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Exploitable mechanisms for combining drugs with radiation: concepts, achievements and future directions.

机译:药物与辐射结合的可利用机制:概念,成就和未来方向。

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摘要

Widening indications for combining radiation therapy with cytotoxic or molecular-targeted drugs have mainly been driven by pragmatic clinical trials. With a flurry of novel drugs in various stages of preclinical and clinical development there is a need to revise the framework that has traditionally been used for discussing possible drug-radiation interactions, especially because many of the new drugs are directed at a specific molecular target. Spatial cooperation, cytotoxic enhancement, biological cooperation, temporal modulation and normal tissue protection are proposed as five primary exploitable mechanisms for the rational combination of drugs with radiation for cancer therapy. These five mechanisms produce different clinical outcomes and, therefore, the optimum clinical end point for assessing therapeutic benefit will depend on the mechanism tested. The dependence of outcome on these mechanisms also affects the selection of preclinical models and the optimum scheduling of the two modalities, i.e. the timing and dosing of the drug relative to the radiation dose fractions. These considerations are discussed in some detail for each mechanism and illustrated with specific clinical examples. Multi-modality therapy for head and neck squamous-cell carcinoma is used to illustrate these concepts. Further clinical progress in this field will require hypothesis-driven trials to ensure efficient identification of treatments with the most favorable risk:benefit ratio.
机译:放射治疗与细胞毒性或分子靶向药物结合的越来越广泛的适应症主要是由实用的临床试验推动的。随着在临床前和临床开发的各个阶段涌现出新药,有必要修改传统上用于讨论可能的药物-辐射相互作用的框架,特别是因为许多新药都针对特定的分子靶标。提出了空间合作,细胞毒增强,生物合作,时间调节和正常组织保护的五种主要开发机制,以将药物与放射线合理地结合用于癌症治疗。这五种机制产生不同的临床结果,因此,评估治疗效果的最佳临床终点将取决于所测试的机制。结果对这些机制的依赖性还影响临床前模型的选择和两种方式的最佳调度,即相对于放射剂量分数的药物的时间和剂量。这些注意事项已针对每种机制进行了详细讨论,并通过特定的临床实例进行了说明。头颈部鳞状细胞癌的多模式疗法被用来说明这些概念。该领域的进一步临床进展将需要假设驱动的试验,以确保有效鉴定具有最有利风险:获益比的治疗方法。

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