

LPA-
AUGCUCAGAAACAGAAUCA
261
GACACUUGAUUCUG
661
AUGCUCAGAA
1061

4803
AGUGTC

UUUCUGAGCAUUG

ACAGAAUCA

LPA-
UGCUCAGAAACAGAAUCAG
262
GGACAUCUGAUUCU
662
UGCUCAGAAA
1062

4804
AUGUCC

GUUUCUGAGCAUU

CAGAAUCAG

LPA-
CUCAGAAACAGAAUCAGGU
263
UAGGAUACCUGAUU
663
CUCAGAAACA
1063

4806
AUCCTA

CUGUUUCUGAGCA

GAAUCAGGU

LPA-
CAGAAACAGAAUCAGGUGU
264
UCUAGUACACCUGA
664
CAGAAACAGA
1064

4808
ACUAGA

UUCUGUUUCUGAG

AUCAGGUGU

LPA-
AGAAACAGAAUCAGGUGUC
265
CUCUAUGACACCUG
665
AGAAACAGAA
1065

4809
AUAGAG

AUUCUGUUUCUGA

UCAGGUGUC

LPA-
GAAACAGAAUCAGGUGUCC
266
UCUCUUGGACACCU
666
GAAACAGAAU
1066

4810
AAGAGA

GAUUCUGUUUCUG

CAGGUGUCC

LPA-
AAACAGAAUCAGGUGUCCU
267
GUCUCUAGGACACC
667
AAACAGAAUC
1067

4811
AGAGAC

UGAUUCUGUUUCU

AGGUGUCCU

LPA-
AACAGAAUCAGGUGUCCUA
268
AGUCUUUAGGACAC
668
AACAGAAUCA
1068

4812
AAGACT

CUGAUUCUGUUUC

GGUGUCCUA

LPA-
CAGAAUCAGGUGUCCUAGA
269
GGAGUUUCUAGGAC
669
CAGAAUCAGG
1069

4814
AACUCC

ACCUGAUUCUGUU

UGUCCUAGA

LPA-
GAAUCAGGUGUCCUAGAGA
270
UGGGAUUCUCUAGG
670
GAAUCAGGUG
1070

4816
AUCCCA

ACACCUGAUUCUG

UCCUAGAGA

LPA-
AUCAGGUGUCCUAGAGACU
271
AGUGGUAGUCUCUA
671
AUCAGGUGUC
1071

4818
ACCACT

GGACACCUGAUUC

CUAGAGACU

LPA-
GGUGUCCUAGAGACUCCCA
272
CAACAUUGGGAGUC
672
GGUGUCCUAG
1072

4822
AUGUTG

UCUAGGACACCUG

AGACUCCCA

LPA-
CCUAGAGACUCCCACUGUU
273
UGGAAUAACAGUGG
673
CCUAGAGACU
1073

4827
AUUCCA

GAGUCUCUAGGAC

CCCACUGUU

LPA-
CUAGAGACUCCCACUGUUG
274
CUGGAUCAACAGUG
674
CUAGAGACUC
1074

4828
AUCCAG

GGAGUCUCUAGGA

CCACUGUUG

LPA-
UAGAGACUCCCACUGUUGU
275
ACUGGUACAACAGU
675
UAGAGACUCC
1075

4829
ACCAGT

GGGAGUCUCUAGG

CACUGUUGU

LPA-
AGAGACUCCCACUGUUGUU
276
AACUGUAACAACAG
676
AGAGACUCCC
1076

4830
ACAGTT

UGGGAGUCUCUAG

ACUGUUGUU

LPA-
GAGACUCCCACUGUUGUUC
277
GAACUUGAACAACA
677
GAGACUCCCA
1077

4831
AAGUTC

GUGGGAGUCUCUA

CUGUUGUUC

LPA-
AGACUCCCACUGUUGUUCC
278
GGAACUGGAACAAC
678
AGACUCCCAC
1078

4832
AGUUCC

AGUGGGAGUCUCU

UGUUGUUCC

LPA-
GCUCAUUCUGAAGCAGCAC
279
CAGUUUGUGCUGCU
679
GCUCAUUCUG
1079

4867
AAACTG

UCAGAAUGAGCCU

AAGCAGCAC

LPA-
CUCAUUCUGAAGCAGCACC
280
UCAGUUGGUGCUGC
680
CUCAUUCUGA
1080

4868
AACUGA

UUCAGAAUGAGCC

AGCAGCACC

LPA-
UCAUUCUGAAGCAGCACCA
281
CUCAGUUGGUGCUG
681
UCAUUCUGAA
1081

4869
ACUGAG

CUUCAGAAUGAGC

GCAGCACCA

LPA-
CAUUCUGAAGCAGCACCAA
282
GCUCAUUUGGUGCU
682
CAUUCUGAAG
1082

4870
AUGAGC

GCUUCAGAAUGAG

CAGCACCAA

LPA-
AUUCUGAAGCAGCACCAAC
283
UGCUCUGUUGGUGC
683
AUUCUGAAGC
1083

4871
AGAGCA

UGCUUCAGAAUGA

AGCACCAAC

LPA-
UUCUGAAGCAGCACCAACU
284
UUGCUUAGUUGGUG
684
UUCUGAAGCA
1084

4872
AAGCAA

CUGCUUCAGAAUG

GCACCAACU

LPA-
UCUGAAGCAGCACCAACUG
285
UUUGCUCAGUUGGU
685
UCUGAAGCAG
1085

4873
AGCAAA

GCUGCUUCAGAAU

CACCAACUG

LPA-
CUGAAGCAGCACCAACUGA
286
GUUUGUUCAGUUGG
686
CUGAAGCAGC
1086

4874
ACAAAC

UGCUGCUUCAGAA

ACCAACUGA

LPA-
UGAAGCAGCACCAACUGAG
287
GGUUUUCUCAGUUG
687
UGAAGCAGCA
1087

4875
AAAACC

GUGCUGCUUCAGA

CCAACUGAG

LPA-
GAAGCAGCACCAACUGAGC
288
GGGUUUGCUCAGUU
688
GAAGCAGCAC
1088

4876
AAACCC

GGUGCUGCUUCAG

CAACUGAGC

LPA-
AAGCAGCACCAACUGAGCA
289
GGGGUUUGCUCAGU
689
AAGCAGCACC
1089

4877
AACCCC

UGGUGCUGCUUCA

AACUGAGCA

LPA-
CAGUGCUACCAUGGUAAUG
290
UCUGGUCAUUACCA
690
CAGUGCUACC
1090

4912
ACCAGA

UGGUAGCACUGCC

AUGGUAAUG

LPA-
AGUGCUACCAUGGUAAUGG
291
CUCUGUCCAUUACC
691
AGUGCUACCA
1091

4913
ACAGAG

AUGGUAGCACUGC

UGGUAAUGG

LPA-
ACAUUCUCCACCACUGUCA
292
UUCCUUUGACAGUG
692
ACAUUCUCCA
1092

4948
AAGGAA

GUGGAGAAUGUGC

CCACUGUCA

LPA-
CACUGUCACAGGAAGGACA
293
UUGACUUGUCCUUC
693
CACUGUCACA
1093

4959
AGUCAA

CUGUGACAGUGGU

GGAAGGACA

LPA-
ACUGUCACAGGAAGGACAU
294
AUUGAUAUGUCCUU
694
ACUGUCACAG
1094

4960
AUCAAT

CCUGUGACAGUGG

GAAGGACAU

LPA-
CUGUCACAGGAAGGACAUG
295
GAUUGUCAUGUCCU
695
CUGUCACAGG
1095

4961
ACAATC

UCCUGUGACAGUG

AAGGACAUG

LPA-
UGUCACAGGAAGGACAUGU
296
AGAUUUACAUGUCC
696
UGUCACAGGA
1096

4962
AAAUCT

UUCCUGUGACAGU

AGGACAUGU

LPA-
GUCACAGGAAGGACAUGUC
297
AAGAUUGACAUGUC
697
GUCACAGGAA
1097

4963
AAUCTT

CUUCCUGUGACAG

GGACAUGUC

LPA-
UCACAGGAAGGACAUGUCA
298
CAAGAUUGACAUGU
698
UCACAGGAAG
1098

4964
AUCUTG

CCUUCCUGUGACA

GACAUGUCA

LPA-
ACAGGAAGGACAUGUCAAU
299
ACCAAUAUUGACAU
699
ACAGGAAGGA
1099

4966
AUUGGT

GUCCUUCCUGUGA

CAUGUCAAU

LPA-
CAGGAAGGACAUGUCAAUC
300
GACCAUGAUUGACA
700
CAGGAAGGAC
1100

4967
AUGGTC

UGUCCUUCCUGUG

AUGUCAAUC

LPA-
AGGAAGGACAUGUCAAUCU
301
UGACCUAGAUUGAC
701
AGGAAGGACA
1101

4968
AGGUCA

AUGUCCUUCCUGU

UGUCAAUCU

LPA-
GGAAGGACAUGUCAAUCUU
302
AUGACUAAGAUUGA
702
GGAAGGACAU
1102

4969
AGUCAT

CAUGUCCUUCCUG

GUCAAUCUU

LPA-
GAAGGACAUGUCAAUCUUG
303
GAUGAUCAAGAUUG
703
GAAGGACAUG
1103

4970
AUCATC

ACAUGUCCUUCCU

UCAAUCUUG

LPA-
AAGGACAUGUCAAUCUUGG
304
GGAUGUCCAAGAUU
704
AAGGACAUGU
1104

4971
ACAUCC

GACAUGUCCUUCC

CAAUCUUGG

LPA-
AGGACAUGUCAAUCUUGGU
305
UGGAUUACCAAGAU
705
AGGACAUGUC
1105

4972
AAUCCA

UGACAUGUCCUUC

AAUCUUGGU

LPA-
GGACAUGUCAAUCUUGGUC
306
AUGGAUGACCAAGA
706
GGACAUGUCA
1106

4973
AUCCAT

UUGACAUGUCCUU

AUCUUGGUC

LPA-
GACAUGUCAAUCUUGGUCA
307
CAUGGUUGACCAAG
707
GACAUGUCAA
1107

4974
ACCATG

AUUGACAUGUCCU

UCUUGGUCA

LPA-
ACAUGUCAAUCUUGGUCAU
308
UCAUGUAUGACCAA
708
ACAUGUCAAU
1108

4975
ACAUGA

GAUUGACAUGUCC

CUUGGUCAU

LPA-
CAUGUCAAUCUUGGUCAUC
309
GUCAUUGAUGACCA
709
CAUGUCAAUC
1109

4976
AAUGAC

AGAUUGACAUGUC

UUGGUCAUC

LPA-
AUGUCAAUCUUGGUCAUCC
310
UGUCAUGGAUGACC
710
AUGUCAAUCU
1110

4977
AUGACA

AAGAUUGACAUGU

UGGUCAUCC

LPA-
UGUCAAUCUUGGUCAUCCA
311
GUGUCUUGGAUGAC
711
UGUCAAUCUU
1111

4978
AGACAC

CAAGAUUGACAUG

GGUCAUCCA

LPA-
GUCAAUCUUGGUCAUCCAU
312
GGUGUUAUGGAUGA
712
GUCAAUCUUG
1112

4979
AACACC

CCAAGAUUGACAU

GUCAUCCAU

LPA-
UCAAUCUUGGUCAUCCAUG
313
UGGUGUCAUGGAUG
713
UCAAUCUUGG
1113

4980
ACACCA

ACCAAGAUUGACA

UCAUCCAUG

LPA-
CAAUCUUGGUCAUCCAUGA
314
GUGGUUUCAUGGAU
714
CAAUCUUGGU
1114

4981
AACCAC

GACCAAGAUUGAC

CAUCCAUGA

LPA-
AAUCUUGGUCAUCCAUGAC
315
UGUGGUGUCAUGGA
715
AAUCUUGGUC
1115

4982
ACCACA

UGACCAAGAUUGA

AUCCAUGAC

LPA-
AUCUUGGUCAUCCAUGACA
316
GUGUGUUGUCAUGG
716
AUCUUGGUCA
1116

4983
ACACAC

AUGACCAAGAUUG

UCCAUGACA

LPA-
UGACAAUGAACUACUGCAG
317
GGAUUUCUGCAGUA
717
UGACAAUGAA
1117

5048
AAAUCC

GUUCAUUGUCAGG

CUACUGCAG

LPA-
GACAAUGAACUACUGCAGG
318
UGGAUUCCUGCAGU
718
GACAAUGAAC
1118

5049
AAUCCA

AGUUCAUUGUCAG

UACUGCAGG

LPA-
ACAAUGAACUACUGCAGGA
319
CUGGAUUCCUGCAG
719
ACAAUGAACU
1119

5050
AUCCAG

UAGUUCAUUGUCA

ACUGCAGGA

LPA-
CAAUGAACUACUGCAGGAA
320
UCUGGUUUCCUGCA
720
CAAUGAACUA
1120

5051
ACCAGA

GUAGUUCAUUGUC

CUGCAGGAA

LPA-
AAUGAACUACUGCAGGAAU
321
AUCUGUAUUCCUGC
721
AAUGAACUAC
1121

5052
ACAGAT

AGUAGUUCAUUGU

UGCAGGAAU

LPA-
AUGAACUACUGCAGGAAUC
322
CAUCUUGAUUCCUG
722
AUGAACUACU
1122

5053
AAGATG

CAGUAGUUCAUUG

GCAGGAAUC

LPA-
UGAACUACUGCAGGAAUCC
323
GCAUCUGGAUUCCU
723
UGAACUACUG
1123

5054
AGAUGC

GCAGUAGUUCAUU

CAGGAAUCC

LPA-
CUACUGCAGGAAUCCAGAU
324
AUCGGUAUCUGGAU
724
CUACUGCAGG
1124

5058
ACCGAT

UCCUGCAGUAGUU

AAUCCAGAU

LPA-
CAGGCCCUUGGUGUUUUAC
325
UCCAUUGUAAAACA
725
CAGGCCCUUG
1125

5084
AAUGGA

CCAAGGGCCUGUA

GUGUUUUAC

LPA-
CUUGGUGUUUUACCAUGGA
326
CUGGGUUCCAUGGU
726
CUUGGUGUUU
1126

5090
ACCCAG

AAAACACCAAGGG

UACCAUGGA

LPA-
UUGGUGUUUUACCAUGGAC
327
GCUGGUGUCCAUGG
727
UUGGUGUUUU
1127

5091
ACCAGC

UAAAACACCAAGG

ACCAUGGAC

LPA-
UGGUGUUUUACCAUGGACC
328
UGCUGUGGUCCAUG
728
UGGUGUUUUA
1128

5092
ACAGCA

GUAAAACACCAAG

CCAUGGACC

LPA-
GGUGUUUUACCAUGGACCC
329
AUGCUUGGGUCCAU
729
GGUGUUUUAC
1129

5093
AAGCAT

GGUAAAACACCAA

CAUGGACCC

LPA-
GUGUUUUACCAUGGACCCC
330
GAUGCUGGGGUCCA
730
GUGUUUUACC
1130

5094
AGCATC

UGGUAAAACACCA

AUGGACCCC

LPA-
GUUUUACCAUGGACCCCAG
331
CUGAUUCUGGGGUC
731
GUUUUACCAU
1131

5096
AAUCAG

CAUGGUAAAACAC

GGACCCCAG

LPA-
GGAGUACUGCAACCUGACG
332
GCAUCUCGUCAGGU
732
GGAGUACUGC
1132

5124
AGAUGC

UGCAGUACUCCCA

AACCUGACG

LPA-
GAGUACUGCAACCUGACGC
333
AGCAUUGCGUCAGG
733
GAGUACUGCA
1133

5125
AAUGCT

UUGCAGUACUCCC

ACCUGACGC

LPA-
GUACUGCAACCUGACGCGA
334
UGAGCUUCGCGUCA
734
GUACUGCAAC
1134

5127
AGCUCA

GGUUGCAGUACUC

CUGACGCGA

LPA-
UACUGCAACCUGACGCGAU
335
CUGAGUAUCGCGUC
735
UACUGCAACC
1135

5128
ACUCAG

AGGUUGCAGUACU

UGACGCGAU

LPA-
UGCAACCUGACGCGAUGCU
336
UGUCUUAGCAUCGC
736
UGCAACCUGA
1136

5131
AAGACA

GUCAGGUUGCAGU

CGCGAUGCU

LPA-
CCUGACGCGAUGCUCAGAC
337
UUCUGUGUCUGAGC
737
CCUGACGCGA
1137

5136
ACAGAA

AUCGCGUCAGGUU

UGCUCAGAC

LPA-
CUGACGCGAUGCUCAGACA
338
CUUCUUUGUCUGAG
738
CUGACGCGAU
1138

5137
AAGAAG

CAUCGCGUCAGGU

GCUCAGACA

LPA-
GAUGCUCAGACACAGAAGG
339
ACAGUUCCUUCUGU
739
GAUGCUCAGA
1139

5144
AACUGT

GUCUGAGCAUCGC

CACAGAAGG

LPA-
AUGCUCAGACACAGAAGGG
340
CACAGUCCCUUCUG
740
AUGCUCAGAC
1140

5145
ACUGTG

UGUCUGAGCAUCG

ACAGAAGGG

LPA-
AGACACAGAAGGGACUGUG
341
AGCGAUCACAGUCC
741
AGACACAGAA
1141

5151
AUCGCT

CUUCUGUGUCUGA

GGGACUGUG

LPA-
GCAUCCUCUUCAUUUGAUU
342
UCCCAUAAUCAAAU
742
GCAUCCUCUU
1142

5467
AUGGGA

GAAGAGGAUGCAC

CAUUUGAUU

LPA-
CAUCCUCUUCAUUUGAUUG
343
UUCCCUCAAUCAAA
743
CAUCCUCUUC
1143

5468
AGGGAA

UGAAGAGGAUGCA

AUUUGAUUG

LPA-
AUCCUCUUCAUUUGAUUGU
344
CUUCCUACAAUCAA
744
AUCCUCUUCA
1144

5469
AGGAAG

AUGAAGAGGAUGC

UUUGAUUGU

LPA-
UCCUCUUCAUUUGAUUGUG
345
GCUUCUCACAAUCA
745
UCCUCUUCAU
1145

5470
AGAAGC

AAUGAAGAGGAUG

UUGAUUGUG

LPA-
CCUCUUCAUUUGAUUGUGG
346
GGCUUUCCACAAUC
746
CCUCUUCAUU
1146

5471
AAAGCC

AAAUGAAGAGGAU

UGAUUGUGG

LPA-
CUUCAUUUGAUUGUGGGAA
347
UGAGGUUUCCCACA
747
CUUCAUUUGA
1147

5474
ACCUCA

AUCAAAUGAAGAG

UUGUGGGAA

LPA-
UUCAUUUGAUUGUGGGAAG
348
UUGAGUCUUCCCAC
748
UUCAUUUGAU
1148

5475
ACUCAA

AAUCAAAUGAAGA

UGUGGGAAG

LPA-
UCAUUUGAUUGUGGGAAGC
349
CUUGAUGCUUCCCA
749
UCAUUUGAUU
1149

5476
AUCAAG

CAAUCAAAUGAAG

GUGGGAAGC

LPA-
CAUUUGAUUGUGGGAAGCC
350
ACUUGUGGCUUCCC
750
CAUUUGAUUG
1150

5477
ACAAGT

ACAAUCAAAUGAA

UGGGAAGCC

LPA-
AUUUGAUUGUGGGAAGCCU
351
CACUUUAGGCUUCC
751
AUUUGAUUGU
1151

5478
AAAGTG

CACAAUCAAAUGA

GGGAAGCCU

LPA-
GUGGGAAGCCUCAAGUGGA
352
UUCGGUUCCACUUG
752
GUGGGAAGCC
1152

5486
ACCGAA

AGGCUUCCCACAA

UCAAGUGGA

LPA-
AAGAAAUGUCCUGGAAGCA
353
CUACAUUGCUUCCA
753
AAGAAAUGUC
1153

5509
AUGUAG

GGACAUUUCUUCG

CUGGAAGCA

LPA-
AGAAAUGUCCUGGAAGCAU
354
CCUACUAUGCUUCC
754
AGAAAUGUCC
1154

5510
AGUAGG

AGGACAUUUCUUC

UGGAAGCAU

LPA-
GAAAUGUCCUGGAAGCAUU
355
CCCUAUAAUGCUUC
755
GAAAUGUCCU
1155

5511
AUAGGG

CAGGACAUUUCUU

GGAAGCAUU

LPA-
AAUGUCCUGGAAGCAUUGU
356
CCCCCUACAAUGCU
756
AAUGUCCUGG
1156

5513
AGGGGG

UCCAGGACAUUUC

AAGCAUUGU

LPA-
AUGUCCUGGAAGCAUUGUA
357
CCCCCUUACAAUGC
757
AUGUCCUGGA
1157

5514
AGGGGG

UUCCAGGACAUUU

AGCAUUGUA

LPA-
AGAACAAGGUUUGGAAAGC
358
AGAAGUGCUUUCCA
758
AGAACAAGGU
1158

5581
ACUUCT

AACCUUGUUCUGA

UUGGAAAGC

LPA-
GAACAAGGUUUGGAAAGCA
359
CAGAAUUGCUUUCC
759
GAACAAGGUU
1159

5582
AUUCTG

AAACCUUGUUCUG

UGGAAAGCA

LPA-
AACAAGGUUUGGAAAGCAC
360
ACAGAUGUGCUUUC
760
AACAAGGUUU
1160

5583
AUCUGT

CAAACCUUGUUCU

GGAAAGCAC

LPA-
ACAAGGUUUGGAAAGCACU
361
CACAGUAGUGCUUU
761
ACAAGGUUUG
1161

5584
ACUGTG

CCAAACCUUGUUC

GAAAGCACU

LPA-
CAAGGUUUGGAAAGCACUU
362
CCACAUAAGUGCUU
762
CAAGGUUUGG
1162

5585
AUGUGG

UCCAAACCUUGUU

AAAGCACUU

LPA-
AAGGUUUGGAAAGCACUUC
363
UCCACUGAAGUGCU
763
AAGGUUUGGA
1163

5586
AGUGGA

UUCCAAACCUUGU

AAGCACUUC

LPA-
AGGUUUGGAAAGCACUUCU
364
CUCCAUAGAAGUGC
764
AGGUUUGGAA
1164

5587
AUGGAG

UUUCCAAACCUUG

AGCACUUCU

LPA-
UGGAAAGCACUUCUGUGGA
365
GGUGCUUCCACAGA
765
UGGAAAGCAC
1165

5592
AGCACC

AGUGCUUUCCAAA

UUCUGUGGA

LPA-
GUGGAGGCACCUUAAUAUC
366
UCUGGUGAUAUUAA
766
GUGGAGGCAC
1166

5606
ACCAGA

GGUGCCUCCACAG

CUUAAUAUC

LPA-
CUUAAUAUCCCCAGAGUGG
367
CAGCAUCCACUCUG
767
CUUAAUAUCC
1167

5616
AUGCTG

GGGAUAUUAAGGU

CCAGAGUGG

LPA-
UAAUAUCCCCAGAGUGGGU
36
GUCAGUACCCACUC
768
UAAUAUCCCC
1168

5618
ACUGAC

UGGGGAUAUUAAG

AGAGUGGGU

LPA-
AGAGUGGGUGCUGACUGCU
369
GUGAGUAGCAGUCA
769
AGAGUGGGUG
1169

5628
ACUCAC

GCACCCACUCUGG

CUGACUGCU

LPA-
CAAGGUCAUCCUGGGUGCA
370
UUGGUUUGCACCCA
770
CAAGGUCAUC
1170

5685
AACCAA

GGAUGACCUUGUA

CUGGGUGCA

LPA-
CCUGGGUGCACACCAAGAA
371
GUUCAUUUCUUGGU
771
CCUGGGUGCA
1171

5694
AUGAAC

GUGCACCCAGGAU

CACCAAGAA

LPA-
GUGCACACCAAGAAGUGAA
372
UCGAGUUUCACUUC
772
GUGCACACCA
1172

5699
ACUCGA

UUGGUGUGCACCC

AGAAGUGAA

LPA-
AGCAGAUAUUGCCUUGCUA
373
UAGCUUUAGCAAGG
773
AGCAGAUAUU
1173

5775
AAGCTA

CAAUAUCUGCUUG

GCCUUGCUA

LPA-
GCAGAUAUUGCCUUGCUAA
374
UUAGCUUUAGCAAG
774
GCAGAUAUUG
1174

5776
AGCUAA

GCAAUAUCUGCUU

CCUUGCUAA

