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反应性代谢物捕获筛选中“硬”亲电试剂形成相关的 liabilities。 (注:这里“liabilities”在该语境下较难准确翻译出一个完全合适的词,暂保留英文,根据上下文可能是“相关问题”“潜在风险”之类的意思 )

Liabilities Associated with the Formation of "Hard" Electrophiles in Reactive Metabolite Trapping Screens.

作者信息

Kalgutkar Amit S

机构信息

Pharmacokinetics, Dynamics, and Metabolism - New Chemical Entities, Pfizer Worldwide Research and Development , 610 Main Street, Cambridge, Massachusetts 02139, United States.

出版信息

Chem Res Toxicol. 2017 Jan 17;30(1):220-238. doi: 10.1021/acs.chemrestox.6b00332. Epub 2016 Nov 10.

DOI:10.1021/acs.chemrestox.6b00332
PMID:27802597
Abstract

Soft electrophiles (e.g., epoxides, quinones, quinone-imines, quinone-methides, etc.) generated via the oxidative bioactivation of phenyl, phenolic, amino-, and alkylphenolic substituents can be trapped with nucleophiles of comparable softness (e.g., glutathione or cysteine) in reactive metabolite screens. In contrast, hard nucleophiles such as cyanide and amines are frequently utilized to trap hard electrophiles (e.g., iminiums and aldehydes) that result from the oxidative bioactivation of cyclic (or acylic) amines and primary alcohols. In some instances, soft sulfydryl nucleophiles have also been utilized to trap aldehydes to yield cyclized thiazolidine adducts. Case studies where hard electrophiles are thought to be responsible for cytochrome P450 inactivation, genotoxicity, and/or target organ toxicity in animals have been presented. The association of hard electrophiles with immune-mediated idiosyncratic adverse drug reactions is less clear given the paucity of available examples and the fact that several marketed drugs containing cyclic amine motifs can generate hard electrophiles via α-carbon ring oxidation. This perspective examines available data associating toxicity with the formation of hard electrophilic intermediates from small molecule drugs/drug candidates. Pragmatic risk mitigation strategies around unwarranted idiosyncratic toxicity risks with drug candidates that generate hard electrophiles are also discussed against the backdrop of marketed agents that possess analogous cyclic amine framework.

摘要

通过苯基、酚类、氨基和烷基酚取代基的氧化生物活化产生的软亲电试剂(如环氧化物、醌类、醌亚胺、醌甲基化物等),可在反应性代谢物筛选中被具有相当软度的亲核试剂(如谷胱甘肽或半胱氨酸)捕获。相比之下,硬亲核试剂如氰化物和胺类经常被用于捕获由环状(或非环状)胺类和伯醇的氧化生物活化产生的硬亲电试剂(如亚胺离子和醛类)。在某些情况下,软巯基亲核试剂也被用于捕获醛类以生成环化的噻唑烷加合物。已经介绍了一些案例研究,其中硬亲电试剂被认为是导致动物体内细胞色素P450失活、遗传毒性和/或靶器官毒性的原因。鉴于可用实例较少,以及几种含有环状胺基序的上市药物可通过α-碳环氧化生成硬亲电试剂这一事实,硬亲电试剂与免疫介导的特异质性药物不良反应之间的关联尚不清楚。本文探讨了将毒性与小分子药物/候选药物形成硬亲电中间体相关联的现有数据。在具有类似环状胺骨架的上市药物背景下,还讨论了针对产生硬亲电试剂的候选药物无端的特异质性毒性风险的实用风险缓解策略。

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