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软、硬亲电毒物毒性的作用机制。

Mechanisms of soft and hard electrophile toxicities.

机构信息

Department of Anesthesiology, Montefiore Medical Center, Albert Einstein College of Medicine, 111 E. 210th St, Bronx NY 10467, United States.

Department of Anesthesiology, Montefiore Medical Center, Albert Einstein College of Medicine, 111 E. 210th St, Bronx NY 10467, United States.

出版信息

Toxicology. 2019 Apr 15;418:62-69. doi: 10.1016/j.tox.2019.02.005. Epub 2019 Feb 28.

DOI:10.1016/j.tox.2019.02.005
PMID:30826385
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6494464/
Abstract

Electron-deficient chemicals (electrophiles) react with compounds that have one or more unshared valence electron pairs (nucleophiles). The resulting covalent reactions between electrophiles and nucleophiles (e.g., Michael addition, S2 reactions) are important, not only to Organic Chemistry, but also to the fields of Molecular Biology and Toxicology. Specifically, covalent bond formation is the operational basis of many critically important cellular processes; e.g., enzyme function, neurotransmitter release, and membrane-vesicle fusion. Given this context it is understandable that these reactions are also relevant to Toxicology, since a significant number of xenobiotic chemicals are toxic electrophiles that can react with endogenous nucleophilic residues. Therefore, the purpose of this Review is to discuss electrophile-nucleophile chemistry as it pertains to cell injury and resulting organ toxicity. Our discussion will involve an introduction to the Hard and Soft, Acids and Bases (HSAB) theory of Pearson. The HSAB concept provides a framework for calculation of quantum chemical parameters that classify the electrophile and nucleophile covalent components according to their respective electronic nature (softness/hardness) and reactivity (electrophilicity/nucleophilicity). The calculated quantum indices in conjunction with corroborative in vivo, in chemico (cell free) and in vitro research can offer an illuminating approach to mechanistic discovery. Accordingly, we will provide examples that demonstrate how this approach has been used to discern mechanisms and sites of electrophile action.

摘要

缺电子化学物质(亲电试剂)与具有一个或多个未共用价电子对的化合物(亲核试剂)反应。亲电试剂和亲核试剂之间的这种共价反应(例如迈克尔加成、S2 反应)非常重要,不仅对有机化学,而且对分子生物学和毒理学领域都很重要。具体而言,共价键的形成是许多极其重要的细胞过程的操作基础;例如,酶的功能、神经递质的释放和膜囊泡融合。鉴于此,这些反应与毒理学也有关,因为许多外源化学物质是有毒的亲电试剂,可以与内源性亲核残基反应。因此,本综述的目的是讨论亲电亲核化学与细胞损伤和由此产生的器官毒性的关系。我们的讨论将包括对 Pearson 的软硬酸碱(HSAB)理论的介绍。HSAB 概念为计算量子化学参数提供了一个框架,根据其各自的电子性质(软度/硬度)和反应性(亲电性/亲核性)对亲电试剂和亲核试剂的共价成分进行分类。计算出的量子指数与体内、化学(无细胞)和体外研究的佐证相结合,可以为发现机制提供一种启发性的方法。因此,我们将提供一些示例,展示如何使用这种方法来辨别亲电试剂的作用机制和作用部位。

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