LPA-
CAGAUAUUGCCUUGCUAAA
375
CUUAGUUUUAGCAA
775
CAGAUAUUGC
1175

5777
ACUAAG

GGCAAUAUCUGCU

CUUGCUAAA

LPA-
AGAUAUUGCCUUGCUAAAG
376
GCUUAUCUUUAGCA
776
AGAUAUUGCC
1176

5778
AUAAGC

AGGCAAUAUCUGC

UUGCUAAAG

LPA-
GAUAUUGCCUUGCUAAAGC
377
UGCUUUGCUUUAGC
777
GAUAUUGCCU
1177

5779
AAAGCA

AAGGCAAUAUCUG

UGCUAAAGC

LPA-
AUAUUGCCUUGCUAAAGCU
378
CUGCUUAGCUUUAG
778
AUAUUGCCUU
1178

5780
AAGCAG

CAAGGCAAUAUCU

GCUAAAGCU

LPA-
UAUUGCCUUGCUAAAGCUA
379
CCUGCUUAGCUUUA
779
UAUUGCCUUG
1179

5781
AGCAGG

GCAAGGCAAUAUC

CUAAAGCUA

LPA-
UCAUCACUGACAAAGUAAU
380
GCUGGUAUUACUUU
780
UCAUCACUGA
1180

5813
ACCAGC

GUCAGUGAUGACG

CAAAGUAAU

LPA-
GGACUGAAUGUUACAUCAC
381
CAGCCUGUGAUGUA
781
GGACUGAAUG
1181

5873
AGGCTG

ACAUUCAGUCCUG

UUACAUCAC

LPA-
GACUGAAUGUUACAUCACU
382
CCAGCUAGUGAUGU
782
GACUGAAUGU
1182

5874
AGCUGG

AACAUUCAGUCCU

UACAUCACU

LPA-
ACUGAAUGUUACAUCACUG
383
CCCAGUCAGUGAUG
783
ACUGAAUGUU
1183

5875
ACUGGG

UAACAUUCAGUCC

ACAUCACUG

LPA-
CUGAAUGUUACAUCACUGG
384
CCCCAUCCAGUGAU
784
CUGAAUGUUA
1184

5876
AUGGGG

GUAACAUUCAGUC

CAUCACUGG

LPA-
UGAAUGUUACAUCACUGGC
385
UCCCCUGCCAGUGA
785
UGAAUGUUAC
1185

5877
AGGGGA

UGUAACAUUCAGU

AUCACUGGC

LPA-
AAUGUUACAUCACUGGCUG
386
UCUCCUCAGCCAGU
786
AAUGUUACAU
1186

5879
AGGAGA

GAUGUAACAUUCA

CACUGGCUG

LPA-
GAAACCCAAGGUACCUUUG
387
CAGUCUCAAAGGUA
787
GAAACCCAAG
1187

5902
AGACTG

CCUUGGGUUUCUC

GUACCUUUG

Control

Gal
GACAACAGAAUAUUAUCCA
1188
UUGGAUAAUAUUCU
1189
GACAACAGAA
1190

XC-LPA-
AGCAGCCGAAAGGCUGC

GUUGUCGG

UAUUAUCCA

3675

NC1
CGUUAAUCGCGUAUAAUAC
1191
AUACGCGUAUUAUA
1192
N/A

GCGUAT

CGCGAUUAACGAC

NC5
CAUAUUGCGCGUAUAGUCG
1193
CUAACGCGACUAUA
1194
N/A

CGUUAG

CGCGCAAUAUGGU

NC7
GGCGCGUAUAGUCGCGCGU
1195
GACUAUACGCGCGA
1196
N/A

AUAGTC

CUAUACGCGCCUC

In Vitro Cell-Based Assays

The ability of each of the DsiRINAs listed in Table 2 to inhibit LPA expression was determined using in vitro cell-based assays. Briefly, human embryonic kidney 293 (HEK293) or HepG2 cells stably expressing a human LPA gene were transfected with each of the DsiRNAs listed in Table 2 at 0.5 nM in separate wells of a multi-well cell-culture plate. Cells were maintained for 24 hours following transfection, and then the amount of remaining LPA mRNA from the transfected cells was determined using TAQMAN®-based qPCR assays. Two qPCR assays, a 3′ assay and a 5′ assay, were used to determine LPA mRNA levels as measured using PCR probes conjugated to 6-carboxyfluorescein (6-FAM).

The results of the HEK293 and HepG2 cell-based assays to evaluate the ability of the DsiRNAs listed in Table 2 to inhibit LPA expression are shown in FIGS. 1-4 and FIG. 5, respectively. Cells transfected with a GalNAc-conjugated LPA oligonucleotide (GalXC-LPA-3675 SEQ ID NO: 1188 and 1189) were used as a positive control. DsiRNAs that resulted in less than or equal to about 15%-20% LPA mRNA remaining in DsiRNA-transfected cells when compared to mock-transfected cells were generally considered to comprise sequences that provide a suitable amount of knockdown or reduction of target mRNA expression for further evaluation. In FIGS. 1-5, the percent of LPA mRNA remaining in cells transfected with DsiRNAs, as indicated, relative to time-matched control cells is shown (3′ assay=circle shapes; 5′ assay=triangle shapes).

To further evaluate the DsiRNA hits, a subset of the DsiRNAs listed in Table 2 were tested to determine their ability to inhibit LPA expression using in vitro cell-based assays at two different DsiRNA concentrations (FIG. 6 and FIG. 7). Briefly, HEK293 cells stably expressing a human LPA gene were transfected with DsiRNAs at 0.1 nM and 0.5 nM in separate wells of a multi-well cell-culture plate. Cells were maintained for 24 hr. following transfection, and then the amount of remaining LPA mRNA from the transfected cells was determined using TAQMAN®-based qPCR assays. Two qPCR assays, a 3′ assay and a 5′ assay, were used to determine LPA mRNA levels as measured using PCR probes conjugated to hexachloro-fluorescein (HEX). Untransfected cells (UT), mock-transfected cells (Mock), and cells transfected with control oligonucleotides (NC1, SEQ ID NOs: 1191 and 1192; NC5, SEQ ID NO: 1193 and 1194; and NC7, SEQ ID NO: 1195 and 1196) were used as negative controls. As shown in FIGS. 6 and 7, the percent of LPA mRNA remaining in HEK293 cells transfected with the indicated DsiRNAs is an average of the LPA mRNA levels from the 3′ assay and 5′ assay and is normalized to time-matched, mock-transfected control HEK293 cells.

Taken together, these results show that DsiRNAs designed to target human LPA mRNA inhibit LPA expression in cells, as determined by a reduced amount of LPA mRNA in DsiRNA-transfected cells relative to control cells. These results demonstrate that the nucleotide sequences comprising the DsiRNA are useful for generating RNAi oligonucleotides to inhibit LPA expression. Further, these results demonstrate that multiple LPA mRNA target sequences are suitable for the RNAi-mediated inhibition of LPA expression.

Example 3: RNAi Oligonucleotide Inhibition of LPA Expression In Vivo

Of the DsiRNAs screened in the cell-based assays described in Example 2, the nucleotide sequences of 14 DsiRNAs were selected for further evaluation in vivo. Briefly, the nucleotide sequences of the 14 selected DsiRNAs were used to generate 14 corresponding double-stranded RNAi oligonucleotides comprising a nicked tetraloop GalNAc-conjugated structure (referred to herein as “GalNAc-conjugated LPA oligonucleotides”) having a 36-mer passenger strand and a 22-mer guide strand (Table 3). Further, the nucleotide sequences comprising the passenger strand and guide strand of the GalNAc-conjugated LPA oligonucleotides have a distinct pattern of modified nucleotides and phosphorothioate linkages (e.g., see FIG. 10 for a schematic of the generic structure and chemical modification patterns (M1, M2, and M3) of the GalNAc-conjugated LPA oligonucleotides). The three adenosine nucleotides comprising the tetraloop are each conjugated to a GalNAc moiety (CAS #: 14131-60-3).

TABLE 3

GalNAc-Conjugated LPA Oligonucleotides Evaluated in Mice

SEQ ID NO
SEQ ID NO

Oligonucleotide
DP#
(Sense)
(Antisense)

LPA-0190-M1
DP15791P:DP15790G
388
788

LPA-0501-M1
DP15634P:DP15633G
389
789

LPA-3100-M1
DP15639P:DP15638G
390
790

LPA-3286-M1
DP15643P:DP15642G
391
791

LPA-3288-M1
DP15645P:DP15644G
392
792

LPA-3291-M1
DP15647P:DP15646G
393
793

LPA-3584-M1
DP15651P:DP15650G
394
794

LPA-3585-M1
DP15653P:DP15652G
395
795

LPA-4645-M1
DP15657P:DP15656G
396
796

LPA-4717-M1
DP15801P:DP15800G
397
797

LPA-5510-M1
DP15815P:DP15814G
398
798

LPA-3750-M1
DP13346P:DP13385G
399
799

LPA-2900-M2
DP13351P:DP14623G
400
800

LPA-3675-M2
DP13346P:DP14624G
401
801

LPA-2900-M3
DP13351P:DP13387G
402
802

LPA-3675-M3
DP13346P:DP13385G
403
803

Mouse Studies

The GalNAc-conjugated LPA oligonucleotides listed in Table 3 were evaluated in an HDI mouse model, wherein HDI mice were engineered to transiently express human LPA mRNA in hepatocytes. The GalNAc-conjugated LPA oligonucleotide LPA-3675-M2 was used as a benchmark control. Briefly, 6-8-week-old female CD-1 mice (n=5) were treated subcutaneously with the indicated GalNAc-conjugated LPA oligonucleotides at a dose level of 0.5 mg/kg (FIG. 8) or at a dose level of 0.25 mg/kg, 0.5 mg/kg, and 1 mg/kg (FIG. 9). Three days later (72 h), the mice were hydrodynamically injected (HDI) with a DNA plasmid encoding the full human LPA gene under control of a ubiquitous cytomegalovirus (CMV) promoter sequence. One day after introduction of the DNA plasmid, liver samples from mice were collected. Total RNA derived from these mice were subjected to qRT-PCR analysis for LPA mRNA, relative to mice treated only with an identical volume of PBS. The values were normalized for transfection efficiency using the NeoR gene included on the plasmid.

As shown in FIG. 8, the indicated GalNAc-conjugated LPA oligonucleotides inhibited LPA expression, as determined by a reduction in the amount of LPA mRNA in liver samples from oligonucleotide-treated HDI mice relative to mice treated with PBS. To further evaluate the ability of GalNAc-conjugated LPA oligonucleotides to inhibit LPA expression, two of the GalNAc-conjugated LPA oligonucleotide sequences (LPA-2900 and LPA-3675) each having a different chemical modification pattern (M2 and M3) were tested for their ability to inhibit LPA expression in the HDI mice described above at three different concentrations (0.25 mg/kg, 0.5 mg/kg, and 1.0 mg/kg). As shown in FIG. 9, the indicated GalNAc-conjugated LPA oligonucleotides inhibited LPA expression in HDI mice in a dose-dependent manner.

Taken together, these results show that GalNAc-conjugated LPA oligonucleotides designed to target human LPA mRNA inhibit LPA expression in mice, as determined by a reduction in the amount of LPA mRNA in HDI mouse livers relative to control mice treated with PBS. Based on these results, 10 of the 14 GalNAc-conjugated LPA oligonucleotides evaluated in HDI mice were selected for evaluation of their ability to inhibit LPA expression in non-human primates (NHPs). The 10 GalNAc-conjugated LPA oligonucleotides listed in Table 4 comprise chemically modified nucleotides having pattern M1, M2, or M3 as described in FIG. 10.

TABLE 4

GalNAc-Conjugated LPA Oligonucleotides Evaluated in NHPs

SEQ ID NO
SEQ ID NO

Oligonucleotide
DP#
(Sense)
(Antisense)

LPA-0190-M1
DP15791P:DP15790G
388
788

LPA-3100-M1
DP15639P:DP15638G
390
790

LPA-3288-M1
DP15645P:DP15644G
392
792

LPA-3291-M1
DP15647P:DP15646G
393
793

LPA-3585-M1
DP15653P:DP15652G
395
795

LPA-4645-M1
DP15657P:DP15656G
396
796

LPA-4717-M1
DP15801P:DP15800G
397
797

LPA-5510-M1
DP15815P:DP15814G
398
798

LPA-2900-M2
DP13351P:DP14623G
400
800

LPA-3675-M3
DP13346P:DP13385G
403
803

Non-Human Primate (NHP) Studies

The GalNAc-conjugated LPA oligonucleotides listed in Table 4 were evaluated in cynomolgus monkeys (Macaca fascicularis). In this study, the monkeys are grouped so that their mean body weights (about 5.4 kg) are comparable between the control and experimental groups. Each cohort contains two male and three female subjects. The GalNAc-conjugated LPA oligonucleotides were administered subcutaneously on Study Day 0. Blood samples were collected on Study Days −8, −5 and 0, and weekly after dosing. Ultrasound-guided core needle liver biopsies were collected on Study Days 28, 56 and 84. At each time point, total RNA derived from the liver biopsy samples was subjected to qRT-PCR analysis to measure LPA mRNA in oligonucleotide-treated monkeys relative to monkeys treated with a comparable volume of PBS. To normalize the data, the measurements were made relative to the geometric mean of two reference genes, PPIB and 18S rRNA. As shown in FIG. 11A (Day 28), FIG. 11B (Day 56), and FIG. 11C (Day 84), treatment of NHPs with the GalNAc-conjugated LPA oligonucleotides listed in Table 4 inhibited LPA expression in the liver, as determined by a reduction in the amount of LPA mRNA in liver samples from oligonucleotide-treated NHPs relative to NHPs treated with PBS. The amount of plasminogen (PLG) mRNA in the liver samples of treated NHPs was also determined and is shown in FIG. 11D. From the same NHP study, inhibition of LPA expression was also determined by measuring apo(a) protein serum from treated NHPs by ELISA. As shown in FIG. 12, a significant reduction in serum apo(a) protein was observed in NHPs treated with GalNAc-conjugated LPA oligonucleotides compared to NHPs treated with PBS. Values from three pre-dose samples are averaged and set to 100%, and data are reported as relative values compared to the pre-dose average. Taken together, these results demonstrate that treatment of NHPs with GalNAc-conjugated LPA oligonucleotides reduced the amount of LPA mRNA in the liver and reduced the amount of apo(a) protein in the serum.

