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稳定同位素标记和质谱联用方法在区分外源性和内源性 DNA 加合物及改善剂量反应评估中的研究进展。

A Review of Stable Isotope Labeling and Mass Spectrometry Methods to Distinguish Exogenous from Endogenous DNA Adducts and Improve Dose-Response Assessments.

机构信息

Department of Environmental Sciences and Engineering, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina 27599, United States.

Rita Schoeny LLC, 726 Fifth Street NE, Washington, D.C. 20002, United States.

出版信息

Chem Res Toxicol. 2022 Jan 17;35(1):7-29. doi: 10.1021/acs.chemrestox.1c00212. Epub 2021 Dec 15.

Abstract

Cancer remains the second most frequent cause of death in human populations worldwide, which has been reflected in the emphasis placed on management of risk from environmental chemicals considered to be potential human carcinogens. The formation of DNA adducts has been considered as one of the key events of cancer, and persistence and/or failure of repair of these adducts may lead to mutation, thus initiating cancer. Some chemical carcinogens can produce DNA adducts, and DNA adducts have been used as biomarkers of exposure. However, DNA adducts of various types are also produced endogenously in the course of normal metabolism. Since both endogenous physiological processes and exogenous exposure to xenobiotics can cause DNA adducts, the differentiation of the sources of DNA adducts can be highly informative for cancer risk assessment. This review summarizes a highly applicable methodology, termed stable isotope labeling and mass spectrometry (SILMS), that is superior to previous methods, as it not only provides absolute quantitation of DNA adducts but also differentiates the exogenous and endogenous origins of DNA adducts. SILMS uses stable isotope-labeled substances for exposure, followed by DNA adduct measurement with highly sensitive mass spectrometry. Herein, the utilities and advantage of SILMS have been demonstrated by the rich data sets generated over the last two decades in improving the risk assessment of chemicals with DNA adducts being induced by both endogenous and exogenous sources, such as formaldehyde, vinyl acetate, vinyl chloride, and ethylene oxide.

摘要

癌症仍然是全球人类死亡的第二大主要原因,这反映在对被认为是潜在人类致癌物的环境化学物质风险管理的重视上。DNA 加合物的形成被认为是癌症的关键事件之一,这些加合物的持续存在和/或修复失败可能导致突变,从而引发癌症。一些化学致癌物可以产生 DNA 加合物,并且 DNA 加合物已被用作暴露的生物标志物。然而,在正常代谢过程中也会在内源性产生各种类型的 DNA 加合物。由于内源性生理过程和外源性暴露于外来物质都可能导致 DNA 加合物,因此区分 DNA 加合物的来源对于癌症风险评估非常有意义。

这篇综述总结了一种非常适用的方法,称为稳定同位素标记和质谱法 (SILMS),它优于以前的方法,因为它不仅提供 DNA 加合物的绝对定量,而且还区分了 DNA 加合物的外源性和内源性来源。SILMS 使用稳定同位素标记的物质进行暴露,然后用高灵敏度的质谱法测量 DNA 加合物。

在过去的二十年中,通过生成丰富的数据集,SILMS 已经证明了其在改善由内源性和外源性来源(如甲醛、醋酸乙烯酯、氯乙烯和环氧乙烷)诱导的具有 DNA 加合物的化学物质的风险评估中的效用和优势。

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