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2-(1-己氧基乙基)-2-去乙烯基焦脱镁叶绿酸-a介导的光动力疗法的显式剂量测定:宏观单线态氧建模

Explicit dosimetry for 2-(1-hexyloxyethyl)-2-devinyl pyropheophorbide-a-mediated photodynamic therapy: macroscopic singlet oxygen modeling.

作者信息

Penjweini Rozhin, Liu Baochang, Kim Michele M, Zhu Timothy C

出版信息

J Biomed Opt. 2015;20(12):128003. doi: 10.1117/1.JBO.20.12.128003.

Abstract

Type II photodynamic therapy (PDT) is based on the photochemical reactions mediated through an interaction between a photosensitizer, ground-state oxygen ([(3)O2]), and light excitation at an appropriate wavelength, which results in production of reactive singlet oxygen ([(1)O2]rx). We use an empirical macroscopic model based on four photochemical parameters for the calculation of [(1)O2]rx threshold concentration ([(1)O2]rx,sh) causing tissue necrosis in tumors after PDT. For this reason, 2-(1-hexyloxyethyl)-2-devinyl pyropheophorbide-a (HPPH)-mediated PDT was performed interstitially on mice with radiation-induced fibrosarcoma (RIF) tumors. A linear light source at 665 nm with total energy released per unit length of 12 to 100  J/cm and source power per unit length (LS) of 12 to 150  mW/cm was used to induce different radii of necrosis. Then the amount of [(1)O2]rx calculated by the macroscopic model incorporating explicit PDT dosimetry of light fluence distribution, tissue optical properties, and HPPH concentration was correlated to the necrotic radius to obtain the model parameters and [(1)O2]rx,sh. We provide evidence that [(1)O2]rx is a better dosimetric quantity for predicting the treatment outcome than PDT dose, which is proportional to the time integral of the products of the photosensitizer concentration and light fluence rate.

摘要

II型光动力疗法(PDT)基于光化学反应,该反应通过光敏剂、基态氧([(3)O2])与适当波长的光激发之间的相互作用介导,从而产生反应性单线态氧([(1)O2]rx)。我们使用基于四个光化学参数的经验宏观模型来计算[(1)O2]rx阈值浓度([(1)O2]rx,sh),该浓度会导致PDT后肿瘤组织坏死。因此,对患有辐射诱导纤维肉瘤(RIF)肿瘤的小鼠进行了间质内2-(1-己氧基乙基)-2-去乙烯基焦脱镁叶绿酸-a(HPPH)介导的PDT。使用665 nm的线性光源,每单位长度释放的总能量为12至100 J/cm,每单位长度的光源功率(LS)为12至150 mW/cm,以诱导不同半径的坏死。然后,通过结合光通量分布、组织光学特性和HPPH浓度的显式PDT剂量测定的宏观模型计算出的[(1)O2]rx量与坏死半径相关,以获得模型参数和[(1)O2]rx,sh。我们提供的证据表明,与PDT剂量相比,[(1)O2]rx是预测治疗结果的更好的剂量学量,PDT剂量与光敏剂浓度和光通量率乘积的时间积分成正比。

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