Taken together, these results show that GalNAc-conjugated LPA oligonucleotides designed to target human LPA mRNA inhibit LPA expression in vivo (as determined by the reduction of the amount of LPA mRNA and apo(a) protein in treated animals).

SEQUENCE LISTING

The following nucleic and/or amino acid sequences are referred to in the disclosure above and are provided below for reference.

TABLE 5

LPA Oligonucleotide Sequences (Unmodified)

SEQ

SEQ

Sequence
ID
Sequence
ID

Oligonucleotide
(Sense Strand)
NO:
(Antisense Strand)
NO:

LPA-125
CUGAGCAAAGCCAUGUGGUAC
4
UCCUGUACCACAUGGCUUUGCUCA
404

AGGA

GGU

LPA-128
AGCAAAGCCAUGUGGUCCAAG
5
CAAUCUUGGACCACAUGGCUUUGC
405

AUTG

UCA

LPA-132
AAGCCAUGUGGUCCAGGAUAG
6
GUAGCUAUCCUGGACCACAUGGCU
406

CUAC

UUG

LPA-133
AGCCAUGUGGUCCAGGAUUAC
7
GGUAGUAAUCCUGGACCACAUGGC
407

UACC

UUU

LPA-134
GCCAUGUGGUCCAGGAUUGAU
8
UGGUAUCAAUCCUGGACCACAUGG
408

ACCA

CUU

LPA-135
CCAUGUGGUCCAGGAUUGCAA
9
AUGGUUGCAAUCCUGGACCACAUG
409

CCAT

GCU

LPA-136
CAUGUGGUCCAGGAUUGCUAC
10
CAUGGUAGCAAUCCUGGACCACAU
410

CATG

GGC

LPA-137
AUGUGGUCCAGGAUUGCUAAC
11
CCAUGUUAGCAAUCCUGGACCACA
411

AUGG

UGG

LPA-138
UGUGGUCCAGGAUUGCUACAA
12
ACCAUUGUAGCAAUCCUGGACCAC
412

UGGT

AUG

LPA-160
GGUGAUGGACAGAGUUAUCAA
13
UGCCUUGAUAACUCUGUCCAUCAC
413

GGCA

CAU

LPA-190
UCCACCACUGUCACAGGAAAG
14
AGGUCUUUCCUGUGACAGUGGUGG
414

ACCT

AGU

LPA-191
CCACCACUGUCACAGGAAGAA
15
CAGGUUCUUCCUGUGACAGUGGUG
415

CCTG

GAG

LPA-197
CUGUCACAGGAAGGACCUGAC
16
GCUUGUCAGGUCCUUCCUGUGACA
416

AAGC

GUG

LPA-205
GGAAGGACCUGCCAAGCUUAG
17
AUGACUAAGCUUGGCAGGUCCUUC
417

UCAT

CUG

LPA-206
GAAGGACCUGCCAAGCUUGAU
18
GAUGAUCAAGCUUGGCAGGUCCUU
418

CATC

CCU

LPA-208
AGGACCUGCCAAGCUUGGUAA
19
UAGAUUACCAAGCUUGGCAGGUCC
419

UCTA

UUC

LPA-209
GGACCUGCCAAGCUUGGUCAU
20
AUAGAUGACCAAGCUUGGCAGGUC
420

CUAT

CUU

LPA-210
GACCUGCCAAGCUUGGUCAAC
21
CAUAGUUGACCAAGCUUGGCAGGU
421

UATG

CCU

LPA-211
ACCUGCCAAGCUUGGUCAUAU
22
UCAUAUAUGACCAAGCUUGGCAGG
422

AUGA

UCC

LPA-212
CCUGCCAAGCUUGGUCAUCAA
23
GUCAUUGAUGACCAAGCUUGGCAG
423

UGAC

GUC

LPA-219
AGCUUGGUCAUCUAUGACAAC
24
AUGUGUUGUCAUAGAUGACCAAGC
424

ACAT

UUG

LPA-225
GUCAUCUAUGACACCACAUAA
25
AUGUUUAUGUGGUGUCAUAGAUGA
425

ACAT

CCA

LPA-258
CACAGAAAACUACCCAAAUAC
26
GCCAGUAUUUGGGUAGUUUUCUGU
426

UGGC

GGU

LPA-261
AGAAAACUACCCAAAUGCUAG
27
CAAGCUAGCAUUUGGGUAGUUUUC
427

CUTG

UGU

LPA-263
AAAACUACCCAAAUGCUGGAU
28
AUCAAUCCAGCAUUUGGGUAGUUU
428

UGAT

UCU

LPA-269
ACCCAAAUGCUGGCUUGAUAA
29
UUCAUUAUCAAGCCAGCAUUUGGG
429

UGAA

UAG

LPA-270
CCCAAAUGCUGGCUUGAUCAU
30
GUUCAUGAUCAAGCCAGCAUUUGG
430

GAAC

GUA

LPA-291
GAACUACUGCAGGAAUCCAAA
31
AGCAUUUGGAUUCCUGCAGUAGUU
431

UGCT

CAU

LPA-295
UACUGCAGGAAUCCAGAUGAU
32
CCACAUCAUCUGGAUUCCUGCAGU
432

GUGG

AGU

LPA-296
ACUGCAGGAAUCCAGAUGCAG
33
GCCACUGCAUCUGGAUUCCUGCAG
433

UGGC

UAG

LPA-298
UGCAGGAAUCCAGAUGCUGAG
34
CUGCCUCAGCAUCUGGAUUCCUGC
434

GCAG

AGU

LPA-355
AGGUGGGAGUACUGCAACCAG
35
GCGUCUGGUUGCAGUACUCCCACC
435

ACGC

UGA

LPA-380
AAUGCUCAGACGCAGAAGGAA
36
GCAGUUCCUUCUGCGUCUGAGCAU
436

CUGC

UGC

LPA-417
GACUGUUACCCCGGUUCCAAG
37
UAGGCUUGGAACCGGGGUAACAGU
437

CCTA

CGG

LPA-418
ACUGUUACCCCGGUUCCAAAC
38
CUAGGUUUGGAACCGGGGUAACAG
438

CUAG

UCG

LPA-419
CUGUUACCCCGGUUCCAAGAC
39
UCUAGUCUUGGAACCGGGGUAACA
439

UAGA

GUC

LPA-420
UGUUACCCCGGUUCCAAGCAU
40
CUCUAUGCUUGGAACCGGGGUAAC
440

AGAG

AGU

LPA-421
GUUACCCCGGUUCCAAGCCAA
41
CCUCUUGGCUUGGAACCGGGGUAA
441

GAGG

CAG

LPA-422
UUACCCCGGUUCCAAGCCUAG
42
GCCUCUAGGCUUGGAACCGGGGUA
442

AGGC

ACA

LPA-423
UACCCCGGUUCCAAGCCUAAA
43
AGCCUUUAGGCUUGGAACCGGGGU
443

GGCT

AAC

LPA-492
GUGCUACCAUGGUAAUGGAAA
44
ACUCUUUCCAUUACCAUGGUAGCA
444

GAGT

CUC

LPA-493
UGCUACCAUGGUAAUGGACAG
45
AACUCUGUCCAUUACCAUGGUAGC
445

AGTT

ACU

LPA-494
GCUACCAUGGUAAUGGACAAA
46
UAACUUUGUCCAUUACCAUGGUAG
446

GUTA

CAC

LPA-495
CUACCAUGGUAAUGGACAGAG
47
AUAACUCUGUCCAUUACCAUGGUA
447

UUAT

GCA

LPA-496
UACCAUGGUAAUGGACAGAAU
48
GAUAAUUCUGUCCAUUACCAUGGU
448

UATC

AGC

LPA-497
ACCAUGGUAAUGGACAGAGAU
49
CGAUAUCUCUGUCCAUUACCAUGG
449

AUCG

UAG

LPA-498
CCAUGGUAAUGGACAGAGUAA
50
UCGAUUACUCUGUCCAUUACCAUG
450

UCGA

GUA

LPA-499
CAUGGUAAUGGACAGAGUUAU
51
CUCGAUAACUCUGUCCAUUACCAU
451

CGAG

GGU

LPA-500
AUGGUAAUGGACAGAGUUAAC
52
CCUCGUUAACUCUGUCCAUUACCA
452

GAGG

UGG

LPA-501
UGGUAAUGGACAGAGUUAUAG
53
GCCUCUAUAACUCUGUCCAUUACC
453

AGGC

AUG

LPA-502
GGUAAUGGACAGAGUUAUCAA
54
UGCCUUGAUAACUCUGUCCAUUAC
454

GGCA

CAU

LPA-503
GUAAUGGACAGAGUUAUCGAG
55
GUGCCUCGAUAACUCUGUCCAUUA
455

GCAC

CCA

LPA-523
GGCACAUACUCCACCACUGAC
56
CUGUGUCAGUGGUGGAGUAUGUGC
456

ACAG

CUC

LPA-563
CUUGGUCAUCUAUGACACCAC
57
GAGUGUGGUGUCAUAGAUGACCAA
457

ACTC

GCU

LPA-567
GUCAUCUAUGACACCACACAC
58
AUGCGUGUGUGGUGUCAUAGAUGA
458

GCAT

CCA

LPA-568
UCAUCUAUGACACCACACUAG
59
UAUGCUAGUGUGGUGUCAUAGAUG
459

CATA

ACC

LPA-569
CAUCUAUGACACCACACUCAC
60
CUAUGUGAGUGUGGUGUCAUAGAU
460

AUAG

GAC

LPA-1208
GCACAUACUCCACCACUGUAA
61
CCAGUUACAGUGGUGGAGUAUGUG
461

CUGG

CCU

LPA-2715
AGCCCCUUAUUGUUAUACGAG
62
AUCCCUCGUAUAACAAUAAGGGGC
462

GGAT

UGC

LPA-2716
GCCCCUUAUUGUUAUACGAAG
63
GAUCCUUCGUAUAACAAUAAGGGG
463

GATC

CUG

LPA-2827
CCAAGCCUAGAGGCUCCUUAU
64
GUUCAUAAGGAGCCUCUAGGCUUG
464

GAAC

GAA

LPA-2837
AGGCUCCUUCUGAACAAGCAC
65
GUUGGUGCUUGUUCAGAAGGAGCC
465

CAAC

UCU

LPA-2900
AUGGACAGAGUUAUCAAGGAA
66
UAUGUUCCUUGAUAACUCUGUCCA
466

CATA

UUU

LPA-2901
UGGACAGAGUUAUCAAGGCAC
67
GUAUGUGCCUUGAUAACUCUGUCC
467

AUAC

AUU

LPA-2902
GGACAGAGUUAUCAAGGCAAA
68
AGUAUUUGCCUUGAUAACUCUGUC
468

UACT

CAU

LPA-2903
GACAGAGUUAUCAAGGCACAU
69
AAGUAUGUGCCUUGAUAACUCUGU
469

ACTT

CCA

LPA-2904
ACAGAGUUAUCAAGGCACAAA
70
GAAGUUUGUGCCUUGAUAACUCUG
470

CUTC

UCC

LPA-2905
CAGAGUUAUCAAGGCACAUAC
71
UGAAGUAUGUGCCUUGAUAACUCU
471

UUCA

GUC

LPA-3004
UACCCAAAUGCUGGCUUGAAC
72
UCUUGUUCAAGCCAGCAUUUGGGU
472

AAGA

AGU

LPA-3007
CCAAAUGCUGGCUUGAUCAAG
73
AGUUCUUGAUCAAGCCAGCAUUUG
473

AACT

GGU

LPA-3023
UCAAGAACUACUGCCGAAAAC
74
UCUGGUUUUCGGCAGUAGUUCUUG
474

CAGA

AUC

LPA-3024
CAAGAACUACUGCCGAAAUAC
75
AUCUGUAUUUCGGCAGUAGUUCUU
475

AGAT

GAU

LPA-3025
AAGAACUACUGCCGAAAUCAA
76
GAUCUUGAUUUCGGCAGUAGUUCU
476

GATC

UGA

LPA-3027
GAACUACUGCCGAAAUCCAAA
77
AGGAUUUGGAUUUCGGCAGUAGUU
477

UCCT

CUU

LPA-3030
CUACUGCCGAAAUCCAGAUAC
78
CACAGUAUCUGGAUUUCGGCAGUA
478

UGTG

GUU

LPA-3051
UGUGGCAGCCCCUUGGUGUAA
79
UGUAUUACACCAAGGGGCUGCCAC
479

UACA

AGG

LPA-3052
GUGGCAGCCCCUUGGUGUUAU
80
UUGUAUAACACCAAGGGGCUGCCA
480

ACAA

CAG

LPA-3053
UGGCAGCCCCUUGGUGUUAAA
81
GUUGUUUAACACCAAGGGGCUGCC
481

CAAC

ACA

LPA-3054
GGCAGCCCCUUGGUGUUAUAC
82
UGUUGUAUAACACCAAGGGGCUGC
482

AACA

CAC

LPA-3055
GCAGCCCCUUGGUGUUAUAAA
83
CUGUUUUAUAACACCAAGGGGCUG
483

ACAG

CCA

LPA-3056
CAGCCCCUUGGUGUUAUACAA
84
UCUGUUGUAUAACACCAAGGGGCU
484

CAGA

GCC

LPA-3057
AGCCCCUUGGUGUUAUACAAC
85
AUCUGUUGUAUAACACCAAGGGGC
485

AGAT

UGC

LPA-3058
GCCCCUUGGUGUUAUACAAAA
86
GAUCUUUUGUAUAACACCAAGGGG
486

GATC

CUG

LPA-3059
CCCCUUGGUGUUAUACAACAG
87
GGAUCUGUUGUAUAACACCAAGGG
487

AUCC

GCU

LPA-3092
GGUGGGAGUACUGCAACCUAA
88
CGUGUUAGGUUGCAGUACUCCCAC
488

CACG

CUG

LPA-3093
GUGGGAGUACUGCAACCUGAC
89
UCGUGUCAGGUUGCAGUACUCCCA
489

ACGA

CCU

LPA-3096
GGAGUACUGCAACCUGACAAG
90
GCAUCUUGUCAGGUUGCAGUACUC
490

AUGC

CCA

LPA-3097
GAGUACUGCAACCUGACACAA
91
AGCAUUGUGUCAGGUUGCAGUACU
491

UGCT

CCC

LPA-3099
GUACUGCAACCUGACACGAAG
92
UGAGCUUCGUGUCAGGUUGCAGUA
492

CUCA

CUC

LPA-3100
UACUGCAACCUGACACGAUAC
93
CUGAGUAUCGUGUCAGGUUGCAGU
493

UCAG

ACU

LPA-3101
ACUGCAACCUGACACGAUGAU
94
UCUGAUCAUCGUGUCAGGUUGCAG
494

CAGA

UAC

LPA-3102
CUGCAACCUGACACGAUGCAC
95
AUCUGUGCAUCGUGUCAGGUUGCA
495

AGAT

GUA

LPA-3103
UGCAACCUGACACGAUGCUAA
96
CAUCUUAGCAUCGUGUCAGGUUGC
496

GATG

AGU

LPA-3105
CAACCUGACACGAUGCUCAAA
97
UGCAUUUGAGCAUCGUGUCAGGUU
497

UGCA

GCA

LPA-3107
ACCUGACACGAUGCUCAGAAG
98
UCUGCUUCUGAGCAUCGUGUCAGG
498

CAGA

UUG

LPA-3108
CCUGACACGAUGCUCAGAUAC
99
UUCUGUAUCUGAGCAUCGUGUCAG
499

AGAA

GUU

LPA-3109
CUGACACGAUGCUCAGAUGAA
100
AUUCUUCAUCUGAGCAUCGUGUCA
500

GAAT

GGU

LPA-3110
UGACACGAUGCUCAGAUGCAG
101
CAUUCUGCAUCUGAGCAUCGUGUC
501

AATG

AGG

LPA-3111
GACACGAUGCUCAGAUGCAAA
102
CCAUUUUGCAUCUGAGCAUCGUGU
502

AUGG

CAG

LPA-3112
ACACGAUGCUCAGAUGCAGAA
103
UCCAUUCUGCAUCUGAGCAUCGUG
503

UGGA

UCA

LPA-3113
CACGAUGCUCAGAUGCAGAAU
104
GUCCAUUCUGCAUCUGAGCAUCGU
504

GGAC

GUC

LPA-3229
UGCUACUACCAUUAUGGACAG
105
AACUCUGUCCAUAAUGGUAGUAGC
505

AGTT

AGU

LPA-3230
GCUACUACCAUUAUGGACAAA
106
UAACUUUGUCCAUAAUGGUAGUAG
506

GUTA

CAG

LPA-3231
CUACUACCAUUAUGGACAGAG
107
GUAACUCUGUCCAUAAUGGUAGUA
507

UUAC

GCA

LPA-3232
UACUACCAUUAUGGACAGAAU
108
GGUAAUUCUGUCCAUAAUGGUAGU
508

UACC

AGC

LPA-3233
ACUACCAUUAUGGACAGAGAU
109
CGGUAUCUCUGUCCAUAAUGGUAG
509

ACCG

UAG

LPA-3234
CUACCAUUAUGGACAGAGUAA
110
UCGGUUACUCUGUCCAUAAUGGUA
510

CCGA

GUA

LPA-3235
UACCAUUAUGGACAGAGUUAC
111
CUCGGUAACUCUGUCCAUAAUGGU
511

CGAG

AGU

LPA-3236
ACCAUUAUGGACAGAGUUAAC
112
CCUCGUUAACUCUGUCCAUAAUGG
512

GAGG

UAG

LPA-3257
GAGGCACAUACUCCACCACAG
113
GUGACUGUGGUGGAGUAUGUGCCU
513

UCAC

CGG

LPA-3267
CUCCACCACUGUCACAGGAAG
114
AGUUCUUCCUGUGACAGUGGUGGA
514

AACT

GUA

LPA-3280
ACAGGAAGAACUUGCCAAGAU
115
ACCAAUCUUGGCAAGUUCUUCCUG
515

UGGT

UGA

LPA-3281
CAGGAAGAACUUGCCAAGCAU
116
GACCAUGCUUGGCAAGUUCUUCCU
516

GGTC

GUG

LPA-3282
AGGAAGAACUUGCCAAGCUAG
117
UGACCUAGCUUGGCAAGUUCUUCC
517

GUCA

UGU

LPA-3283
GGAAGAACUUGCCAAGCUUAG
118
AUGACUAAGCUUGGCAAGUUCUUC
518

UCAT

CUG

LPA-3284
GAAGAACUUGCCAAGCUUGAU
119
GAUGAUCAAGCUUGGCAAGUUCUU
519

CATC

CCU

LPA-3285
AAGAACUUGCCAAGCUUGGAC
120
AGAUGUCCAAGCUUGGCAAGUUCU
520

AUCT

UCC

LPA-3286
AGAACUUGCCAAGCUUGGUAA
121
UAGAUUACCAAGCUUGGCAAGUUC
521

UCTA

UUC

LPA-3287
GAACUUGCCAAGCUUGGUCAU
122
AUAGAUGACCAAGCUUGGCAAGUU
522

CUAT

CUU

LPA-3288
AACUUGCCAAGCUUGGUCAAC
123
CAUAGUUGACCAAGCUUGGCAAGU
523

UATG

UCU

LPA-3289
ACUUGCCAAGCUUGGUCAUAU
124
UCAUAUAUGACCAAGCUUGGCAAG
524

AUGA

UUC

LPA-3290
CUUGCCAAGCUUGGUCAUCAA
125
GUCAUUGAUGACCAAGCUUGGCAA
525

UGAC

GUU

LPA-3291
UUGCCAAGCUUGGUCAUCUAU
126
UGUCAUAGAUGACCAAGCUUGGCA
526

GACA

AGU

LPA-3292
UGCCAAGCUUGGUCAUCUAAG
127
GUGUCUUAGAUGACCAAGCUUGGC
527

ACAC

AAG

LPA-3298
GCUUGGUCAUCUAUGACACAA
128
GGUGUUGUGUCAUAGAUGACCAAG
528

CACC

CUU

LPA-3300
UUGGUCAUCUAUGACACCAAA
129
CUGGUUUGGUGUCAUAGAUGACCA
529

CCAG

AGC

LPA-3301
UGGUCAUCUAUGACACCACAC
130
GCUGGUGUGGUGUCAUAGAUGACC
530

CAGC

AAG

LPA-3303
GUCAUCUAUGACACCACACAA
131
AUGCUUGUGUGGUGUCAUAGAUGA
531

GCAT

CCA

LPA-3305
CAUCUAUGACACCACACCAAC
132
CUAUGUUGGUGUGGUGUCAUAGAU
532

AUAG

GAC

LPA-3306
AUCUAUGACACCACACCAGAA
133
ACUAUUCUGGUGUGGUGUCAUAGA
533

UAGT

UGA

LPA-3308
CUAUGACACCACACCAGCAAA
134
CGACUUUGCUGGUGUGGUGUCAUA
