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通过碱性全甲基化鉴定与蛋白质硫亲核试剂形成的共价加合物。

Identification of covalent adducts to protein sulfur nucleophiles by alkaline permethylation.

作者信息

Slaughter D E, Zheng J, Harriman S, Hanzlik R P

机构信息

Department of Medicinal Chemistry, University of Kansas, Lawrence 66045.

出版信息

Anal Biochem. 1993 Feb 1;208(2):288-95. doi: 10.1006/abio.1993.1048.

Abstract

We recently reported on the identification of metabolites of the hepatotoxin bromobenzene covalently bound to rat liver protein sulfur nucleophiles (D. E. Slaughter and R. P. Hanzlik, Chem. Res. Toxicol. 4, 349-359 (1991). Central to that study was our development of a method called alkaline permethylation which converts protein-S adducts of xenobiotic electrophiles to stable extractable thioanisole derivatives. We report here on substantial improvements to our original alkaline permethylation method which should greatly expand its potential utility. Specifically, we have developed significantly milder reaction conditions, eliminated side reactions, improved the amount of and consistency of thioanisole yields from various mercapturic acid model compounds, and increased the overall sensitivity of the method at least 50-fold. Using the procedure described herein it is routinely possible to generate, detect, and identify by GC/MS as little as 2 pmol of a thioanisole derivative. This method is potentially quite general and should prove useful for studies in the toxicology of reactive metabolites, for industrial hygiene and biomonitoring, and for agrichemical residue analysis.

摘要

我们最近报道了对与大鼠肝脏蛋白质硫亲核试剂共价结合的肝毒素溴苯代谢物的鉴定(D. E. 斯劳特和R. P. 汉兹利克,《化学研究毒理学》4,349 - 359(1991年))。该研究的核心是我们开发的一种称为碱性全甲基化的方法,该方法可将外源性亲电试剂的蛋白质 - S加合物转化为稳定的可提取硫代苯甲醚衍生物。我们在此报告对我们原来的碱性全甲基化方法的重大改进,这应该会大大扩展其潜在用途。具体而言,我们开发了明显更温和的反应条件,消除了副反应,提高了各种硫醚氨酸模型化合物的硫代苯甲醚产率的数量和一致性,并将该方法的整体灵敏度提高了至少50倍。使用本文所述的方法,常规情况下可以通过气相色谱/质谱法生成、检测和鉴定低至2皮摩尔的硫代苯甲醚衍生物。这种方法可能非常通用,应该对反应性代谢物毒理学研究、工业卫生和生物监测以及农用化学品残留分析有用。

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