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光动力疗法(pPDT)中血卟啉介导的胸膜 PDT 剂量测定。

PDT dose dosimetry for Photofrin-mediated pleural photodynamic therapy (pPDT).

机构信息

Department of Radiation Oncology, University of Pennsylvania, Philadelphia, PA 19104, United States of America. Department of Physics and Astronomy, University of Pennsylvania, Philadelphia, PA 19104, United States of America.

出版信息

Phys Med Biol. 2017 Dec 29;63(1):015031. doi: 10.1088/1361-6560/aa9874.

Abstract

Photosensitizer fluorescence excited by photodynamic therapy (PDT) treatment light can be used to monitor the in vivo concentration of the photosensitizer and its photobleaching. The temporal integral of the product of in vivo photosensitizer concentration and light fluence is called PDT dose, which is an important dosimetry quantity for PDT. However, the detected photosensitizer fluorescence may be distorted by variations in the absorption and scattering of both excitation and fluorescence light in tissue. Therefore, correction of the measured fluorescence for distortion due to variable optical properties is required for absolute quantification of photosensitizer concentration. In this study, we have developed a four-channel PDT dose dosimetry system to simultaneously acquire light dosimetry and photosensitizer fluorescence data. We measured PDT dose at four sites in the pleural cavity during pleural PDT. We have determined an empirical optical property correction function using Monte Carlo simulations of fluorescence for a range of physiologically relevant tissue optical properties. Parameters of the optical property correction function for Photofrin fluorescence were determined experimentally using tissue-simulating phantoms. In vivo measurements of photosensitizer fluorescence showed negligible photobleaching of Photofrin during the PDT treatment, but large intra- and inter-patient heterogeneities of in vivo Photofrin concentration are observed. PDT doses delivered to 22 sites in the pleural cavity of 8 patients were different by 2.9 times intra-patient and 8.3 times inter-patient.

摘要

光动力疗法 (PDT) 治疗光激发的光敏剂荧光可用于监测体内光敏剂的浓度及其光漂白。体内光敏剂浓度与光辐照度的乘积的时间积分称为 PDT 剂量,这是 PDT 的重要剂量学参数。然而,由于组织中激发光和荧光的吸收和散射的变化,检测到的光敏剂荧光可能会发生失真。因此,为了对光敏剂浓度进行绝对定量,需要对由于可变光学特性引起的测量荧光进行校正。在这项研究中,我们开发了一个四通道 PDT 剂量剂量测定系统,以同时获取光剂量和光敏剂荧光数据。我们在胸腔 PDT 期间测量了胸腔内四个部位的 PDT 剂量。我们使用荧光的蒙特卡罗模拟确定了一个经验光学特性校正函数,用于一系列与生理相关的组织光学特性。使用组织模拟体实验确定了 Photofrin 荧光的光学特性校正函数的参数。体内光敏剂荧光的测量表明,在 PDT 治疗过程中 Photofrin 几乎没有光漂白,但观察到体内 Photofrin 浓度的个体内和个体间存在很大的异质性。8 名患者胸腔 22 个部位的 PDT 剂量,个体内差异 2.9 倍,个体间差异 8.3 倍。

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