534

GUCG

GAU

LPA-3329
GUCGGACCCCAGAAAACUAAC
135
UUUGGUUAGUUUUCUGGGGUCCGA
535

CAAA

CUA

LPA-3330
UCGGACCCCAGAAAACUACAC
136
AUUUGUGUAGUUUUCUGGGGUCCG
536

AAAT

ACU

LPA-3340
GAAAACUACCCAAAUGCUGAC
137
UCAGGUCAGCAUUUGGGUAGUUUU
537

CUGA

CUG

LPA-3391
GCUGAGAUUCGCCCUUGGUAU
138
UGUAAUACCAAGGGCGAAUCUCAG
538

UACA

CAU

LPA-3392
CUGAGAUUCGCCCUUGGUGAU
139
GUGUAUCACCAAGGGCGAAUCUCA
539

ACAC

GCA

LPA-3394
GAGAUUCGCCCUUGGUGUUAC
140
UGGUGUAACACCAAGGGCGAAUCU
540

ACCA

CAG

LPA-3395
AGAUUCGCCCUUGGUGUUAAA
141
AUGGUUUAACACCAAGGGCGAAUC
541

CCAT

UCA

LPA-3398
UUCGCCCUUGGUGUUACACAA
142
UCCAUUGUGUAACACCAAGGGCGA
542

UGGA

AUC

LPA-3404
CUUGGUGUUACACCAUGGAAC
143
CUGGGUUCCAUGGUGUAACACCAA
543

CCAG

GGG

LPA-3405
UUGGUGUUACACCAUGGAUAC
144
ACUGGUAUCCAUGGUGUAACACCA
544

CAGT

AGG

LPA-3406
UGGUGUUACACCAUGGAUCAC
145
CACUGUGAUCCAUGGUGUAACACC
545

AGTG

AAG

LPA-3407
GGUGUUACACCAUGGAUCCAA
146
ACACUUGGAUCCAUGGUGUAACAC
546

GUGT

CAA

LPA-3409
UGUUACACCAUGGAUCCCAAU
147
UGACAUUGGGAUCCAUGGUGUAAC
547

GUCA

ACC

LPA-3472
GAAUCAAGUGUCCUUGCAAAU
148
UGAGAUUUGCAAGGACACUUGAUU
548

CUCA

CUG

LPA-3473
AAUCAAGUGUCCUUGCAACAC
149
GUGAGUGUUGCAAGGACACUUGAU
549

UCAC

UCU

LPA-3474
AUCAAGUGUCCUUGCAACUAU
150
CGUGAUAGUUGCAAGGACACUUGA
550

CACG

UUC

LPA-3584
AUGGACAGAGUUAUCGAGGAU
151
AAUGAUCCUCGAUAACUCUGUCCA
551

CATT

UCA

LPA-3585
UGGACAGAGUUAUCGAGGCAC
152
GAAUGUGCCUCGAUAACUCUGUCC
552

AUTC

AUC

LPA-3655
ACACCACACUGGCAUCAGAAG
153
UUGUCUUCUGAUGCCAGUGUGGUG
553

ACAA

UCA

LPA-3747
UUGGUGUUAUACCAUGGAUAC
154
AUUGGUAUCCAUGGUAUAACACCA
554

CAAT

AGG

LPA-3748
UGGUGUUAUACCAUGGAUCAC
155
CAUUGUGAUCCAUGGUAUAACACC
555

AATG

AAG

LPA-3749
GGUGUUAUACCAUGGAUCCAA
156
ACAUUUGGAUCCAUGGUAUAACAC
556

AUGT

CAA

LPA-3750
GUGUUAUACCAUGGAUCCCAA
157
GACAUUGGGAUCCAUGGUAUAACA
557

UGTC

CCA

LPA-3773
UCAGAUGGGAGUACUGCAAAC
158
GUCAGUUUGCAGUACUCCCAUCUG
558

UGAC

ACA

LPA-3776
GAUGGGAGUACUGCAACCUAA
159
UGUGUUAGGUUGCAGUACUCCCAU
559

CACA

CUG

LPA-3777
AUGGGAGUACUGCAACCUGAC
160
UUGUGUCAGGUUGCAGUACUCCCA
560

ACAA

UCU

LPA-3778
UGGGAGUACUGCAACCUGAAA
161
AUUGUUUCAGGUUGCAGUACUCCC
561

CAAT

AUC

LPA-3779
GGGAGUACUGCAACCUGACAC
162
CAUUGUGUCAGGUUGCAGUACUCC
562

AATG

CAU

LPA-3840
GGCUGUUUCUGAACAAGCAAC
163
CGUUGUUGCUUGUUCAGAAACAGC
563

AACG

CGU

LPA-3844
GUUUCUGAACAAGCACCAAAG
164
GCUCCUUUGGUGCUUGUUCAGAAA
564

GAGC

CAG

LPA-3927
CUCCACCACUGUUACAGGAAG
165
UGUCCUUCCUGUAACAGUGGUGGA
565

GACA

GAA

LPA-3928
UCCACCACUGUUACAGGAAAG
166
AUGUCUUUCCUGUAACAGUGGUGG
566

ACAT

AGA

LPA-3929
CCACCACUGUUACAGGAAGAA
167
CAUGUUCUUCCUGUAACAGUGGUG
567

CATG

GAG

LPA-3972
GACACCACACUGGCAUCAGAG
168
GGUUCUCUGAUGCCAGUGUGGUGU
568

AACC

CAU

LPA-3973
ACACCACACUGGCAUCAGAAA
169
UGGUUUUCUGAUGCCAGUGUGGUG
569

ACCA

UCA

LPA-3999
AGAAUACUACCCAAAUGGUAG
170
CAGGCUACCAUUUGGGUAGUAUUC
570

CCTG

UGU

LPA-4000
GAAUACUACCCAAAUGGUGAC
171
UCAGGUCACCAUUUGGGUAGUAUU
571

CUGA

CUG

LPA-4001
AAUACUACCCAAAUGGUGGAC
172
GUCAGUCCACCAUUUGGGUAGUAU
572

UGAC

UCU

LPA-4185
UCCUUCUGAAGAAGCACCAAC
173
UUCAGUUGGUGCUUCUUCAGAAGG
573

UGAA

AAG

LPA-4186
CCUUCUGAAGAAGCACCAAAU
174
UUUCAUUUGGUGCUUCUUCAGAAG
574

GAAA

GAA

LPA-4187
CUUCUGAAGAAGCACCAACAG
175
UUUUCUGUUGGUGCUUCUUCAGAA
575

AAAA

GGA

LPA-4188
UUCUGAAGAAGCACCAACUAA
176
GUUUUUAGUUGGUGCUUCUUCAGA
576

AAAC

AGG

LPA-4189
UCUGAAGAAGCACCAACUGAA
177
UGUUUUCAGUUGGUGCUUCUUCAG
577

AACA

AAG

LPA-4190
CUGAAGAAGCACCAACUGAAA
178
CUGUUUUCAGUUGGUGCUUCUUCA
578

ACAG

GAA

LPA-4191
UGAAGAAGCACCAACUGAAAA
179
GCUGUUUUCAGUUGGUGCUUCUUC
579

CAGC

AGA

LPA-4192
GAAGAAGCACCAACUGAAAAC
180
UGCUGUUUUCAGUUGGUGCUUCUU
580

AGCA

CAG

LPA-4193
AAGAAGCACCAACUGAAAAAA
181
GUGCUUUUUUCAGUUGGUGCUUCU
581

GCAC

UCA

LPA-4194
AGAAGCACCAACUGAAAACAG
182
AGUGCUGUUUUCAGUUGGUGCUUC
582

CACT

UUC

LPA-4195
GAAGCACCAACUGAAAACAAC
183
CAGUGUUGUUUUCAGUUGGUGCUU
583

ACTG

CUU

LPA-4196
AAGCACCAACUGAAAACAGAA
184
CCAGUUCUGUUUUCAGUUGGUGCU
584

CUGG

UCU

LPA-4239
AGGUGAUGGACAGAGUUAUAG
185
GCCUCUAUAACUCUGUCCAUCACC
585

AGGC

UCG

LPA-4269
CUCCACCACUAUCACAGGAAG
186
UGUUCUUCCUGUGAUAGUGGUGGA
586

AACA

GAG

LPA-4270
UCCACCACUAUCACAGGAAAA
187
AUGUUUUUCCUGUGAUAGUGGUGG
587

ACAT

AGA

LPA-4271
CCACCACUAUCACAGGAAGAA
188
CAUGUUCUUCCUGUGAUAGUGGUG
588

CATG

GAG

LPA-4272
CACCACUAUCACAGGAAGAAC
189
ACAUGUUCUUCCUGUGAUAGUGGU
589

AUGT

GGA

LPA-4273
ACCACUAUCACAGGAAGAAAA
190
GACAUUUUCUUCCUGUGAUAGUGG
590

UGTC

UGG

LPA-4274
CCACUAUCACAGGAAGAACAU
191
UGACAUGUUCUUCCUGUGAUAGUG
591

GUCA

GUG

LPA-4275
CACUAUCACAGGAAGAACAAG
192
CUGACUUGUUCUUCCUGUGAUAGU
592

UCAG

GGU

LPA-4276
ACUAUCACAGGAAGAACAUAU
193
ACUGAUAUGUUCUUCCUGUGAUAG
593

CAGT

UGG

LPA-4277
CUAUCACAGGAAGAACAUGAC
194
GACUGUCAUGUUCUUCCUGUGAUA
594

AGTC

GUG

LPA-4278
UAUCACAGGAAGAACAUGUAA
195
AGACUUACAUGUUCUUCCUGUGAU
595

GUCT

AGU

LPA-4279
AUCACAGGAAGAACAUGUCAG
196
AAGACUGACAUGUUCUUCCUGUGA
596

UCTT

UAG

LPA-4280
UCACAGGAAGAACAUGUCAAU
197
CAAGAUUGACAUGUUCUUCCUGUG
597

CUTG

AUA

LPA-4281
CACAGGAAGAACAUGUCAGAC
198
CCAAGUCUGACAUGUUCUUCCUGU
598

UUGG

GAU

LPA-4282
ACAGGAAGAACAUGUCAGUAU
199
ACCAAUACUGACAUGUUCUUCCUG
599

UGGT

UGA

LPA-4285
GGAAGAACAUGUCAGUCUUAG
200
ACGACUAAGACUGACAUGUUCUUC
600

UCGT

CUG

LPA-4286
GAAGAACAUGUCAGUCUUGAU
201
GACGAUCAAGACUGACAUGUUCUU
601

CGTC

CCU

LPA-4287
AAGAACAUGUCAGUCUUGGAC
202
AGACGUCCAAGACUGACAUGUUCU
602

GUCT

UCC

LPA-4288
AGAACAUGUCAGUCUUGGUAG
203
UAGACUACCAAGACUGACAUGUUC
603

UCTA

UUC

LPA-4325
GGCAUCGGAGGAUCCCAUUAU
204
UAGUAUAAUGGGAUCCUCCGAUGC
604

ACTA

CAA

LPA-4346
ACUAUCCAAAUGCUGGCCUAA
205
CUGGUUAGGCCAGCAUUUGGAUAG
605

CCAG

UAU

LPA-4517
GCACAGAGGCUCCUUCUGAAC
206
GCUUGUUCAGAAGGAGCCUCUGUG
606

AAGC

CUU

LPA-4527
UCCUUCUGAACAAGCACCAAC
207
CUCAGUUGGUGCUUGUUCAGAAGG
607

UGAG

AGC

LPA-4528
CCUUCUGAACAAGCACCACAU
208
UCUCAUGUGGUGCUUGUUCAGAAG
608

GAGA

GAG

LPA-4529
CUUCUGAACAAGCACCACCAG
209
UUCUCUGGUGGUGCUUGUUCAGAA
609

AGAA

GGA

LPA-4530
UUCUGAACAAGCACCACCUAA
210
UUUCUUAGGUGGUGCUUGUUCAGA
610

GAAA

AGG

LPA-4531
UCUGAACAAGCACCACCUGAG
211
UUUUCUCAGGUGGUGCUUGUUCAG
611

AAAA

AAG

LPA-4532
CUGAACAAGCACCACCUGAAA
212
CUUUUUUCAGGUGGUGCUUGUUCA
612

AAAG

GAA

LPA-4533
UGAACAAGCACCACCUGAGAA
213
GCUUUUCUCAGGUGGUGCUUGUUC
613

AAGC

AGA

LPA-4534
GAACAAGCACCACCUGAGAAA
214
GGCUUUUCUCAGGUGGUGCUUGUU
614

AGCC

CAG

LPA-4535
AACAAGCACCACCUGAGAAAA
215
GGGCUUUUCUCAGGUGGUGCUUGU
615

GCCC

UCA

LPA-4537
CAAGCACCACCUGAGAAAAAC
216
CAGGGUUUUUCUCAGGUGGUGCUU
616

CCTG

GUU

LPA-4538
AAGCACCACCUGAGAAAAGAC
217
ACAGGUCUUUUCUCAGGUGGUGCU
617

CUGT

UGU

LPA-4539
AGCACCACCUGAGAAAAGCAC
218
CACAGUGCUUUUCUCAGGUGGUGC
618

UGTG

UUG

LPA-4547
CUGAGAAAAGCCCUGUGGUAC
219
UCCUGUACCACAGGGCUUUUCUCA
619

AGGA

GGU

LPA-4556
GCCCUGUGGUCCAGGAUUGAU
220
UGGUAUCAAUCCUGGACCACAGGG
620

ACCA

CUU

LPA-4559
CUGUGGUCCAGGAUUGCUAAC
221
CCAUGUUAGCAAUCCUGGACCACA
621

AUGG

GGG

LPA-4611
CUCCACCACUGUCACAGGAAG
222
GGUCCUUCCUGUGACAGUGGUGGA
622

GACC

GGA

LPA-4612
UCCACCACUGUCACAGGAAAG
223
AGGUCUUUCCUGUGACAGUGGUGG
623

ACCT

AGG

LPA-4642
UCUUGGUCAUCUAUGAUACAA
224
AGUGUUGUAUCAUAGAUGACCAAG
624

CACT

AUU

LPA-4643
CUUGGUCAUCUAUGAUACCAC
225
CAGUGUGGUAUCAUAGAUGACCAA
625

ACTG

GAU

LPA-4644
UUGGUCAUCUAUGAUACCAAA
226
CCAGUUUGGUAUCAUAGAUGACCA
626

CUGG

AGA

LPA-4645
UGGUCAUCUAUGAUACCACAC
227
GCCAGUGUGGUAUCAUAGAUGACC
627

UGGC

AAG

LPA-4646
GGUCAUCUAUGAUACCACAAU
228
UGCCAUUGUGGUAUCAUAGAUGAC
628

GGCA

CAA

LPA-4647
GUCAUCUAUGAUACCACACAG
229
AUGCCUGUGUGGUAUCAUAGAUGA
629

GCAT

CCA

LPA-4648
UCAUCUAUGAUACCACACUAG
230
GAUGCUAGUGUGGUAUCAUAGAUG
630

CATC

ACC

LPA-4649
CAUCUAUGAUACCACACUGAC
231
UGAUGUCAGUGUGGUAUCAUAGAU
631

AUCA

GAC

LPA-4650
AUCUAUGAUACCACACUGGAA
232
CUGAUUCCAGUGUGGUAUCAUAGA
632

UCAG

UGA

LPA-4651
UCUAUGAUACCACACUGGCAU
233
UCUGAUGCCAGUGUGGUAUCAUAG
633

CAGA

AUG

LPA-4652
CUAUGAUACCACACUGGCAAC
234
CUCUGUUGCCAGUGUGGUAUCAUA
634

AGAG

GAU

LPA-4655
UGAUACCACACUGGCAUCAAA
235
GUCCUUUGAUGCCAGUGUGGUAUC
635

GGAC

AUA

LPA-4657
AUACCACACUGGCAUCAGAAG
236
GGGUCUUCUGAUGCCAGUGUGGUA
636

ACCC

UCA

LPA-4673
AGAGGACCCCAGAAAACUAAC
237
UUUGGUUAGUUUUCUGGGGUCCUC
637

CAAA

UGA

LPA-4674
GAGGACCCCAGAAAACUACAC
238
AUUUGUGUAGUUUUCUGGGGUCCU
638

AAAT

CUG

LPA-4712
AGAACUACUGCAGGAAUCCAG
239
GAAUCUGGAUUCCUGCAGUAGUUC
639

AUTC

UCG

LPA-4715
ACUACUGCAGGAAUCCAGAAU
240
CCAGAUUCUGGAUUCCUGCAGUAG
640

CUGG

UUC

LPA-4717
UACUGCAGGAAUCCAGAUUAU
241
UCCCAUAAUCUGGAUUCCUGCAGU
641

GGGA

AGU

LPA-4718
ACUGCAGGAAUCCAGAUUCAG
242
UUCCCUGAAUCUGGAUUCCUGCAG
642

GGAA

UAG

LPA-4719
CUGCAGGAAUCCAGAUUCUAG
243
UUUCCUAGAAUCUGGAUUCCUGCA
643

GAAA

GUA

LPA-4720
UGCAGGAAUCCAGAUUCUGAG
244
GUUUCUCAGAAUCUGGAUUCCUGC
644

AAAC

AGU

LPA-4721
GCAGGAAUCCAGAUUCUGGAA
245
UGUUUUCCAGAAUCUGGAUUCCUG
645

AACA

CAG

LPA-4724
GGAAUCCAGAUUCUGGGAAAC
246
GGUUGUUUCCCAGAAUCUGGAUUC
646

AACC

CUG

LPA-4738
GGGAAACAACCCUGGUGUUAC
247
UUGUGUAACACCAGGGUUGUUUCC
647

ACAA

CAG

LPA-4739
GGAAACAACCCUGGUGUUAAA
248
GUUGUUUAACACCAGGGUUGUUUC
648

CAAC

CCA

LPA-4771
UGUGUGAGGUGGGAGUACUAC
249
GAUUGUAGUACUCCCACCUCACAC
649

AATC

ACG

LPA-4772
GUGUGAGGUGGGAGUACUGAA
250
AGAUUUCAGUACUCCCACCUCACA
650

AUCT

CAC

LPA-4774
GUGAGGUGGGAGUACUGCAAU
251
UCAGAUUGCAGUACUCCCACCUCA
651

CUGA

CAC

LPA-4775
UGAGGUGGGAGUACUGCAAAC
252
GUCAGUUUGCAGUACUCCCACCUC
652

UGAC

ACA

LPA-4795
CUGACACAAUGCUCAGAAAAA
253
AUUCUUUUUCUGAGCAUUGUGUCA
653

GAAT

GAU

LPA-4796
UGACACAAUGCUCAGAAACAG
254
GAUUCUGUUUCUGAGCAUUGUGUC
654

AATC

AGA

LPA-4797
GACACAAUGCUCAGAAACAAA
255
UGAUUUUGUUUCUGAGCAUUGUGU
655

AUCA

CAG

LPA-4798
ACACAAUGCUCAGAAACAGAA
256
CUGAUUCUGUUUCUGAGCAUUGUG
656

UCAG

UCA

LPA-4799
CACAAUGCUCAGAAACAGAAU
257
CCUGAUUCUGUUUCUGAGCAUUGU
657

CAGG

GUC

LPA-4800
ACAAUGCUCAGAAACAGAAAC
258
ACCUGUUUCUGUUUCUGAGCAUUG
658

AGGT

UGU

LPA-4801
CAAUGCUCAGAAACAGAAUAA
259
CACCUUAUUCUGUUUCUGAGCAUU
659

GGTG

GUG

LPA-4802
AAUGCUCAGAAACAGAAUCAG
260
ACACCUGAUUCUGUUUCUGAGCAU
660

GUGT

UGU

LPA-4803
AUGCUCAGAAACAGAAUCAAG
261
GACACUUGAUUCUGUUUCUGAGCA
661

UGTC

UUG

LPA-4804
UGCUCAGAAACAGAAUCAGAU
262
GGACAUCUGAUUCUGUUUCUGAGC
662

GUCC

AUU

LPA-4806
CUCAGAAACAGAAUCAGGUAU
263
UAGGAUACCUGAUUCUGUUUCUGA
663

CCTA

GCA

LPA-4808
CAGAAACAGAAUCAGGUGUAC
264
UCUAGUACACCUGAUUCUGUUUCU
664

UAGA

GAG

LPA-4809
AGAAACAGAAUCAGGUGUCAU
265
CUCUAUGACACCUGAUUCUGUUUC
665

AGAG

UGA

LPA-4810
GAAACAGAAUCAGGUGUCCAA
266
UCUCUUGGACACCUGAUUCUGUUU
666

GAGA

CUG

LPA-4811
AAACAGAAUCAGGUGUCCUAG
267
GUCUCUAGGACACCUGAUUCUGUU
667

AGAC

UCU

LPA-4812
AACAGAAUCAGGUGUCCUAAA
268
AGUCUUUAGGACACCUGAUUCUGU
668

GACT

UUC

LPA-4814
CAGAAUCAGGUGUCCUAGAAA
269
GGAGUUUCUAGGACACCUGAUUCU
669

CUCC

GUU

LPA-4816
GAAUCAGGUGUCCUAGAGAAU
