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Strategies for Discovery of Small Molecule Radiation Protectors and Radiation Mitigators

机译:发现小分子辐射防护剂和辐射缓解剂的策略

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摘要

Mitochondrial targeted radiation damage protectors (delivered prior to irradiation) and mitigators (delivered after irradiation, but before the appearance of symptoms associated with radiation syndrome) have been a recent focus in drug discovery for (1) normal tissue radiation protection during fractionated radiotherapy, and (2) radiation terrorism counter measures. Several categories of such molecules have been discovered: nitroxide-linked hybrid molecules, including GS-nitroxide, GS-nitric oxide synthase inhibitors, p53/mdm2/mdm4 inhibitors, and pharmaceutical agents including inhibitors of the phosphoinositide-3-kinase pathway and the anti-seizure medicine, carbamazepine. Evaluation of potential new radiation dose modifying molecules to protect normal tissue includes: clonogenic radiation survival curves, assays for apoptosis and DNA repair, and irradiation-induced depletion of antioxidant stores. Studies of organ specific radioprotection and in total body irradiation-induced hematopoietic syndrome in the mouse model for protection/mitigation facilitate rational means by which to move candidate small molecule drugs along the drug discovery pipeline into clinical development.
机译:线粒体靶向放射损伤保护剂(在放射线之前交付)和缓解剂(在放射线之后但在与放射综合征相关的症状出现之前交付)已经成为药物发现的新焦点,其目的是:(1)分级放疗期间的正常组织放射防护, (2)防辐射恐怖主义对策。已经发现了几类此类分子:与氮氧化物连接的杂合分子,包括GS-硝基氧,GS-一氧化氮合酶抑制剂,p53 / mdm2 / mdm4抑制剂以及药物,包括磷酸肌醇-3-激酶途径的抑制剂和抗-癫痫药,卡马西平。用于保护正常组织的潜在新的辐射剂量调节分子的评估包括:克隆形成的辐射存活曲线,凋亡和DNA修复检测以及辐射诱导的抗氧化剂存储耗竭。在用于保护/缓解的小鼠模型中,对器官特异性放射防护和全身辐射诱发的造血综合症的研究促进了合理的方法,通过该方法,可以将候选的小分子药物沿着药物发现管线转移到临床开发中。

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