The invention and its various embodiments can now be better understood by turning to the following detailed description of the preferred embodiments which are presented as illustrated examples of the invention defined in the claims. It is expressly understood that the invention as defined by the claims may be broader than the illustrated embodiments described below.
Differences in tissue water state have been measured in normal and malignant breast tissues. Broadband diffuse optical spectroscopy (DOS) has been used to acquire 650-1000 nm absorption spectra of normal and tumor breast tissues from 7 patients in vivo. The absolute values of spectral differences between normalized tissue water spectra and pure water spectra were summed and divided by the number of points in sum to form the bound water index (BWI).
In all subjects in the study of the illustrated embodiment, the average BWIs of all line scan points were significantly lower in tumor tissues (1.62±0.27×10−3) than normal tissues (3.06±0.51×10−3, Wilcoxon Ranked Sum Test z=0.003 and power=0.98). These results imply that water in tumors behaves more like free water than the water in normal tissues. The BWI is therefore a functional parameter that distinguishes between malignant and normal tissues in the breast. Although breast tissue is the tissue of study in the illustrated embodiment, it is to be explicitly understood that any human or animal tissue may be subjected to the method and apparatus of the invention.
Bound water also has been measured by MRI groups by measuring diffusion of water in tissues. In diffusion-weighted MRI, the ADC (apparent diffusion coefficient) of water has been shown to be associated with the fraction changes of intracellular and extracellular water. This cellular level water fraction changes observed by diffusion weighted MRI can be compared to the BWI measured by DOS. The actual bound water fraction of tissues is currently unknown and will be figured out.
Methods
Instrumentation
The instrumentation details of a broadband DOS system have been described in literature and hence can be taken as known, e.g. Cerussi et al. JBO 11(4) 044005, 2006; and Bevilacqua et al. Appl. Opt. 39, 6498-6507, 2000. See also the instrument described in patent application Ser. No. 10/191,693, which is incorporated herein by reference. The core characteristic of the broadband DOS system insofar as the illustrated embodiment is concerned is the combination of modulated multi frequency domain (FDPM component) and broadband steady state domain (SS component). For the FDPM part, the lights from 658, 682, 785, 810, 830 and 850 nm laser diodes were amplitude modulated from 50 to 600 MHz sweeping 401 frequencies by combining a DC current and RF modulation current provided by a network analyzer. Such values are exemplary only and many other values can be chosen consistent with the teachings of the present invention. The laser diodes delivered less than 20 mW optical power to the tissue. An avalanche photodiode detector (APD) detected phase and amplitude of the diffused optical signals after the light's propagating through the tissue. The detected phases and amplitudes were compared to those of the source by the network analyzer which worked as a fast electronic heterodyning digitizer. The SS system is composed of a high intensity tungsten-halogen light source and a high resolution spectrometer (B&W Tek 611).
Because bound water calculation algorithm is based on the absolute wavelengths of the spectrum, automatic and stable calibration of the spectrometer is necessary. The SS system enabled acquisition of continuous absorption spectrum even in the water spectrum wavelength range (>935 nm) longer than the wavelengths of the laser diodes.
We employed a conventional handheld probe as described in the paper of Cerussi et al. above to measure breast cancer patients. In the handheld probe, optical fibers for the source of FDPM system, for the source light of SS system and for the detector of SS system are secured. The APD is housed in the handheld probe directly. The distance between sources and detectors of FDPM and SS systems can be changed by moving a plastic attachment on the probe.
To remove artifacts of cable length and source strength variability of FDPM system, a tissue-simulating phantom with known optical property has been used as described in the paper of Cerussi et al. above. For the SS system, an integrating sphere has been used to eliminate wavelength dependent artifact of the system.
Spectral Processing
Reduced scattering coefficient (μs) and absorption coefficient (μa) have been measured and separated by FDPM theory and practice. The details about this theory and practice have been well described in the literatures, e.g. the two papers cited above and Pham et al., Rev. Sci. Instr., 71, 2500, 2000. The volume fraction of major chromophores (ctHHb, ctHbO2, ctH2O and lipid concentration) have been calculated as described in Cerussi et al. above, but there were a few differences in the employed molar extinction values. For water, the molar extinction coefficients were obtained by our group by measuring distilled water in a spectrophotometer in various temperatures. Those water spectra at various temperatures have been used in the post-processing step to cancel out temperature effect. The employed molar extinction values of lipid were obtained from conventional values published in the literature by van Veen et al. “Determination of VIS-NIR absorption coefficients of mammalian fat, with time- and spatially resolved diffuse reflectance and transmission spectroscopy,” OSA Annual BIOMED Topical Meeting, 2004.