270
UGGGAUUCUCUAGGACACCUGAUU
670

CCCA

CUG

LPA-4818
AUCAGGUGUCCUAGAGACUAC
271
AGUGGUAGUCUCUAGGACACCUGA
671

CACT

UUC

LPA-4822
GGUGUCCUAGAGACUCCCAAU
272
CAACAUUGGGAGUCUCUAGGACAC
672

GUTG

CUG

LPA-4827
CCUAGAGACUCCCACUGUUAU
273
UGGAAUAACAGUGGGAGUCUCUAG
673

UCCA

GAC

LPA-4828
CUAGAGACUCCCACUGUUGAU
274
CUGGAUCAACAGUGGGAGUCUCUA
674

CCAG

GGA

LPA-4829
UAGAGACUCCCACUGUUGUAC
275
ACUGGUACAACAGUGGGAGUCUCU
675

CAGT

AGG

LPA-4830
AGAGACUCCCACUGUUGUUAC
276
AACUGUAACAACAGUGGGAGUCUC
676

AGTT

UAG

LPA-4831
GAGACUCCCACUGUUGUUCAA
277
GAACUUGAACAACAGUGGGAGUCU
677

GUTC

CUA

LPA-4832
AGACUCCCACUGUUGUUCCAG
278
GGAACUGGAACAACAGUGGGAGUC
678

UUCC

UCU

LPA-4867
GCUCAUUCUGAAGCAGCACAA
279
CAGUUUGUGCUGCUUCAGAAUGAG
679

ACTG

CCU

LPA-4868
CUCAUUCUGAAGCAGCACCAA
280
UCAGUUGGUGCUGCUUCAGAAUGA
680

CUGA

GCC

LPA-4869
UCAUUCUGAAGCAGCACCAAC
281
CUCAGUUGGUGCUGCUUCAGAAUG
681

UGAG

AGC

LPA-4870
CAUUCUGAAGCAGCACCAAAU
282
GCUCAUUUGGUGCUGCUUCAGAAU
682

GAGC

GAG

LPA-4871
AUUCUGAAGCAGCACCAACAG
283
UGCUCUGUUGGUGCUGCUUCAGAA
683

AGCA

UGA

LPA-4872
UUCUGAAGCAGCACCAACUAA
284
UUGCUUAGUUGGUGCUGCUUCAGA
684

GCAA

AUG

LPA-4873
UCUGAAGCAGCACCAACUGAG
285
UUUGCUCAGUUGGUGCUGCUUCAG
685

CAAA

AAU

LPA-4874
CUGAAGCAGCACCAACUGAAC
286
GUUUGUUCAGUUGGUGCUGCUUCA
686

AAAC

GAA

LPA-4875
UGAAGCAGCACCAACUGAGAA
287
GGUUUUCUCAGUUGGUGCUGCUUC
687

AACC

AGA

LPA-4876
GAAGCAGCACCAACUGAGCAA
288
GGGUUUGCUCAGUUGGUGCUGCUU
688

ACCC

CAG

LPA-4877
AAGCAGCACCAACUGAGCAAA
289
GGGGUUUGCUCAGUUGGUGCUGCU
689

CCCC

UCA

LPA-4912
CAGUGCUACCAUGGUAAUGAC
290
UCUGGUCAUUACCAUGGUAGCACU
690

CAGA

GCC

LPA-4913
AGUGCUACCAUGGUAAUGGAC
291
CUCUGUCCAUUACCAUGGUAGCAC
691

AGAG

UGC

LPA-4948
ACAUUCUCCACCACUGUCAAA
292
UUCCUUUGACAGUGGUGGAGAAUG
692

GGAA

UGC

LPA-4959
CACUGUCACAGGAAGGACAAG
293
UUGACUUGUCCUUCCUGUGACAGU
693

UCAA

GGU

LPA-4960
ACUGUCACAGGAAGGACAUAU
294
AUUGAUAUGUCCUUCCUGUGACAG
694

CAAT

UGG

LPA-4961
CUGUCACAGGAAGGACAUGAC
295
GAUUGUCAUGUCCUUCCUGUGACA
695

AATC

GUG

LPA-4962
UGUCACAGGAAGGACAUGUAA
296
AGAUUUACAUGUCCUUCCUGUGAC
696

AUCT

AGU

LPA-4963
GUCACAGGAAGGACAUGUCAA
297
AAGAUUGACAUGUCCUUCCUGUGA
697

UCTT

CAG

LPA-4964
UCACAGGAAGGACAUGUCAAU
298
CAAGAUUGACAUGUCCUUCCUGUG
698

CUTG

ACA

LPA-4966
ACAGGAAGGACAUGUCAAUAU
299
ACCAAUAUUGACAUGUCCUUCCUG
699

UGGT

UGA

LPA-4967
CAGGAAGGACAUGUCAAUCAU
300
GACCAUGAUUGACAUGUCCUUCCU
700

GGTC

GUG

LPA-4968
AGGAAGGACAUGUCAAUCUAG
301
UGACCUAGAUUGACAUGUCCUUCC
701

GUCA

UGU

LPA-4969
GGAAGGACAUGUCAAUCUUAG
302
AUGACUAAGAUUGACAUGUCCUUC
702

UCAT

CUG

LPA-4970
GAAGGACAUGUCAAUCUUGAU
303
GAUGAUCAAGAUUGACAUGUCCUU
703

CATC

CCU

LPA-4971
AAGGACAUGUCAAUCUUGGAC
304
GGAUGUCCAAGAUUGACAUGUCCU
704

AUCC

UCC

LPA-4972
AGGACAUGUCAAUCUUGGUAA
305
UGGAUUACCAAGAUUGACAUGUCC
705

UCCA

UUC

LPA-4973
GGACAUGUCAAUCUUGGUCAU
306
AUGGAUGACCAAGAUUGACAUGUC
706

CCAT

CUU

LPA-4974
GACAUGUCAAUCUUGGUCAAC
307
CAUGGUUGACCAAGAUUGACAUGU
707

CATG

CCU

LPA-4975
ACAUGUCAAUCUUGGUCAUAC
308
UCAUGUAUGACCAAGAUUGACAUG
708

AUGA

UCC

LPA-4976
CAUGUCAAUCUUGGUCAUCAA
309
GUCAUUGAUGACCAAGAUUGACAU
709

UGAC

GUC

LPA-4977
AUGUCAAUCUUGGUCAUCCAU
310
UGUCAUGGAUGACCAAGAUUGACA
710

GACA

UGU

LPA-4978
UGUCAAUCUUGGUCAUCCAAG
311
GUGUCUUGGAUGACCAAGAUUGAC
711

ACAC

AUG

LPA-4979
GUCAAUCUUGGUCAUCCAUAA
312
GGUGUUAUGGAUGACCAAGAUUGA
712

CACC

CAU

LPA-4980
UCAAUCUUGGUCAUCCAUGAC
313
UGGUGUCAUGGAUGACCAAGAUUG
713

ACCA

ACA

LPA-4981
CAAUCUUGGUCAUCCAUGAAA
314
GUGGUUUCAUGGAUGACCAAGAUU
714

CCAC

GAC

LPA-4982
AAUCUUGGUCAUCCAUGACAC
315
UGUGGUGUCAUGGAUGACCAAGAU
715

CACA

UGA

LPA-4983
AUCUUGGUCAUCCAUGACAAC
316
GUGUGUUGUCAUGGAUGACCAAGA
716

ACAC

UUG

LPA-5048
UGACAAUGAACUACUGCAGAA
317
GGAUUUCUGCAGUAGUUCAUUGUC
717

AUCC

AGG

LPA-5049
GACAAUGAACUACUGCAGGAA
318
UGGAUUCCUGCAGUAGUUCAUUGU
718

UCCA

CAG

LPA-5050
ACAAUGAACUACUGCAGGAAU
319
CUGGAUUCCUGCAGUAGUUCAUUG
719

CCAG

UCA

LPA-5051
CAAUGAACUACUGCAGGAAAC
320
UCUGGUUUCCUGCAGUAGUUCAUU
720

CAGA

GUC

LPA-5052
AAUGAACUACUGCAGGAAUAC
321
AUCUGUAUUCCUGCAGUAGUUCAU
721

AGAT

UGU

LPA-5053
AUGAACUACUGCAGGAAUCAA
322
CAUCUUGAUUCCUGCAGUAGUUCA
722

GATG

UUG

LPA-5054
UGAACUACUGCAGGAAUCCAG
323
GCAUCUGGAUUCCUGCAGUAGUUC
723

AUGC

AUU

LPA-5058
CUACUGCAGGAAUCCAGAUAC
324
AUCGGUAUCUGGAUUCCUGCAGUA
724

CGAT

GUU

LPA-5084
CAGGCCCUUGGUGUUUUACAA
325
UCCAUUGUAAAACACCAAGGGCCU
725

UGGA

GUA

LPA-5090
CUUGGUGUUUUACCAUGGAAC
326
CUGGGUUCCAUGGUAAAACACCAA
726

CCAG

GGG

LPA-5091
UUGGUGUUUUACCAUGGACAC
327
GCUGGUGUCCAUGGUAAAACACCA
727

CAGC

AGG

LPA-5092
UGGUGUUUUACCAUGGACCAC
328
UGCUGUGGUCCAUGGUAAAACACC
728

AGCA

AAG

LPA-5093
GGUGUUUUACCAUGGACCCAA
329
AUGCUUGGGUCCAUGGUAAAACAC
729

GCAT

CAA

LPA-5094
GUGUUUUACCAUGGACCCCAG
330
GAUGCUGGGGUCCAUGGUAAAACA
730

CATC

CCA

LPA-5096
GUUUUACCAUGGACCCCAGAA
331
CUGAUUCUGGGGUCCAUGGUAAAA
731

UCAG

CAC

LPA-5124
GGAGUACUGCAACCUGACGAG
332
GCAUCUCGUCAGGUUGCAGUACUC
732

AUGC

CCA

LPA-5125
GAGUACUGCAACCUGACGCAA
333
AGCAUUGCGUCAGGUUGCAGUACU
733

UGCT

CCC

LPA-5127
GUACUGCAACCUGACGCGAAG
334
UGAGCUUCGCGUCAGGUUGCAGUA
734

CUCA

CUC

LPA-5128
UACUGCAACCUGACGCGAUAC
335
CUGAGUAUCGCGUCAGGUUGCAGU
735

UCAG

ACU

LPA-5131
UGCAACCUGACGCGAUGCUAA
336
UGUCUUAGCAUCGCGUCAGGUUGC
736

GACA

AGU

LPA-5136
CCUGACGCGAUGCUCAGACAC
337
UUCUGUGUCUGAGCAUCGCGUCAG
737

AGAA

GUU

LPA-5137
CUGACGCGAUGCUCAGACAAA
338
CUUCUUUGUCUGAGCAUCGCGUCA
738

GAAG

GGU

LPA-5144
GAUGCUCAGACACAGAAGGAA
339
ACAGUUCCUUCUGUGUCUGAGCAU
739

CUGT

CGC

LPA-5145
AUGCUCAGACACAGAAGGGAC
340
CACAGUCCCUUCUGUGUCUGAGCA
740

UGTG

UCG

LPA-5151
AGACACAGAAGGGACUGUGAU
341
AGCGAUCACAGUCCCUUCUGUGUC
741

CGCT

UGA

LPA-5467
GCAUCCUCUUCAUUUGAUUAU
342
UCCCAUAAUCAAAUGAAGAGGAUG
742

GGGA

CAC

LPA-5468
CAUCCUCUUCAUUUGAUUGAG
343
UUCCCUCAAUCAAAUGAAGAGGAU
743

GGAA

GCA

LPA-5469
AUCCUCUUCAUUUGAUUGUAG
344
CUUCCUACAAUCAAAUGAAGAGGA
744

GAAG

UGC

LPA-5470
UCCUCUUCAUUUGAUUGUGAG
345
GCUUCUCACAAUCAAAUGAAGAGG
745

AAGC

AUG

LPA-5471
CCUCUUCAUUUGAUUGUGGAA
346
GGCUUUCCACAAUCAAAUGAAGAG
746

AGCC

GAU

LPA-5474
CUUCAUUUGAUUGUGGGAAAC
347
UGAGGUUUCCCACAAUCAAAUGAA
747

CUCA

GAG

LPA-5475
UUCAUUUGAUUGUGGGAAGAC
348
UUGAGUCUUCCCACAAUCAAAUGA
748

UCAA

AGA

LPA-5476
UCAUUUGAUUGUGGGAAGCAU
349
CUUGAUGCUUCCCACAAUCAAAUG
749

CAAG

AAG

LPA-5477
CAUUUGAUUGUGGGAAGCCAC
350
ACUUGUGGCUUCCCACAAUCAAAU
750

AAGT

GAA

LPA-5478
AUUUGAUUGUGGGAAGCCUAA
351
CACUUUAGGCUUCCCACAAUCAAA
751

AGTG

UGA

LPA-5486
GUGGGAAGCCUCAAGUGGAAC
352
UUCGGUUCCACUUGAGGCUUCCCA
752

CGAA

CAA

LPA-5509
AAGAAAUGUCCUGGAAGCAAU
353
CUACAUUGCUUCCAGGACAUUUCU
753

GUAG

UCG

LPA-5510
AGAAAUGUCCUGGAAGCAUAG
354
CCUACUAUGCUUCCAGGACAUUUC
754

UAGG

UUC

LPA-5511
GAAAUGUCCUGGAAGCAUUAU
355
CCCUAUAAUGCUUCCAGGACAUUU
755

AGGG

CUU

LPA-5513
AAUGUCCUGGAAGCAUUGUAG
356
CCCCCUACAAUGCUUCCAGGACAU
756

GGGG

UUC

LPA-5514
AUGUCCUGGAAGCAUUGUAAG
357
CCCCCUUACAAUGCUUCCAGGACA
757

GGGG

UUU

LPA-5581
AGAACAAGGUUUGGAAAGCAC
358
AGAAGUGCUUUCCAAACCUUGUUC
758

UUCT

UGA

LPA-5582
GAACAAGGUUUGGAAAGCAAU
359
CAGAAUUGCUUUCCAAACCUUGUU
759

UCTG

CUG

LPA-5583
AACAAGGUUUGGAAAGCACAU
360
ACAGAUGUGCUUUCCAAACCUUGU
760

CUGT

UCU

LPA-5584
ACAAGGUUUGGAAAGCACUAC
361
CACAGUAGUGCUUUCCAAACCUUG
761

UGTG

UUC

LPA-5585
CAAGGUUUGGAAAGCACUUAU
362
CCACAUAAGUGCUUUCCAAACCUU
762

GUGG

GUU

LPA-5586
AAGGUUUGGAAAGCACUUCAG
363
UCCACUGAAGUGCUUUCCAAACCU
763

UGGA

UGU

LPA-5587
AGGUUUGGAAAGCACUUCUAU
364
CUCCAUAGAAGUGCUUUCCAAACC
764

GGAG

UUG

LPA-5592
UGGAAAGCACUUCUGUGGAAG
365
GGUGCUUCCACAGAAGUGCUUUCC
765

CACC

AAA

LPA-5606
GUGGAGGCACCUUAAUAUCAC
366
UCUGGUGAUAUUAAGGUGCCUCCA
766

CAGA

CAG

LPA-5616
CUUAAUAUCCCCAGAGUGGAU
367
CAGCAUCCACUCUGGGGAUAUUAA
767

GCTG

GGU

LPA-5618
UAAUAUCCCCAGAGUGGGUAC
368
GUCAGUACCCACUCUGGGGAUAUU
768

UGAC

AAG

LPA-5628
AGAGUGGGUGCUGACUGCUAC
369
GUGAGUAGCAGUCAGCACCCACUC
769

UCAC

UGG

LPA-5685
CAAGGUCAUCCUGGGUGCAAA
370
UUGGUUUGCACCCAGGAUGACCUU
770

CCAA

GUA

LPA-5694
CCUGGGUGCACACCAAGAAAU
371
GUUCAUUUCUUGGUGUGCACCCAG
771

GAAC

GAU

LPA-5699
GUGCACACCAAGAAGUGAAAC
372
UCGAGUUUCACUUCUUGGUGUGCA
772

UCGA

CCC

LPA-5775
AGCAGAUAUUGCCUUGCUAAA
373
UAGCUUUAGCAAGGCAAUAUCUGC
773

GCTA

UUG

LPA-5776
GCAGAUAUUGCCUUGCUAAAG
374
UUAGCUUUAGCAAGGCAAUAUCUG
774

CUAA

CUU

LPA-5777
CAGAUAUUGCCUUGCUAAAAC
375
CUUAGUUUUAGCAAGGCAAUAUCU
775

UAAG

GCU

LPA-5778
AGAUAUUGCCUUGCUAAAGAU
376
GCUUAUCUUUAGCAAGGCAAUAUC
776

AAGC

UGC

LPA-5779
GAUAUUGCCUUGCUAAAGCAA
377
UGCUUUGCUUUAGCAAGGCAAUAU
777

AGCA

CUG

LPA-5780
AUAUUGCCUUGCUAAAGCUAA
378
CUGCUUAGCUUUAGCAAGGCAAUA
778

GCAG

UCU

LPA-5781
UAUUGCCUUGCUAAAGCUAAG
379
CCUGCUUAGCUUUAGCAAGGCAAU
779

CAGG

AUC

LPA-5813
UCAUCACUGACAAAGUAAUAC
380
GCUGGUAUUACUUUGUCAGUGAUG
780

CAGC

ACG

LPA-5873
GGACUGAAUGUUACAUCACAG
381
CAGCCUGUGAUGUAACAUUCAGUC
781

GCTG

CUG

LPA-5874
GACUGAAUGUUACAUCACUAG
382
CCAGCUAGUGAUGUAACAUUCAGU
782

CUGG

CCU

LPA-5875
ACUGAAUGUUACAUCACUGAC
383
CCCAGUCAGUGAUGUAACAUUCAG
783

UGGG

UCC

LPA-5876
CUGAAUGUUACAUCACUGGAU
384
CCCCAUCCAGUGAUGUAACAUUCA
784

GGGG

GUC

LPA-5877
UGAAUGUUACAUCACUGGCAG
385
UCCCCUGCCAGUGAUGUAACAUUC
785

GGGA

AGU

LPA-5879
AAUGUUACAUCACUGGCUGAG
386
UCUCCUCAGCCAGUGAUGUAACAU
786

GAGA

UCA

LPA-5902
GAAACCCAAGGUACCUUUGAG
387
CAGUCUCAAAGGUACCUUGGGUUU
787

ACTG

CUC

LPA-0190-M1
UCCACCACUGUCACAGGAAAG
388
UUUCCUGUGACAGUGGUGGAGG
788

CAGCCGAAAGGCUGC

LPA-0501-M1
UGGUAAUGGACAGAGUUAUAG
389
UAUAACUCUGUCCAUUACCAGG
789

CAGCCGAAAGGCUGC

LPA-3100-M1
UACUGCAACCUGACACGAUAG
390
UAUCGUGUCAGGUUGCAGUAGG
790

CAGCCGAAAGGCUGC

LPA-3286-M1
AGAACUUGCCAAGCUUGGUAG
391
UACCAAGCUUGGCAAGUUCUGG
791

CAGCCGAAAGGCUGC

LPA-3288-M1
AACUUGCCAAGCUUGGUCAAG
392
UUGACCAAGCUUGGCAAGUUGG
792

CAGCCGAAAGGCUGC

LPA-3291-M1
UUGCCAAGCUUGGUCAUCUAG
393
UAGAUGACCAAGCUUGGCAAGG
793

CAGCCGAAAGGCUGC

LPA-3584-M1
AUGGACAGAGUUAUCGAGGAG
394
UCCUCGAUAACUCUGUCCAUGG
794

CAGCCGAAAGGCUGC

LPA-3585-M1
UGGACAGAGUUAUCGAGGCAG
395
UGCCUCGAUAACUCUGUCCAGG
795

CAGCCGAAAGGCUGC

LPA-4645-M1
UGGUCAUCUAUGAUACCACAG
396
UGUGGUAUCAUAGAUGACCAGG
796

CAGCCGAAAGGCUGC

LPA-4717-M1
UACUGCAGGAAUCCAGAUUAG
397
UAAUCUGGAUUCCUGCAGUAGG
797

CAGCCGAAAGGCUGC

LPA-5510-M1
AGAAAUGUCCUGGAAGCAUAG
398
UAUGCUUCCAGGACAUUUCUGG
798

CAGCCGAAAGGCUGC

LPA-3750-M1
GACAACAGAAUAUUAUCCAAG
399
UUGGAUAAUAUUCUGUUGUCGG
799

CAGCCGAAAGGCUGC

LPA-2900-M2
AUGGACAGAGUUAUCAAGGAG
400
UCCUUGAUAACUCUGUCCAUGG
800

CAGCCGAAAGGCUGC

LPA-3675-M2
GACAACAGAAUAUUAUCCAAG
401
UUGGAUAAUAUUCUGUUGUCGG
801

CAGCCGAAAGGCUGC

LPA-2900-M3
AUGGACAGAGUUAUCAAGGAG
402
UCCUUGAUAACUCUGUCCAUGG
802

CAGCCGAAAGGCUGC

LPA-3675-M3
GACAACAGAAUAUUAUCCAAG
403
UUGGAUAAUAUUCUGUUGUCGG
803

CAGCCGAAAGGCUGC

Human (Hs): NM_005577.3 (SEQ ID NO: 1)

