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通过气相色谱-质谱联用仪测定尿液中血红蛋白和核酸碱基的加合物来估算烷基化致癌物的暴露量。

Estimation of exposure to alkylating carcinogens by the GC-MS determination of adducts to hemoglobin and nucleic acid bases in urine.

作者信息

Bailey E, Farmer P B, Shuker D E

出版信息

Arch Toxicol. 1987;60(1-3):187-91. doi: 10.1007/BF00296978.

Abstract

Many carcinogens and mutagens are electrophilic in nature and will react with nucleophilic sites in protein and nucleic acid. Determination of the extent of formation of these adducts of genotoxic agents with protein provides a practical method of monitoring human exposure and of determining the possible risk associated with the exposure. Proteins are predominantly attacked on the cysteine, histidine and N-terminal amino acids. Hemoglobin is the most suitable protein for dose monitoring due to its ready availability and its long lifetime. Methods have been developed using capillary gas chromatography with mass spectrometry for determining S-methylcysteine, Nr-[2-hydroxyethyl]histidine and Nr-[2-hydroxypropyl]histidine in hemoglobin, allowing the monitoring of in vivo exposure of laboratory animals and humans to methylating agents, ethylene oxide and propylene oxide, respectively. A method for monitoring exposure to acrylamide has also been devised based on the determination by gas chromatography-mass spectrometry of the adduct formed with cysteine residues in hemoglobin. An alternative method of dose monitoring of some methylating agents by the measurement of the urinary N-7-methylated guanine derived from alkylated DNA breakdown products has also been investigated.

摘要

许多致癌物和诱变剂本质上是亲电的,会与蛋白质和核酸中的亲核位点发生反应。测定这些基因毒性剂与蛋白质形成加合物的程度,为监测人体暴露情况以及确定与暴露相关的潜在风险提供了一种实用方法。蛋白质主要在半胱氨酸、组氨酸和N端氨基酸处受到攻击。血红蛋白因其易于获取且寿命长,是最适合用于剂量监测的蛋白质。已开发出使用毛细管气相色谱-质谱联用技术测定血红蛋白中S-甲基半胱氨酸、Nτ-[2-羟乙基]组氨酸和Nτ-[2-羟丙基]组氨酸的方法,分别用于监测实验动物和人类体内对甲基化剂、环氧乙烷和环氧丙烷的暴露情况。还设计了一种基于气相色谱-质谱联用技术测定血红蛋白中与半胱氨酸残基形成的加合物来监测丙烯酰胺暴露的方法。另外,通过测量源自烷基化DNA分解产物的尿N-7-甲基鸟嘌呤来监测某些甲基化剂剂量的替代方法也已得到研究。

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