Post-Processing for Bound Water Measurements
The obtained μa values were post processed to measure different states of water. In order to get only water spectrum, spectra of oxy- and deoxy-hemoglobin and lipid were subtracted from the original absorption spectrum under assumption that only oxy- and deoxy-hemoglobin, lipid and water are major influential chromophores in breast tissues. Then the obtained water spectrum was compared to a pure water spectrum of breast temperature. The difference between the tissue water spectrum and the pure water spectrum was calculated by subtracting pure water spectra from normalized tissue water spectra in the wavelength range from 935 nm to 998 nm. Then, the absolute values of the differences were summed and divided by number of points in sum to form bound water index (BWI).
In-Vivo Breast Measurements
Line scans were performed to measure in-vivo malignant breast tumors. There were seven subjects (age: 48.3±7.4) and all of them were measured by the same spectrometer (B&W Tek 611) which performed auto calibration. The methods used for characterizing the optical and physiological properties of line scans were the same as the paper of Cerussi et al. above. The same arbitrary DOS parameters were employed to characterize physiological properties of tumor and normal tissues. In order to test statistical significance, two-tailed Wilcoxon/Kruskal-Wallis Rank Sums test was employed.
Tissue absorption spectra were acquired from the seven subjects who had malignant breast cancers. The measurements were performed contralaterally so that spectra could be acquired from both normal tissues and tumor tissues from the same subject. In
In summary, in the illustrated embodiment tissue bound water has been measured in breast cancer tissues using broadband DOS. BWI of normal tissues and malignant tumor tissues were different with statistical significance. Lower BWI in tumor tissues means that there is more free water in tumor tissues than normal tissues. We hypothesize that this is due to edema of tumor tissues. We contend that there is a statistical significance of the BWI in normal and cancer tissues. Furthermore, water states in a benign tumor and cyst as measured differentiate the water state in a malignant tumor from that of other types of lesion. In order to test the accuracy of bound water measurement and to acquire fraction of bound water, gelatin phantoms can be measured by broadband DOS and nuclear magnetic resonance both and the data can be compared. Also, the BWI can be compared to the apparent diffusion coefficient of water measured in vivo. Therefore tissue water states in cancer tissues under chemotherapy can be measured to show that BWI is helpful to monitor early response to chemotherapy agents for breast and other types of cancer patients.
Many alterations and modifications may be made by those having ordinary skill in the art without departing from the spirit and scope of the invention. Therefore, it must be understood that the illustrated embodiment has been set forth only for the purposes of example and that it should not be taken as limiting the invention as defined by the following invention and its various embodiments.
Therefore, it must be understood that the illustrated embodiment has been set forth only for the purposes of example and that it should not be taken as limiting the invention as defined by the following claims. For example, notwithstanding the fact that the elements of a claim are set forth below in a certain combination, it must be expressly understood that the invention includes other combinations of fewer, more or different elements, which are disclosed in above even when not initially claimed in such combinations. A teaching that two elements are combined in a claimed combination is further to be understood as also allowing for a claimed combination in which the two elements are not combined with each other, but may be used alone or combined in other combinations. The excision of any disclosed element of the invention is explicitly contemplated as within the scope of the invention.
The words used in this specification to describe the invention and its various embodiments are to be understood not only in the sense of their commonly defined meanings, but to include by special definition in this specification structure, material or acts beyond the scope of the commonly defined meanings. Thus if an element can be understood in the context of this specification as including more than one meaning, then its use in a claim must be understood as being generic to all possible meanings supported by the specification and by the word itself.
The definitions of the words or elements of the following claims are, therefore, defined in this specification to include not only the combination of elements which are literally set forth, but all equivalent structure, material or acts for performing substantially the same function in substantially the same way to obtain substantially the same result. In this sense it is therefore contemplated that an equivalent substitution of two or more elements may be made for any one of the elements in the claims below or that a single element may be substituted for two or more elements in a claim. Although elements may be described above as acting in certain combinations and even initially claimed as such, it is to be expressly understood that one or more elements from a claimed combination can in some cases be excised from the combination and that the claimed combination may be directed to a subcombination or variation of a subcombination.
Insubstantial changes from the claimed subject matter as viewed by a person with ordinary skill in the art, now known or later devised, are expressly contemplated as being equivalently within the scope of the claims. Therefore, obvious substitutions now or later known to one with ordinary skill in the art are defined to be within the scope of the defined elements.
The claims are thus to be understood to include what is specifically illustrated and described above, what is conceptionally equivalent, what can be obviously substituted and also what essentially incorporates the essential idea of the invention.
The present application is related to U.S. Provisional Patent Application Ser. No. 60/811,225, filed on Jun. 5, 2006, which is incorporated herein by reference and to which priority is claimed pursuant to 35 USC 119.
This invention was made with Government Support under Grant No. RR001192, awarded by the National Institutes of Health. The Government has certain rights in this invention.
Number | Date | Country | |
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60811225 | Jun 2006 | US |