CTGGGATTGG GACACACTTT CTGGGCACTG CTGGCCAGTC CCAAAATGGA ACATAAGGAA

GTGGTTCTTC TACTTCTTTT ATTTCTGAAA TCAGCAGCAC CTGAGCAAAG CCATGTGGTC

CAGGATTGCT ACCATGGTGA TGGACAGAGT TATCGAGGCA CGTACTCCAC CACTGTCACA

GGAAGGACCT GCCAAGCTTG GTCATCTATG ACACCACATC AACATAATAG GACCACAGAA

AACTACCCAA ATGCTGGCTT GATCATGAAC TACTGCAGGA ATCCAGATGC TGTGGCAGCT

CCTTATTGTT ATACGAGGGA TCCCGGTGTC AGGTGGGAGT ACTGCAACCT GACGCAATGC

TCAGACGCAG AAGGGACTGC CGTCGCGCCT CCGACTGTTA CCCCGGTTCC AAGCCTAGAG

GCTCCTTCCG AACAAGCACC GACTGAGCAA AGGCCTGGGG TGCAGGAGTG CTACCATGGT

AATGGACAGA GTTATCGAGG CACATACTCC ACCACTGTCA CAGGAAGAAC CTGCCAAGCT

TGGTCATCTA TGACACCACA CTCGCATAGT CGGACCCCAG AATACTACCC AAATGCTGGC

TTGATCATGA ACTACTGCAG GAATCCAGAT GCTGTGGCAG CTCCTTATTG TTATACGAGG

GATCCCGGTG TCAGGTGGGA GTACTGCAAC CTGACGCAAT GCTCAGACGC AGAAGGGACT

GCCGTCGCGC CTCCGACTGT TACCCCGGTT CCAAGCCTAG AGGCTCCTTC CGAACAAGCA

CCGACTGAGC AAAGGCCTGG GGTGCAGGAG TGCTACCATG GTAATGGACA GAGTTATCGA

GGCACATACT CCACCACTGT CACAGGAAGA ACCTGCCAAG CTTGGTCATC TATGACACCA

CACTCGCATA GTCGGACCCC AGAATACTAC CCAAATGCTG GCTTGATCAT GAACTACTGC

AGGAATCCAG ATGCTGTGGC AGCTCCTTAT TGTTATACGA GGGATCCCGG TGTCAGGTGG

GAGTACTGCA ACCTGACGCA ATGCTCAGAC GCAGAAGGGA CTGCCGTCGC GCCTCCGACT

GTTACCCCGG TTCCAAGCCT AGAGGCTCCT TCCGAACAAG CACCGACTGA GCAGAGGCCT

GGGGTGCAGG AGTGCTACCA CGGTAATGGA CAGAGTTATC GAGGCACATA CTCCACCACT

GTCACTGGAA GAACCTGCCA AGCTTGGTCA TCTATGACAC CACACTCGCA TAGTCGGACC

CCAGAATACT ACCCAAATGC TGGCTTGATC ATGAACTACT GCAGGAATCC AGATGCTGTG

GCAGCTCCTT ATTGTTATAC GAGGGATCCC GGTGTCAGGT GGGAGTACTG CAACCTGACG

CAATGCTCAG ACGCAGAAGG GACTGCCGTC GCGCCTCCGA CTGTTACCCC GGTTCCAAGC

CTAGAGGCTC CTTCCGAACA AGCACCGACT GAGCAAAGGC CTGGGGTGCA GGAGTGCTAC

CATGGTAATG GACAGAGTTA TCGAGGCACA TACTCCACCA CTGTCACAGG AAGAACCTGC

CAAGCTTGGT CATCTATGAC ACCACACTCG CATAGTCGGA CCCCAGAATA CTACCCAAAT

GCTGGCTTGA TCATGAACTA CTGCAGGAAT CCAGATGCTG TGGCAGCTCC TTATTGTTAT

ACGAGGGATC CCGGTGTCAG GTGGGAGTAC TGCAACCTGA CGCAATGCTC AGACGCAGAA

GGGACTGCCG TCGCGCCTCC GACTGTTACC CCGGTTCCAA GCCTAGAGGC TCCTTCCGAA

CAAGCACCGA CTGAGCAAAG GCCTGGGGTG CAGGAGTGCT ACCATGGTAA TGGACAGAGT

TATCGAGGCA CATACTCCAC CACTGTCACA GGAAGAACCT GCCAAGCTTG GTCATCTATG

ACACCACACT CGCATAGTCG GACCCCAGAA TACTACCCAA ATGCTGGCTT GATCATGAAC

TACTGCAGGA ATCCAGATGC TGTGGCAGCT CCTTATTGTT ATACGAGGGA TCCCGGTGTC

AGGTGGGAGT ACTGCAACCT GACGCAATGC TCAGACGCAG AAGGGACTGC CGTCGCGCCT

CCGACTGTTA CCCCGGTTCC AAGCCTAGAG GCTCCTTCCG AACAAGCACC GACTGAGCAA

AGGCCTGGGG TGCAGGAGTG CTACCATGGT AATGGACAGA GTTATCGAGG CACATACTCC

ACCACTGTCA CAGGAAGAAC CTGCCAAGCT TGGTCATCTA TGACACCACA CTCGCATAGT

CGGACCCCAG AATACTACCC AAATGCTGGC TTGATCATGA ACTACTGCAG GAATCCAGAT

GCTGTGGCAG CTCCTTATTG TTATACGAGG GATCCCGGTG TCAGGTGGGA GTACTGCAAC

CTGACGCAAT GCTCAGACGC AGAAGGGACT GCCGTCGCGC CTCCGACTGT TACCCCGGTT

CCAAGCCTAG AGGCTCCTTC CGAACAAGCA CCGACTGAGC AGAGGCCTGG GGTGCAGGAG

TGCTACCACG GTAATGGACA GAGTTATCGA GGCACATACT CCACCACTGT CACTGGAAGA

ACCTGCCAAG CTTGGTCATC TATGACACCA CACTCGCATA GTCGGACCCC AGAATACTAC

CCAAATGCTG GCTTGATCAT GAACTACTGC AGGAATCCAG ATCCTGTGGC AGCCCCTTAT

TGTTATACGA GGGATCCCAG TGTCAGGTGG GAGTACTGCA ACCTGACACA ATGCTCAGAC

GCAGAAGGGA CTGCCGTCGC GCCTCCAACT ATTACCCCGA TTCCAAGCCT AGAGGCTCCT

TCTGAACAAG CACCAACTGA GCAAAGGCCT GGGGTGCAGG AGTGCTACCA CGGAAATGGA

CAGAGTTATC AAGGCACATA CTTCATTACT GTCACAGGAA GAACCTGCCA AGCTTGGTCA

TCTATGACAC CACACTCGCA TAGTCGGACC CCAGCATACT ACCCAAATGC TGGCTTGATC

AAGAACTACT GCCGAAATCC AGATCCTGTG GCAGCCCCTT GGTGTTATAC AACAGATCCC

AGTGTCAGGT GGGAGTACTG CAACCTGACA CGATGCTCAG ATGCAGAATG GACTGCCTTC

GTCCCTCCGA ATGTTATTCT GGCTCCAAGC CTAGAGGCTT TTTTTGAACA AGCACTGACT

GAGGAAACCC CCGGGGTACA GGACTGCTAC TACCATTATG GACAGAGTTA CCGAGGCACA

TACTCCACCA CTGTCACAGG AAGAACTTGC CAAGCTTGGT CATCTATGAC ACCACACCAG

CATAGTCGGA CCCCAGAAAA CTACCCAAAT GCTGGCCTGA CCAGGAACTA CTGCAGGAAT

CCAGATGCTG AGATTCGCCC TTGGTGTTAC ACCATGGATC CCAGTGTCAG GTGGGAGTAC

TGCAACCTGA CACAATGCCT GGTGACAGAA TCAAGTGTCC TTGCAACTCT CACGGTGGTC

CCAGATCCAA GCACAGAGGC TTCTTCTGAA GAAGCACCAA CGGAGCAAAG CCCCGGGGTC

CAGGATTGCT ACCATGGTGA TGGACAGAGT TATCGAGGCT CATTCTCTAC CACTGTCACA

GGAAGGACAT GTCAGTCTTG GTCCTCTATG ACACCACACT GGCATCAGAG GACAACAGAA

TATTATCCAA ATGGTGGCCT GACCAGGAAC TACTGCAGGA ATCCAGATGC TGAGATTAGT

CCTTGGTGTT ATACCATGGA TCCCAATGTC AGATGGGAGT ACTGCAACCT GACACAATGT

CCAGTGACAG AATCAAGTGT CCTTGCGACG TCCACGGCTG TTTCTGAACA AGCACCAACG

GAGCAAAGCC CCACAGTCCA GGACTGCTAC CATGGTGATG GACAGAGTTA TCGAGGCTCA

TTCTCCACCA CTGTTACAGG AAGGACATGT CAGTCTTGGT CCTCTATGAC ACCACACTGG

CATCAGAGAA CCACAGAATA CTACCCAAAT GGTGGCCTGA CCAGGAACTA CTGCAGGAAT

CCAGATGCTG AGATTCGCCC TTGGTGTTAT ACCATGGATC CCAGTGTCAG ATGGGAGTAC

TGCAACCTGA CGCAATGTCC AGTGATGGAA TCAACTCTCC TCACAACTCC CACGGTGGTC

CCAGTTCCAA GCACAGAGCT TCCTTCTGAA GAAGCACCAA CTGAAAACAG CACTGGGGTC

CAGGACTGCT ACCGAGGTGA TGGACAGAGT TATCGAGGCA CACTCTCCAC CACTATCACA

GGAAGAACAT GTCAGTCTTG GTCGTCTATG ACACCACATT GGCATCGGAG GATCCCATTA

TACTATCCAA ATGCTGGCCT GACCAGGAAC TACTGCAGGA ATCCAGATGC TGAGATTCGC

CCTTGGTGTT ACACCATGGA TCCCAGTGTC AGGTGGGAGT ACTGCAACCT GACACGATGT

CCAGTGACAG AATCGAGTGT CCTCACAACT CCCACAGTGG CCCCGGTTCC AAGCACAGAG

GCTCCTTCTG AACAAGCACC ACCTGAGAAA AGCCCTGTGG TCCAGGATTG CTACCATGGT

GATGGACGGA GTTATCGAGG CATATCCTCC ACCACTGTCA CAGGAAGGAC CTGTCAATCT

TGGTCATCTA TGATACCACA CTGGCATCAG AGGACCCCAG AAAACTACCC AAATGCTGGC

CTGACCGAGA ACTACTGCAG GAATCCAGAT TCTGGGAAAC AACCCTGGTG TTACACAACC

GATCCGTGTG TGAGGTGGGA GTACTGCAAT CTGACACAAT GCTCAGAAAC AGAATCAGGT

GTCCTAGAGA CTCCCACTGT TGTTCCAGTT CCAAGCATGG AGGCTCATTC TGAAGCAGCA

CCAACTGAGC AAACCCCTGT GGTCCGGCAG TGCTACCATG GTAATGGCCA GAGTTATCGA

GGCACATTCT CCACCACTGT CACAGGAAGG ACATGTCAAT CTTGGTCATC CATGACACCA

CACCGGCATC AGAGGACCCC AGAAAACTAC CCAAATGATG GCCTGACAAT GAACTACTGC

AGGAATCCAG ATGCCGATAC AGGCCCTTGG TGTTTTACCA TGGACCCCAG CATCAGGTGG

GAGTACTGCA ACCTGACGCG ATGCTCAGAC ACAGAAGGGA CTGTGGTCGC TCCTCCGACT

GTCATCCAGG TTCCAAGCCT AGGGCCTCCT TCTGAACAAG ACTGTATGTT TGGGAATGGG

AAAGGATACC GGGGCAAGAA GGCAACCACT GTTACTGGGA CGCCATGCCA GGAATGGGCT

GCCCAGGAGC CCCATAGACA CAGCACGTTC ATTCCAGGGA CAAATAAATG GGCAGGTCTG

GAAAAAAATT ACTGCCGTAA CCCTGATGGT GACATCAATG GTCCCTGGTG CTACACAATG

AATCCAAGAA AACTTTTTGA CTACTGTGAT ATCCCTCTCT GTGCATCCTC TTCATTTGAT

TGTGGGAAGC CTCAAGTGGA GCCGAAGAAA TGTCCTGGAA GCATTGTAGG GGGGTGTGTG

GCCCACCCAC ATTCCTGGCC CTGGCAAGTC AGTCTCAGAA CAAGGTTTGG AAAGCACTTC

TGTGGAGGCA CCTTAATATC CCCAGAGTGG GTGCTGACTG CTGCTCACTG CTTGAAGAAG

TCCTCAAGGC CTTCATCCTA CAAGGTCATC CTGGGTGCAC ACCAAGAAGT GAACCTCGAA

TCTCATGTTC AGGAAATAGA AGTGTCTAGG CTGTTCTTGG AGCCCACACA AGCAGATATT

GCCTTGCTAA AGCTAAGCAG GCCTGCCGTC ATCACTGACA AAGTAATGCC AGCTTGTCTG

CCATCCCCAG ACTACATGGT CACCGCCAGG ACTGAATGTT ACATCACTGG CTGGGGAGAA

ACCCAAGGTA CCTTTGGGAC TGGCCTTCTC AAGGAAGCCC AGCTCCTTGT TATTGAGAAT

