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加合物组学:描述对反应性亲电子试剂的暴露情况。

Adductomics: characterizing exposures to reactive electrophiles.

机构信息

Center for Exposure Biology, School of Public Health and College of Chemistry, University of California, Berkeley, CA 94720-7356, USA.

出版信息

Toxicol Lett. 2012 Aug 13;213(1):83-90. doi: 10.1016/j.toxlet.2011.04.002. Epub 2011 Apr 8.

Abstract

To understand environmental causes of disease, unbiased methods are needed to characterize the human exposome, which represents all toxicants to which people are exposed from both exogenous and endogenous sources. Because they directly modify DNA and important proteins, reactive electrophiles are probably the most important constituents of the exposome. Exposures to reactive electrophiles can be characterized by measuring adducts from reactions between circulating electrophiles and blood nucleophiles. We define an 'adductome' as the totality of such adducts with a given nucleophilic target. Because of their greater abundance and residence times in human blood, adducts of hemoglobin (Hb) and human serum albumin (HSA) are preferable to those of DNA and glutathione for characterizing adductomes. In fact, the nucleophilic hotspot represented by the only free sulfhydryl group in HSA (HSA-Cys(34)) offers particular advantages for adductomic experiments. Although targeted adducts of HSA-Cys(34) have been monitored for decades, an unbiased method has only recently been reported for visualizing the HSA-Cys(34) 'subadductome'. The method relies upon a novel mass spectrometry application, termed fixed-step selected reaction monitoring (FS-SRM), to profile Cys(34) adducts in tryptic digests of HSA. Here, we selectively review the literature regarding the potential of adductomics to partially elucidate the human exposome, with particular attention to the HSA-Cys(34) subadductome.

摘要

为了了解疾病的环境原因,需要使用公正的方法来描述人体暴露组,它代表了人们从外源性和内源性来源接触的所有毒物。由于它们直接修饰 DNA 和重要蛋白质,反应性亲电试剂可能是暴露组中最重要的成分。可以通过测量循环亲电试剂与血液亲核试剂之间反应的加合物来描述反应性亲电试剂的暴露。我们将“加合物组”定义为与特定亲核靶标发生反应的所有此类加合物的总和。由于其在人血液中的丰度和停留时间更长,血红蛋白 (Hb) 和人血清白蛋白 (HSA) 的加合物比 DNA 和谷胱甘肽的加合物更适合用于描述加合物组。事实上,HSA 中唯一游离巯基代表的亲核热点 (HSA-Cys(34)) 为加合物组实验提供了特别的优势。尽管已经监测 HSA-Cys(34) 的靶向加合物数十年,但直到最近才报道了一种用于可视化 HSA-Cys(34)“亚加合物组”的非靶向方法。该方法依赖于一种新的质谱应用,称为固定步长选择反应监测 (FS-SRM),用于分析 HSA 中 Cys(34)加合物的肽谱。在这里,我们选择性地回顾了关于加合物组学部分阐明人体暴露组的潜力的文献,特别关注 HSA-Cys(34) 亚加合物组。

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