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Photon dynamics in tissue imaging

机译:组织成像中的光子动力学

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The emerging need for a fast, safe economical approach to global and localized measures of desaturation of hemoglobin with oxygen (%HbO2) in the human brain motivates further research on time-resolved spectroscopy in four areas of study. (1) To afford quantization of hemoglobin saturation through time-resolved spectroscopy in the time domain (TD) and in the frequency domain (FD). Evaluation of dual-wavelength TD and FD spectrometers for determining quantitatively hemoglobin desaturation and blood-volume changes by calculations that are insensitive to mutual interference is proposed. The diffusion equation, as it applies especially to TD studies, and the absorption ($mu$-a$/) and scattering ($mu$-s$/) coefficients provide their independent determination from the late and early respective portions of the kinetics of the emergent photons in response to a short input pulse (50-100 psec). (2) The identification of the photon-pathlength change due to the arterial pulse in the brain tissue by FD methods with Fourier transformation affords an opportunity to employ principles of pulse oximetry to vessels localized deep within the brain tissue. (3) Localization of desaturation of hemoglobin in portions of the brain can be achieved through dual-wavelength scanning of the input/output optical fibers across the head for an X-Y coordinate and varying the distance between input and output ($rho@) or the time delay in data acquisition to afford an in-depth Z scan. Localizations of shed blood, which have an effective concentration of over 10 times that of capillary-bed blood, are identified by X, Y, Z scans using only a single wavelength. (4) Independent measurements of absorption ($mu$-a$/) and scattering ($mu$-s$/) coefficients, particularly by TD techniques, affords structural mapping of the brain, which can be used to diagnose brain tumor and neuronal degeneration. Two experimental systems are used to critically evaluate these studies; the first, a hemoglobin/lipid/yeast model in which intermittent oxygenation gives saturation/desaturation effects and addition of hemoglobin simulates increased blood volume. These models can be global or may contain localized 'black' absorbers simulating brain bleeds or model-stroke volumes in which oxygenation/deoxygenation simulates normoxia/hypoxia. Secondly, animal brains are used to model the following changes in vivo: global or localized hypoxia, brain bleeding, and hematomas by epidural blood injection, and physiological changes by epilepsy. Neuronal degeneration causing scattering effects is modeled by injection, epidurally or into the animal model brain, highly scattering material such as polystyrene spheres. The proposal envisages a basic science study of photon migration in the brain with important applications to stroke, epilepsy, brain trauma, and neuronal degenerative disease.
机译:新兴需求对人脑中的氧气(%HBO2)的血红蛋白去饱和度的全球和局部措施的快速,安全的经济方法促进了四个研究领域的时间分辨光谱的进一步研究。 (1)通过时域(TD)中的时间分辨光谱和频域(FD)提供血红蛋白饱和度的量化。提出了一种评价双波长Td和FD光谱仪来确定通过计算对相互干扰不敏感的计算的定量血红蛋白去饱和度和血容量的变化。尤其适用于TD研究的扩散方程,以及吸收($ mu $-$ /)和散射($ mu $ /)系数提供了从动力学的晚期和早期各部分的自主决定响应于短输入脉冲(50-100psec)的紧急光子。 (2)通过FD方法具有傅立叶变换的FD方法由于脑组织中的动脉脉冲引起的光子 - 脉冲的鉴定提供了机会,用于采用脉冲血氧血管原理对脑组织内部局部深处的血管。 (3)通过对头部的输入/输出光纤的双波长扫描来实现血红蛋白的未去饱和的定位,用于XY坐标并改变输入和输出之间的距离($ RHO @)或数据采集​​中的时间延迟,以提供深入的Z扫描。通过仅使用单个波长识别X,Y,Z扫描鉴定毛细血管床血液的有效浓度超过10倍的血液血液的本地化。 (4)吸收的独立测量($ MU $-$ /)和散射($ MU $ /)系数,特别是TD技术,提供了大脑的结构映射,可用于诊断脑肿瘤和神经元变性。两种实验系统用于批判性评估这些研究;首先,一种血红蛋白/脂质/酵母模型,其中间歇氧合产生饱和/去饱和效应并添加血红蛋白模拟血液量增加。这些模型可以是全球性的,也可以包含局部的“黑色”吸收剂,模拟脑出血或模型行程体积,其中氧合/脱氧模拟常氧/缺氧。其次,动物脑用于模拟体内的变化:全球或局部缺氧,脑出血和血肿,外膜血液注射,癫痫患者的生理变化。引起散射效果的神经元变性是通过注射,渗透的或进入动物模型脑,高散射材料,例如聚苯乙烯球体的建模。该提案设想了大脑中光子迁移的基础科学研究,其具有中风,癫痫,脑外疾病和神经元退行性疾病的重要应用。

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