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PDT 剂量参数影响三维卵巢癌模型中的肿瘤杀伤持久性和细胞死亡途径。

PDT dose parameters impact tumoricidal durability and cell death pathways in a 3D ovarian cancer model.

机构信息

Wellman Center for Photomedicine, Department of Dermatology, Massachusetts General Hospital, Harvard Medical School, Boston, MA, USA.

出版信息

Photochem Photobiol. 2013 Jul-Aug;89(4):942-52. doi: 10.1111/php.12065. Epub 2013 Apr 4.

Abstract

The successful implementation of photodynamic therapy (PDT)-based regimens depends on an improved understanding of the dosimetric and biological factors that govern therapeutic variability. Here, the kinetics of tumor destruction and regrowth are characterized by systematically varying benzoporphyrin derivative (BPD)-light combinations to achieve fixed PDT doses (M × J cm(-2)). Three endpoints were used to evaluate treatment response: (1) Viability evaluated every 24 h for 5 days post-PDT; (2) Photobleaching assessed immediately post-PDT; and (3) Caspase-3 activation determined 24 h post-PDT. The specific BPD-light parameters used to construct a given PDT dose significantly impact not only acute cytotoxic efficacy, but also treatment durability. For each dose, PDT with 0.25 μM BPD produces the most significant and sustained reduction in normalized viability compared to 1 and 10 μM BPD. Percent photobleaching correlates with normalized viability for a range of PDT doses achieved within BPD concentrations. To produce a cytotoxic response with 10 μM BPD that is comparable to 0.25 and 1 μM BPD a reduction in irradiance from 150 to 0.5 mW cm(-2) is required. Activated caspase-3 does not correlate with normalized viability. The parameter-dependent durability of outcomes within fixed PDT doses provides opportunities for treatment customization and improved therapeutic planning.

摘要

光动力疗法(PDT)方案的成功实施取决于对控制治疗变异性的剂量学和生物学因素的深入了解。在这里,通过系统地改变苯并卟啉衍生物(BPD)-光组合来实现固定 PDT 剂量(M×J cm(-2)),从而描述肿瘤破坏和再生长的动力学。使用三个终点来评估治疗反应:(1)PDT 后 5 天内每 24 小时评估一次活力;(2)PDT 后立即评估光漂白;(3)PDT 后 24 小时确定半胱天冬酶-3 激活。用于构建特定 PDT 剂量的特定 BPD-光参数不仅显著影响急性细胞毒性功效,而且还影响治疗持久性。对于每个剂量,与 1 和 10 μM BPD 相比,0.25 μM BPD 的 PDT 产生最显著和持续的归一化活力降低。在 BPD 浓度范围内实现的一系列 PDT 剂量的光漂白百分比与归一化活力相关。为了用 10 μM BPD 产生与 0.25 和 1 μM BPD 相当的细胞毒性反应,需要将辐照度从 150 降低到 0.5 mW cm(-2)。激活的半胱天冬酶-3与归一化活力无关。固定 PDT 剂量内结果的参数依赖性耐久性为治疗定制和改善治疗计划提供了机会。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2c43/3701746/b08f4fa29340/nihms453750f1.jpg

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