GAAGTGTGCA ATCACTATAA GTATATTTGT GCTGAGCATT TGGCCAGAGG CACTGACAGT

TGCCAGGGTG ACAGTGGAGG GCCTCTGGTT TGCTTCGAGA AGGACAAATA CATTTTACAA

GGAGTCACTT CTTGGGGTCT TGGCTGTGCA CGCCCCAATA AGCCTGGTGT CTATGCTCGT

GTTTCAAGGT TTGTTACTTG GATTGAGGGA ATGATGAGAA ATAATTAATT GGACGGGAGA

CAGAGTGAAG CATCAACCTA CTTAGAAGCT GAAACGTGGG TAAGGATTTA GCATGCTGGA

AATAATAGAC AGCAATCAAA CGAAGACACT GTTCCCAGCT ACCAGCTATG CCAAACCTTG

GCATTTTTGG TATTTTTGTG TATAAGCTTT TAAGGTCTGA CTGACAAATT CTGTATTAAG

GTGTCATAGC TATGACATTT GTTAAAAATA AACTCTGCAC TTATTTTGAT TTGA

Cynomolgus monkey (Mf): XM_015448517. 1 (SEQ ID NO: 2)

GATGCTGCAT ACTTAATGTC GAAAGGTTGC TTCATCCAAG AGCCTGGAGT TTTCAGAGAC

ACTGTCCTGA AACTATGTCC TGAAACTATG TCATTGAAAC TGAAACATTG TCCTGAAGCT

GGTATTGGGC AATACCAGCG CCTGCAGGCA ACAGCTCGGA TGCACTTAAG ATTTAAATAT

TACCCACAGA AGTTCTGGCT TGTCTGGGAA AACCTTTTGC TAAACAGAAG AGCAACATTT

TTTTTTTTTT CTTTTCTGGA ATTTGTAAAC AGCATTTATT CTCAGCCTTA CCTTCCAAAC

GTTGCACTTG GAACATTGCT GGGCCCCGTG GAAACAGAAG CGAACGTCAG CCAGGCCGGC

AGGGGGCGGC AGACCCCACA CTTCGCCGGG CGCCCTCACC TCCCTGGGAG GGAGTGTGCA

GCTGCCAAAA TCTTCGGCGG GGTTCAGTCC AAGCGACTTC AGCCAGCAGA TGGTCATTCT

CCTGTGACCG TGTGTACTAC AGACTGTTTC AAAACCGGGC AGGCAATTAA CAATGGGAAT

TCTGCCATCA TCGCTGACAA AGTCATCCCA GTTTGTCTGC CATCCCCAAA TTATGTGGTC

GCCAACCAGA CTGAATGTTA TGTCACTGGC TGGGGAGAAA CCCAAGCACT ACCTGAGCAA

AGCCATGTGG TCCAGGATTG CTACCATGGT GATGGACAGA GTTATCAAGG CACATCCTCC

ACCACTGTCA CAGGAAGGAC CTGCCAAGCT TGGTCATCTA TGGAACCACA TCAGCATAAT

AGAACCACAG AAAACTACCC AAATGCTGGC TTGATCAGGA ACTACTGCAG GAATCCAGAT

CCTGTGGCAG CCCCTTATTG TTATACGATG GATCCCAATG TCAGGTGGGA GTACTGCAAC

CTGACACAAT GCTCAGACGC AGAAGGGACT GCCGTCGCAC CTCCGAATGT CACCCCGGTT

CCAAGCCTAG AGGCTCCTTC CGAACAAGCA CCGACTGAGC AAAGGCCTGG GGTGCAGGAG

TGCTACCACG GTAATGGACA GAGTTATCGA GGCACATACT TCACCACTGT GACAGGAAGA

ACCTGCCAAG CTTGGTCATC TATGACACCG CACTCTCATA GTCGGACCCC GGAAAACTAC

CCAAATGGTG GCTTGATCAG GAACTACTGC AGGAATCCAG ATCCTGTGGC AGCCCCTTAT

TGTTATACCA TGGATCCCAA TGTCAGGTGG GAGTACTGCA ACCTGACACA ATGCTCAGAC

GCAGAAGGGA TTGCCGTCAC ACCTCTGACT GTTACCCCGG TTCCAAGCCT AGAGGCTCCT

TCCAAGCAAG CACCAACTGA GCAAAGGCCT GGTGTCCAGG AGTGCTACCA CGGTAATGGA

CAGAGTTATC GAGGCACATA CTTCACCACT GTGACAGGAA GAACCTGCCA AGCTTGGTCA

TCTATGACAC CACATTCTCA TAGTCGTACC CCAGAAAACT ACCCAAATGG TGGCTTGATC

AGGAACTACT GCAGGAATCC AGATCCTGTG GCAGCCCCTT ATTGTTATAC CATGGATCCC

AATGTCAGGT GGGAGTACTG CAACCTGACA CAATGCTCAG ACGCAGAAGG GACTGCCGTC

GCACCTCCGA CTGTCACCCC GGTTCCAAGC CTAGAGGCTC CTTCCGAACA AGCACCGACT

GAGCAAAGGC CTGGGGTGCA GGAGTGCTAC CACGGTAATG GACAGAGTTA TCGAGGCACA

TACTTCACCA CTGTGACAGG AAGAACCTGC CAAGCTTGGT CATCTATGAC ACCGCACTCT

CATAGTCGGA CCCCGGAAAA CTACCCAAAT GGTGGCTTGA TCAGGAACTA CTGCAGGAAT

CCAGATCCTG TGGCAGCCCC TTATTGTTAT ACCATGGATC CCAATGTCAG GTGGGAGTAC

TGCAACCTGA CACAATGCTC AGACGCAGAA GGGACTGCCG TCGCACCTCC GAATGTCACC

CCGGTTCCAA GCCTAGAGGC TCCTTCTGAG CAAGCACCAA CTGAGCAAAG GCTTGGGGTG

CAGGAGTGCT ACCACGGTAA TGGACAGAGT TATCGAGGCA CATACTTCAC CACTGTGACA

GGAAGAACCT GCCAAGCTTG GTCATCTATG ACACCACACT CTCATAGTCG GACCCCAGAA

AACTACCCAA ATGCTGGCTT GGTCAAGAAC TACTGCCGAA ATCCAGATCC TGTGGCAGCC

CCTTGGTGTT ATACAACGGA TCCCAGTGTC AGGTGGGAGT ACTGCAACCT GACACGATGC

TCAGATGCAG AAGGGACTGC TGTTGTGCCT CCAAATATTA TTCCGGTTCC AAGCCTAGAG

GCTTTTCTTG AACAAGAACC GACTGAGGAA ACCCCCGGGG TACAGGAGTG CTACTACCAT

TATGGACAGA GTTATAGAGG CACATACTCC ACCACTGTTA CAGGAAGAAC TTGCCAAGCT

TGGTCATCTA TGACACCACA CCAGCATAGT CGGACCCCAA AAAACTATCC AAATGCTGGC

CTGACCAGGA ACTACTGCAG GAATCCAGAT GCTGAGATTC GCCCTTGGTG TTATACCATG

GATCCCAGTG TCAGGTGGGA GTACTGCAAC CTGACACAAT GTCTGGTGAC AGAATCAAGT

GTCCTTGAAA CTCTCACAGT GGTCCCAGAT CCAAGCACAC AGGCTTCTTC TGAAGAAGCA

CCAACGGAGC AAAGTCCCGA GGTCCAGGAC TGCTACCATG GTGATGGACA GAGTTATCGA

GGCTCATTCT CCACCACTGT CACAGGAAGG ACATGTCAGT CTTGGTCCTC TATGACACCA

CACTGGCATC AGAGGACAAC AGAATATTAT CCAGATGGTG GCCTGACCAG GAACTACTGC

AGGAATCCAG ATGCTGAGAT TCGCCCTTGG TGTTATACCA TGGATCCCAG TGTCAGGTGG

GAGTACTGCA ACCTGACACA ATGTCCAGTG ACAGAATCAA GTGTCCTCGC AACGTCCATG

GCTGTTTCTG AACAAGCACC AATGGAGCAA AGCCCCGGGG TCCAGGACTG CTACCATGGT

GATGGACAGA GTTATCGAGG TTCATTCTCC ACCACTGTCA CAGGAAGGAC ATGTCAGTCT

TGGTCCTCTA TGACACCACA CTGGCATCAG AGGACCATAG AATACTACCC AAATGGTGGC

CTGACCAAGA ACTACTGCAG GAATCCAGAT GCTGAGATTC GCCCTTGGTG TTATACCATG

GATCCCAGAG TCAGATGGGA GTACTGCAAC CTGACACAAT GTGTGGTGAT GGAATCAAGT

GTCCTTGCAA CTCCCATGGT GGTCCCAGTT CCAAGCAGAG AGGTTCCTTC TGAAGAAGCA

CCAACTGAAA ACAGCCCTGG GGTCCAGGAC TGCTACCAAG GTGATGGACA GAGTTATCGA

GGCACATTCT CCACCACTAT CACAGGAAGA ACATGTCAGT CTTGGTTGTC TATGACACCA

CATCGGCATC GGAGGATCCC ATTACGCTAT CCAAATGCTG GCCTGACCAG GAACTATTGC

AGAAATCCAG ATGCTGAGAT TCGCCCTTGG TGTTACACCA TGGATCCCAG TGTCAGGTGG

GAGTACTGCA ACCTGACACA ATGTCCAGTG ACAGAATCAA GTGTCCTCAC AACTCCCACG

GTGGTCCCGG TTCCAAGCAC AGAGGCTCCT TCTGAACAAG CACCACCTGA GAAAAGCCCT

GTGGTCCAGG ATTGCTACCA TGGTGATGGA CAGAGTTATC GAGGCACATC CTCCACCACT

GTCACAGGAA GGAACTGTCA GTCTTGGTCA TCTATGATAC CACACTGGCA TCAGAGGACC

CCAGAAAACT ACCCAAATGC TGGCCTGACC AGGAACTACT GCAGGAATCC AGATTCTGGG

AAACAACCCT GGTGTTACAC GACTGATCCA TGTGTGAGGT GGGAGTACTG CAACCTGACA

CAATGCTCAG AAACAGAATC AGGTGTCCTA GAGACTCCCA CTGTTGTTCC GGTTCCAAGC

ATGGAAGCTC ATTCTGAAGC AGCACCAACT GAGCAAACTC CTGTGGTCCA GCAGTGCTAC

CATGGTAATG GACAGAGTTA TCGAGGCACA TTCTCCACCA CTGTCACAGG AAGGACATGT

CAATCTTGGT CATCCATGAC ACCACACCAG CATAAGAGGA CCCCGGAAAA CCACCCAAAT

GATGACTTGA CAATGAACTA CTGCAGGAAT CCAGATGCTG ACACAGGCCC TTGGTGTTTT

ACCATGGACC CCAGCGTCAG GCGGGAGTAC TGCAACCTGA CGCGATGCTC AGACACAGAA

GGGACTGTGG TCACACCTCC GACTGTTATC CCGGTTCCAA GCCTAGAGGC TCCTTCTGAA

CAAGCATCCT CTTCATTTGA TTGTGGGAAG CCTCAAGTGG AGCCAAAGAA ATGTCCTGGA

AGCATTGTAG GTGGGTGTGT GGCCCACCCA CATTCCTGGC CCTGGCAAGT CAGTCTTAGA

ACAAGGTTTG GAAAGCACTT CTGTGGAGGC ACCTTAATAT CCCCAGAGTG GGTGCTGACT

GCTGCTTGCT GCTTGGAGAC GTTCTCAAGG CCTTCCTTCT ACAAGGTCAT CCTGGGTGCA

CACCAAGAAG TGAATCTCGA ATCTCACGTT CAAGAAATAG AAGTGTCTAG GTTGTTCTTG

GAGCCCATAG GAGCAGATAT TGCCTTGCTA AAGCTAAGCA GGCCTGCCAT CATCACTGAC

AAAGTAATCC CAGCCTGTCT GCCGTCTCCA AATTACGTGA TCACCGTCTG GACTGAATGT

TACATCACTG GCTGGGGAGA AACCCAAGGT ACCTTTGGGG CTGGCCTTCT CAAGGAAGCC

CAGCTTCATG TGATTGAGAA TACAGTGTGC AATCACTACG AGTTTCTGAA TGGAAGAGTC

AAATCCACCG AGCTCTGTGC TGGGCATTTG GCCGGAGGCA CTGACAGATG CCAGGGTGAC

AGTGGAGGGC CTGTGGTTTG CTTCGACAAG GACAAATACA TTTTACGAGG AATAACTTCT

TGGGGTCCTG GCTGTGCATG CCCCAATAAG CCTGGTGTCT ATGTTCGTGT TTCAAGCTTT

GTCACTTGGA TTGAGGGAGT GATGAGAAAT AATTAATTGA ACAAGAGACA GAGTGAAGCA

TTGACTCACC TAGAGGCTAG AATGGGGGTA GGGATTTAGC ACGCTGGAAA TAACGGACAG

TAATCAAACG AAGACACTGT CCCCAGCTAC CAACTATGCC AAACCTCAGC ATTTTTGGTA

TTATTGTGTA TAAGCTTTTC CCGTCTGACT GCTGGGTTCT CCAATAAGGT GACATAGCTA

TGCCATTTGT TAAAAATAAA CTCTGTACTT ATTTTGATTT GAGTAAA

Rhesus monkey: XM_028847001.1 (SEQ ID NO: 3)

