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非均匀组织模型中II型卟吩姆钠介导的光动力治疗过程建模

Modeling of a type II photofrin-mediated photodynamic therapy process in a heterogeneous tissue phantom.

作者信息

Hu Xin-Hua, Feng Yuanming, Lu Jun Q, Allison Ron R, Cuenca Rosa E, Downie Gordon H, Sibata Claudio H

机构信息

Department of Physics, East Carolina University, Greenville, NC 27858, USA.

出版信息

Photochem Photobiol. 2005 Nov-Dec;81(6):1460-8. doi: 10.1562/2005-05-04-RA-513.

DOI:10.1562/2005-05-04-RA-513
PMID:15960591
Abstract

We present a quantitative framework to model a Type II photodynamic therapy (PDT) process in the time domain in which a set of rate equations are solved to describe molecular reactions. Calculation of steady-state light distributions using a Monte Carlo method in a heterogeneous tissue phantom model demonstrates that the photon density differs significantly in a superficial tumor of only 3 mm thickness. The time dependences of the photosensitizer, oxygen and intracellular unoxidized receptor concentrations were obtained and monotonic decreases in the concentrations of the ground-state photosensitizer and receptor were observed. By defining respective decay times, we quantitatively studied the effects of photon density, drug dose and oxygen concentration on photobleaching and cytotoxicity of a photofrin-mediated PDT process. Comparison of the dependences of the receptor decay time on photon density and drug dose at different concentrations of oxygen clearly shows an oxygen threshold under which the receptor concentration remains constant or PDT exhibits no cytotoxicity. Furthermore, the dependence of the photosensitizer and receptor decay times on the drug dose and photon density suggests the possibility of PDT improvement by maximizing cytotoxicity in a tumor with optimized light and drug doses. We also discuss the utility of this model toward the understanding of clinical PDT treatment of chest wall recurrence of breast carcinoma.

摘要

我们提出了一个定量框架,用于在时域中对II型光动力疗法(PDT)过程进行建模,其中求解一组速率方程以描述分子反应。在异质组织体模模型中使用蒙特卡罗方法计算稳态光分布表明,在仅3毫米厚的浅表肿瘤中,光子密度存在显著差异。获得了光敏剂、氧气和细胞内未氧化受体浓度的时间依赖性,并观察到基态光敏剂和受体浓度的单调下降。通过定义各自的衰减时间,我们定量研究了光子密度、药物剂量和氧气浓度对卟啉介导的PDT过程的光漂白和细胞毒性的影响。在不同氧气浓度下,受体衰减时间对光子密度和药物剂量的依赖性比较清楚地显示了一个氧气阈值,低于该阈值时受体浓度保持恒定或PDT不表现出细胞毒性。此外,光敏剂和受体衰减时间对药物剂量和光子密度的依赖性表明,通过在肿瘤中以优化的光剂量和药物剂量最大化细胞毒性,有可能改善PDT。我们还讨论了该模型对于理解乳腺癌胸壁复发的临床PDT治疗的实用性。

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