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组织药物浓度决定了在外源性造影剂的扩散光学断层成像中,荧光测量还是吸收测量更为灵敏。

Tissue drug concentration determines whether fluorescence or absorption measurements are more sensitive in diffuse optical tomography of exogenous contrast agents.

作者信息

Davis Scott C, Pogue Brian W, Dehghani Hamid, Paulsen Keith D

机构信息

Thayer School of Engineering, Dartmouth College, Hanover, New Hampshire 03755, USA.

出版信息

Appl Opt. 2009 Apr 1;48(10):D262-72. doi: 10.1364/ao.48.00d262.

Abstract

The measurement sensitivities of absorbing and fluorescing objects in tissue are compared to determine conditions for which fluorescence data are favorable over those derived from absorption. A simulated human breast volume was used to model the relative perturbation in boundary data caused by a deeply embedded anomaly containing elevated concentrations of theoretical exogenous contrast agents with absorption properties resembling lutetium texaphyrin (LuTex) and Indocyanine Green (ICG). Synthetic data were used to produce quantum yield values representing the transition between conditions favorable to fluorescence versus absorption imaging. The parameters explored include tumor-to-background contrast, background drug concentration, and excitation light filtering efficiency. Drug concentration in the background was the primary factor that determined which contrast mechanism provided the more sensitive measurements. Specifically, fluorescence measurements are favorable if background drug concentrations are below 135-200 nM for LuTex and 25-50 nM for ICG, while absorption measurements are more sensitive above these ranges.

摘要

比较组织中吸收性和荧光性物体的测量灵敏度,以确定荧光数据优于吸收数据的条件。使用模拟的人体乳房体积来模拟由深部嵌入的异常引起的边界数据的相对扰动,该异常含有理论上的外源性造影剂,其吸收特性类似于镥四氮杂卟啉(LuTex)和吲哚菁绿(ICG),且浓度升高。合成数据用于生成量子产率值,以表示有利于荧光成像与吸收成像的条件之间的转变。探索的参数包括肿瘤与背景的对比度、背景药物浓度和激发光过滤效率。背景中的药物浓度是决定哪种对比机制能提供更灵敏测量的主要因素。具体而言,如果背景药物浓度低于LuTex的135 - 200 nM和ICG的25 - 50 nM,则荧光测量更有利,而在这些范围之上吸收测量更灵敏。

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