AGCCTTGCCT TTGAAATGTT CCAGTTGGAA CATTGCTGGG CAGCGTGCAA ACAGGAGCGA

ACGTCAGCCG GGGCGGCAGG GGGCAGCAGA CCCCACACTT TGTCCATGCC TCAGGTGGGA

GGAAGTGTCC GGCTCCAGAA ACCTGCCGCG GGCTTTATCC CAAGCGACTT CAGCCAGCAG

ACGGTTCATG TCCTGAGGCT GCAAAATACG AGTTCTGCCA TCATCGCTGA CAAAGTCATC

CCAGTTTGTC TGCCATCCCC AAATTATGCG ATCGCCAACC AGACTGAATG TTATGTCACT

GGCTGGGGAG AAACCCAAGC ACTACCTGAG CAAAGCCATG TGGTCCAGGA TTGCTACCAT

GGTGATGGAC AGAGTTATCA AGGCACATCC TCCACCACTG TCACAGGAAG GACCTGCCAA

GCTTGGTCAT CTATGGAACC ACATCAGCAT AATAGAACCA CAGAAAACTA CCCAAATGCT

GGCTTGATCA GGAACTACTG CAGGAATCCA GATCCTGTGG CAGCCCCTTA TTGTTATACG

ATGGATCCCA ATGTCAGGTG GGAGTACTGC AACCTGACAC AATGCTCAGA CGCAGAAGGG

ACTGCCGTCG CACCTCCGAA TGTCACCCCG GTTCCAAGCC TAGAGGCTCT TTCCGAACAA

GCACCGACTG AGCAAAGGCC TGGGGTGCAG GAGTGCTACC ACGGTAATGG ACAGAGTTAT

CGAGGCACAT ACTTCACCAC TGTGACAGGA AGAACCTGCC AAGCTTGGTC ATCTATGACA

CCACATTCTC ATAGTCGTAC CCCAGAAAAC TACCCAAATG GTGGCTTGAT CAGGAACTAC

TGCAGGAATC CAGATCCTGT GGCAGCCCCT TATTGTTATA CCATGGATCC CAATGTCAGG

TGGGAGTACT GCAACCTGAC ACAATGCTCA GACGCAGAAG GGACTGCCGT CGCACCTCCG

AATGTCACCC CGGTTCCAAG CCTAGAGGCT CCTTCCGAAC AAGCACCGAC TGAGCAAAGG

CCTGGGGTGC AGGAGTGCTA CCACGGTAAT GGACAGAGTT ATCGAGGCAC ATACTTCACC

ACTGTGACAG GAAGAACCTG CCAAGCTTGG TCATCTATGA CACCACATTC TCATAGTCGT

ACCCCAGAAA ACTACCCAAA TGGTGGCTTG ATCAGGAACT ACTGCAGGAA TCCAGATCCT

GTGGCAGCCC CTTATTGTTA TACCATGGAT CCCAATGTCA GGTGGGAGTA CTGCAACCTG

ACACAATGCT CAGACGCAGA GGGGACTGCC GTCGCACCTC CGACTGTCAC CCCGGTTCCA

AGCCTAGAGG CTCCTTCTGA GCAAGCACCG ACTGAGCAAA GGCCTGGGGT GCAGGAGTGC

TACCACGGTA ATGGACAGAG TTATCGAGGC ACATACTTCA CCACTGTGAC AGGAAGAACC

TGCCAAGCTT GGTCATCTAT GACACCGCAC TCTCATAGTC GGACCCCGGA AAACTACCCA

AATGGTGGCT TGATCAGGAA CTACTGCAGG AATCCAGATC CTGTGGCAGC CCCTTATTGT

TATACGATGG ATCCCAATGT CAGGTGGGAG TACTGCAACC TGACACAATG CTCAGACGCA

GAAGGGACTG CCGTCGCACC TCCGAATGTC ACCCCGGTTC CAAGCCTAGA GGCTCCTTCC

GAACAAGCAC CGACTGAGCA AAGGCCTGGG GTGCAGGAGT GCTACCACGG TAATGGACAG

AGTTATCGAG GCACATACTT CACCACTGTG ACAGGAAGAA CCTGCCAAGC TTGGTCATCT

ATGACACCGC ACTCTCATAG TCGGACCCCG GAAAACTACC CAAATGGTGG CTTGATCAGG

AACTACTGCA GGAATCCAGA TCCTGTGGCA GCCCCTTATT GTTATACGAT GGATCCCAAT

GTCAGGTGGG AGTACTGCAA CCTGACACAA TGCTCAGACG CAGAAGGGAC TGCCGTCGCA

CCTCCGAATG TCACCCCGGT TCCAAGCCTA GAGGCTCCTT CCGAACAAGC ACCAACTGAG

CAAAGGCCTG GGNTGCAGGA GTGCTACCAT GGTAATGGAC AGAGTTATCG AGGCACATAC

TTCACCACTG TGACAGGAAG AACCTGCCAA GCTTGGTCAT CTATGACACC GCACTCTCAT

AGTCGGACCC CGGAAAACTA CCCAAATGGT GGCTTGATCA GGAACTACTG CAGGAATCCA

GATCCTGTGG CAGCCCCTTA TTGTTATACC ATGGATCCCA ATGTCAGGTG GNAGTACTGC

AACCTGACAC AATGCTCAGA CGCAGAAGGG ACTGCCGTCG CACCTCCGAC TGTCACCCCG

GTTCCAAGCC TAGAGGCTCC TTCGAGCAAG GCACCGACTG AGCAAAGGCC TGGGNTGCAG

GAGTGCTACC ACGGTAATGG ACAGAGTTAT CGAGGCACAT ACTTCACCAC TGTGACAGGA

AGAACCTGCC AAGCTTGGTC ATCTATGACA CCGCACTCTC ATAGTCGGAC CCCGGAAAAC

TACCCAAATG GTGGCTTGAT CAGGAACTAC TGCAGGAATC CAGATCCTGT GGCAGCCCCT

TATTGTTATA CGATGGATCC CAATGTCAGG TGGGAGTACT GCAACCTGAC ACAATGCTCA

GACGCAGAAG GGACTGCCGT CGCACCTCCG AATGTCACCC CGGTTCCAAG CCTAGAGGCT

CCTTCCGAAC AAGCACCGAC TGAGCAAAGG CCTGGGGTGC AGGAGTGCTA CCACGGTAAT

GGACAGAGTT ATCGAGGCAC ATACTTCACC ACTGTGACAG GAAGAACCTG CCAAGCTTGG

TCATCTATGA CACCGCACTC TCATAGTCGG ACCCCGGAAA ACTACCCAAA TGGTGGCTTG

ATCAGGAACT ACTGCAGGAA TCCAGATCCT GTGGCAGCCC CTTATTGTTA TACCATGGAT

CCCAATGTCA GGTGGGAGTA CTGCAACCTG ACACAATGCT CAGACGCAGA AGGGACTGCC

GTCGCACCTC CGAATGTCAC CCCGGTTCCA AGCCTAGAGG CTCCTTCTGA GCAAGCACCA

ACTGAGCAAA GGCTTGGGGT GCAGGAGTGC TACCACAGTA ATGGACAGAG TTATCGAGGC

ACATACTTCA CCACTGTGAC AGGAAGAACC TGCCAAGCTT GGTCATCTAT GACACCACAC

TCTCATAGTC GGACCCCAGA AAACTACCCA AATGCTGGCT TGGTCAAGAA CTACTGCCGA

AATCCAGATC CTGTGGCAGC CCCTTGGTGT TATACAACGG ATCCCAGTGT CAGGTGGGAG

TACTGCAACC TGACACGATG CTCAGATGCA GAAGGGACTG CTGTCATGCC TCCAAATATT

ATTCCGGTTC CAAGCCTAGA GGCTTTTCTT GAACAAGAAC CTACTGAGGA AACCCCCGGG

GTACAGGAGT GCTACTACCA TTATGGACAG AGTTATCGAG GCACATACTC CACCACTGTT

ACAGGAAGAA CTTGCCAAGC TTGGTCATCT ATGACACCAC ACCAGCATAG TCGGACCCCA

AAAAACTATC CAAATGCTGG CCTGACCAGG AACTACTGCA GGAATCCAGA TGCTGAGATT

CGCCCTTGGT GTTATACCAT GGATCCCAGT GTCAGGTGGG AGTACTGCAA CCTGACACAA

TGTCTGGTGA CAGAATCAAG TGTCCTTGAA ACTCTCACAG TGGTCCCAGA TCCAAGCACA

CAGGCTTCTT CTGAAGAAGC ACCAACGGAG CAAAGTCCCG AGGTCCAGGA CTGCTACCAT

GGTGATGGAC AGAGTTATCG AGGCTCATTC TCCACCACTG TCACAGGAAG GACATGTCAG

TCTTGGTCCT CTATGACACC ACACTGGCAT CAGAGGACAA CAGAATATTA TCCAGATGGT

GGCCTGACCA GGAACTACTG CAGGAATCCA GATGCTGAGA TTCGCCCTTG GTGTTATACC

ATGGATCCCA GTGTCAGGTG GGAGTACTGC AACCTGACAC AATGTCCAGT GACAGAATCA

AGTGTCCTCG CAACGTCCAT GGCTGTTTCT GAACAAGCAC CAATGGAGCA AAGCCCCGGG

GTCCAGGACT GCTACCATGG TGATGGACAG AGTTATCGAG GTTCATTCTC CACCACTGTC

ACAGGAAGGA CATGTCAGTC TTGGTCCTCT ATGACACCAC ACTGGCATCA GAGGACCATA

GAATACTACC CAAATGGTGG CCTGACCAAG AACTACTGCA GGAATCCAGA TGCTGAGATT

CGCCCTTGGT GTTATACCAT GGATCCCAGA GTCAGATGGG AGTACTGCAA CCTGACACAA

TGTGTGGTGA TGGAATCAAG TGTCCTTGCA ACTCCCATGG TGGTCCCAGT TCCAAGCAGA

GAGGTTCCTT CTGAAGAAGC ACCAACTGAA AACAGCCCTG GGGTCCAGGA CTGCTACCAA

GGTGATGGAC AGAGTTATCG AGGCACATTC TCCACCACTA TCACAGGAAG AACATGTCAG

TCTTGGTTGT CTATGACACC ACATCGGCAT CGGAGGATCC CATTACGCTA TCCAAATGCT

GGCCTGACCA GGAACTATTG CAGAAATCCA GATGCTGAGA TTCGCCCTTG GTGTTACACC

ATGGATCCCA GTGTCAGGTG GGAGTACTGC AACCTGACAC AATGTCCAGT GACAGAATCA

AGTGTCCTCA CAACTCCCAC GGTGGTCCCG GTTCCAAGCA CAGAGGCTCC TTCTGAACAA

GCACCACCTG AGAAAAGCCC TGTGGTCCAG GATTGCTACC ATGGTGATGG ACAGAGTTAT

CGAGGCACAT CCTCCACCAC TGTCACAGGA AGGAACTGTC AATCTTGGTC ATCTATGATA

CCACACTGGC ATCAGAGGAC CCCAGAAAAC TACCCAAATG CTGGCCTGAC CAGGAACTAC

TGCAGGAATC CAGATTCTGG GAAACAACCC TGGTGTTACA CGACTGATCC ATGTGTGAGG

TGGGAGTACT GCAACCTGAC ACAATGCTCA GAAACAGAAT CAGGTGTCCT AGAGACTCCC

ACTGTTGTTC CGGTTCCAAG CATGGAAGCT CATTCTGAAG CAGCACCAAC TGAGCAAACC

CCTGTGGTCC AGCAGTGCTA CCATGGTAAT GGACAGAGTT ATCGAGGCAC ATTCTCCACC

ACTGTCACAG GAAGGACATG TCAATCTTGG TCATCCATGA CACCACACCA GCATAAGAGG

ACCCCGGAAA ACCACCCAAA TGATGACTTG ACAATGAACT ACTGCAGGAA TCCAGATGCT

GACACAGGCC CTTGGTGTTT TACCATGGAC CCCAGCGTCA GGCGGGAGTA CTGCAACCTG

ACGCGATGCT CAGACACAGA AGGGACTGTG GTCACACCTC CGACTGTTAT CCCGGTTCCA

AGCCTAGAGG CTCCTTCTGA ACAAGCATCC TCTTCATTTG ATTGTGGGAA GCCTCAAGTG

GAGCCAAAGA AATGTCCTGG AAGCATTGTA GGTGGGTGTG TGGCCCACCC ACATTCCTGG

CCCTGGCAAG TCAGTCTTAG AACAAGGTTT GGAAAGCACT TCTGTGGAGG CACCTTAATA

TCCCCAGAGT GGGTGCTGAC TGCTGCTTGC TGCTTGGAGA CGTTCTCAAG GCCTTCCTTC

TACAAGGTCA TCCTGGGTGC ACACCAAGAA GTGAATCTCG AATCTCATGT TCAAGAAATA

GAAGTGTCTA GGTTGTTCTT GGAGCCCATA GGAGCAGATA TTGCCTTGCT AAAGCTAAGC

AGGCCTGCCA TCATCACTGA CAAAGTAATC CCAGCCTGTC TGCCGTCTCC AAATTACGTG

ATCACCGCCT GGACTGAATG TTACATCACT GGCTGGGGAG AAACCCAAGG TACCTTTGGG

GCTGGCCTTC TCAAGGAAGC CCAGCTTCAT GTGATTGAGA ATACAGTGTG CAATCACTAC

GAGTTTCTGA ATGGAAGAGT CAAATCCACT GAGCTCTGTG CTGGGCATTT GGCCGGAGGC

ACTGACAGAT GCCAGGGTGA CAATGGAGGG CCTGTGGTTT GCTTCGACAA GGACAAATAC

ATTTTACGAG GAATAACTTC TTGGGGTCCT GGCTGTGCAT GCCCCAATAA GCCTGGTGTC

TATGTTCGTG TTTCAAGCTT TGTCACTTGG ATTGAGGGAG TGATGAGAAA TAATTAATTG

AACAAGAGAC AGAGTGAAGC ATTGACTCAC CTAGAGGCTA GAATGGGGGT AGGGATTTAG

CACGCTGGAA ATAACGGACA GTAATCAAAC GAAGACACTG TCCCCAGCTA CCAACTATGC

CAAACCTCAG CATTTTTGGT ATTATTGTGT ATAAGCTTTT CCTGTCTGAC TGCTGGGTTC

TCCAATAAGG TGACATAGCT ATGCCATTTG TTAAAAATAA ACTCTGTACT TATTTTGATT

TGAGTAAA

TABLE 6

LPA Oligonucleotide Sequences (modified)

SEQ

SEQ

Sequence
ID
Sequence
ID

Oligonucleotide
(Sense Strand)
NO:
(Antisense Strand)
NO:

LPA-0190-M1
[mUs][mC][mC][mA][mC]
388
[Me Phosphonate-4O-
788

[mC][mA][fC][fU][fG]

mUs][fUs][fUs][fC][fC]

[fU][mC][mA][mC][mA]

[mU][fG][mU][mG][fA][mC]

[mG][mG][mA][mA][mA]

[mA][mG][fU][mG][mG][mU]

[mG][mC][mA][mG][mC][mC]

[mG][mG][mAs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC]

[mU][mG][mC]

LPA-0501-M1
[mUs][mG][mG][mU][mA]
389
[Me Phosphonate-4O-
789

[mA][mU][fG][fG][fA]

mUs][fAs][fUs][fA][fA]

[fC][mA][mG][mA][mG][mU]

[mC][fU][mC][mU][fG][mU]

[mU][mA][mU][mA][mG]

[mC][mC][fA][mU][mU][mA]

[mC][mA][mG][mC][mC]

[mC][mC][mAs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC]

[mU][mG][mC]

LPA-3100-M1
[mUs][mA][mC][mU][mG]
390
[Me Phosphonate-4O-
790

[mC][mA][fA][fC][fC]

mUs][fAs][fUs][fC][fG]

[fU][mG][mA][mC][mA][mC]

[mU][fG][mU][mC][fA][mG]

[mG][mA][mU][mA][mG]

[mG][mU][fU][mG][mC][mA]

[mC][mA][mG][mC][mC]

[mG][mU][mAs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-3286-M1
[mAs][mG][mA][mA][mC]
391
[Me Phosphonate-4O-
791

[mU][mU][fG][fC][fC]

mUs][fAs][fCs][fC][fA]

[fA][mA][mG][mC][mU][mU]

[mA][fG][mC][mU][fU][mG]

[mG][mG][mU][mA][mG]

[mG][mC][fA][mA][mG][mU]

[mC][mA][mG][mC][mC]

[mU][mC][mUs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-3288-M1
[mAs][mA][mC][mU][mU]
392
[Me Phosphonate-4O-
792

[mG][mC][fC][fA][fA]

mUs][fUs][fGs][fA][fC]

[fG][mC][mU][mU][mG][mG]

[mC][FA][mA][mG][fC][mU]

[mU][mC][mA][mA][mG]

[mU][mG][fG][mC][mA][mA]

[mC][mA][mG][mC][mC]

[mG][mU][mUs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-3291-M1
[mUs][mU][mG][mC][mC]
393
[Me Phosphonate-4O-
793

[mA][mA][fG][fC][fU]

mUs][fAs][fGs][fA][fU]

[fU][mG][mG][mU][mC][mA]

[mG][fA][mC][mC][fA][mA]

[mU][mC][mU][mA][mG]

[mG][mC][fU][mU][mG][mG]

[mC][mA][mG][mC][mC]

[mC][mA][mAs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-3584-M1
[mAs][mU][mG][mG][mA]
394
[Me Phosphonate-4O-
794

[mC][mA][fG][fA][fG]

mUs][fCs][fCs][fU][fC]

[fU][mU][mA][mU][mC][mG]

[mG][fA][mU][mA][fA][mC]

[mA][mG][mG][mA][mG]

[mU][mC][fU][mG][mU][mC]

[mC][mA][mG][mC][mC]

[mC][mA][mUs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-3585-M1
[mUs][mG][mG][mA][mC]
395
[Me Phosphonate-4O-
795

[mA][mG][fA][fG][fU]

mUs][fGs][fCs][fC][fU]

[fU][mA][mU][mC][mG][mA]

[mC][fG][mA][mU][fA][mA]

[mG][mG][mC][mA][mG]

[mC][mU][fC][mU][mG][mU]

[mC][mA][mG][mC][mC]

[mC][mC][mAs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-4645-M1
[mUs][mG][mG][mU][mC]
396
[Me Phosphonate-4O-
796

[mA][mU][fC][fU][fA]

mUs][fGs][fUs][fG][fG]

[fU][mG][mA][mU][mA][mC]

[mU][fA][mU][mC][fA][mU]

[mC][mA][mC][mA][mG]

[mA][mG][fA][mU][mG][mA]

[mC][mA][mG][mC][mC]

[mC][mC][mAs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-4717-M1
[mUs][mA][mC][mU][mG]
397
[Me Phosphonate-4O-
797

[mC][mA][fG][fG][fA]

mUs][fAs][fAs][fU][fC]

[fA][mU][mC][mC][mA][mG]

[mU][fG][mG][mA][fU][mU]

[mA][mU][mU][mA][mG]

[mC][mC][fU][mG][mC][mA]

[mC][mA][mG][mC][mC]

[mG][mU][mAs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-5510-M1
[mAs][mG][mA][mA][mA]
398
[Me Phosphonate-4O-
798

[mU][mG][fU][fC][fC]

mUs][fAs][fUs][fG][fC]

[fU][mG][mG][mA][mA][mG]

[mU][fU][mC][mC][fA][mG]

[mC][mA][mU][mA][mG]

[mG][mA][fC][mA][mU][mU]

[mC][mA][mG][mC][mC]

[mU][mC][mUs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-3750-M1
[mGs][mA][mC][mA][mA]
399
[Me Phosphonate-4O-
799

[mC][mA][fG][fA][fA]

mUs][fUs][fGs][fG][fA]

[fU][mA][mU][mU][mA][mU]

[mU][fA][mA][mU][fA][mU]

[mC][mC][mA][mA][mG]

[mU][mC][fU][mG][mU][mU]

[mC][mA][mG][mC][mC]

[mG][mU][mCs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-2900-M2
[mAs][mU][mG][mG][mA]
400
[Me Phosphonate-4O-
800

[mC][mA][fG][fA][fG]

mUs][fCs][fC][fU][fU][mG]

[fU][mU][mA][mU][mC][mA]

[fA][mU][mA][fA][mC][mU]

[mA][mG][mG][mA][mG]

[mC][fU][mG][mU][mC][mC]

[mC][mA][mG][mC][mC]

[mA][mUs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-3675-M2
[mGs][mA][mC][mA][mA]
401
[Me Phosphonate-4O-
801

[mC][mA][fG][fA][fA]

mUs][fUs][fG][fG][fA][mU]

[fU][mA][mU][mU][mA][mU]

[fA][mA][mU][fA][mU][mU]

[mC][mC][mA][mA][mG]

[mC][fU][mG][mU][mU][mG]

[mC][mA][mG][mC][mC]

[mU][mCs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-2900-M3
[mAs][mU][mG][mG][mA]
402
[Me Phosphonate-4O-
802

[mC][mA][fG][fA][fG]

mUs][fCs][fC][mU][fU][mG]

[fU][mU][mA][mU][mC][mA]

[fA][mU][mA][fA][mC][mU]

[mA][mG][mG][mA][mG]

[mC][fU][mG][mU][mC][mC]

[mC][mA][mG][mC][mC]

[mA][mUs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

LPA-3675-M3
[mGs][mA][mC][mA][mA]
403
[Me Phosphonate-4O-
803

[mC][mA][fG][fA][fA]

mUs][fUs][fG][mG][fA][mU]

[fU][mA][mU][mU][mA][mU]

[fA][mA][mU][fA][mU][mU]

[mC][mC][mA][mA][mG]

[mC][fU][mG][mU][mU][mG]

[mC][mA][mG][mC][mC]

[mU][mCs][mGs][mG]

[mG][ademA-

GalNAc][ademA-

GalNAc][ademA-

GalNAc][mG][mG][mC][mU]

[mG][mC]

Modifications in Table 6:

mC, mA, mG, mU=2′-OMe ribonucleosides; fA, fC, fG, fU=2′-F ribonucleosides; s=phosphorothioate; MePhosphonate-40-mUs=

embedded image

ademA-GalNAc=GalNAc attached to an adenine nucleotide:

embedded image

	Number	Date	Country
	63074779	Sep 2020	US
	63061676	Aug 2020	US

COMPOSITIONS AND METHODS FOR INHIBITING LPA EXPRESSION

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Abstract

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