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Reactive oxygen species explicit dosimetry to predict tumor growth for BPD-mediated vascular photodynamic therapy

机译:活性氧显式剂量法预测BPD介导的血管光动力疗法治疗肿瘤的生长

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摘要

Photodynamic therapy (PDT) is a well-established treatment modality for cancer and other malignant diseases; however, quantities such as light fluence, and PDT dose do not fully account for all of the dynamic interactions between the key components involved. In particular, fluence rate (ϕ) effects are not accounted for, which has a large effect on the oxygen consumption rate. In this preclinical study, reacted reactive oxygen species ([ROS]rx) was investigated as a dosimetric quantity for PDT outcome. We studied the ability of [ROS]rx to predict the cure index (CI) after PDT of murine tumors; CI = 1 - k/kctr, where k and kctr are the growth rate of PDT-treated and control(untreated) tumor, respectively. Mice bearing radiation induced fibrosarcoma (RIF) tumors were treated with BPD-mediated PDT at different in-air fluences (22.5, 40, 45, 50, 70 and 100 J/cm2) and in-air ϕ (75 and 150 mW/cm2) with a BPD dose of 1 mg/kg and a drug-light interval of 15 mins. Treatment was delivered with a collimated laser beam of 1 cm diameter at 690 nm. Explicit dosimetry of initial tissue oxygen concentration, tissue optical properties, and BPD concentration was used to calculate [1O2]rx. ϕ was calculated for the treatment volume based on Monte-Carlo simulations and measured tissue optical properties. CI was used as an endpoint for four dose metrics: light fluence, PDT dose, and [ROS]rx. PDT dose was defined as the product of the time-integral of photosensitizer concentration and ϕ at a 3 mm tumor depth. Preliminary studies show that [ROS]rx best correlates with CI and is an effective dosimetric quantity that can predict treatment outcome. The threshold dose for [ROS]rx is determined to be 0.23 mM and is about 4.3 times smaller than the corresponding value for conventional BPD-mediated PDT using DLI of 3 hrs.
机译:光动力疗法(PDT)是一种公认​​的治疗癌症和其他恶性疾病的方法。但是,诸如光通量和PDT剂量之类的量并不能完全说明所涉及的关键组件之间的所有动态相互作用。特别地,没有考虑注量率(ϕ)的影响,这对耗氧率有很大的影响。在这项临床前研究中,研究了反应性活性氧([ROS] rx)作为PDT结果的剂量学剂量。我们研究了[ROS] rx预测小鼠肿瘤PDT后治愈指数(CI)的能力; CI = 1-k / kctr,其中k和kctr分别是PDT治疗和对照(未治疗)肿瘤的生长速率。用BPD介导的PDT以不同的空气通量(22.5、40、45、50、70和100 J / cm 2 )和空气中的剂量通过BPD介导的PDT治疗具有放射诱发性纤维肉瘤(RIF)的小鼠ϕ(75和150 mW / cm 2 ),BPD剂量为1 mg / kg,光照间隔为15分钟。用直径为1 cm的准直激光束在690 nm处进行处理。初始组织氧浓度,组织光学性质和BPD浓度的显式剂量学用于计算 [ 1 < / msup> O 2 ] < mtext> rx 。根据蒙特卡洛模拟和测得的组织光学特性计算治疗体积的。 CI被用作四个剂量指标的终点:光通量,PDT剂量和[ROS] rx。 PDT剂量定义为光敏剂浓度与3 mm肿瘤深度处的时间积分的乘积。初步研究表明[ROS] rx与CI最相关,并且是可以预测治疗结果的有效剂量。确定[ROS] rx的阈值剂量为0.23 mM,比使用DLI 3小时的常规BPD介导的PDT的相应值小约4.3倍。

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