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环氧化物及生成环氧化物的化学物质行为的致癌性及作用机制见解

Carcinogenicity and mechanistic insights on the behavior of epoxides and epoxide-forming chemicals.

作者信息

Melnick Ronald L

机构信息

National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina 27709, USA.

出版信息

Ann N Y Acad Sci. 2002 Dec;982:177-89. doi: 10.1111/j.1749-6632.2002.tb04932.x.

Abstract

Many epoxides and their precursors are high production volume chemicals that have major uses in the polymer industry and as intermediates in the manufacture of other chemicals. Several of these chemicals were demonstrated to be carcinogenic in laboratory animal studies conducted by the Ramazzini Foundation (e.g., vinyl chloride, acrylonitrile, styrene, styrene oxide, and benzene) and by the National Toxicology Program (e.g., ethylene oxide, 1,3-butadiene, isoprene, chloroprene, acrylonitrile, glycidol, and benzene). The most common sites of tumor induction were lung, liver, harderian gland, and circulatory system in mice; Zymbal's gland and brain in rats; and mammary gland and forestomach in both species. Differences in cancer outcome among studies of epoxide chemicals may be related to differences in study design (e.g., dose, duration, and route of exposure; observation period; animal strains), as well as biological factors affecting target organ dosimetry of the DNA-reactive epoxide (toxicokinetics) and tissue response (toxicodynamics). N7-Alkylguanine, N1-alkyladenine, and cyclic etheno adducts, as well as K-ras and p53 mutations, have been detected in animals and/or workers exposed to several of these chemicals. The classifications of these chemical carcinogens by IARC and NTP are based on animal and human data and results of mechanistic studies. Reducing occupational and environmental exposures to these chemicals will certainly reduce human cancer risks.

摘要

许多环氧化物及其前体都是高产量化学品,在聚合物工业中具有主要用途,并作为制造其他化学品的中间体。拉马齐尼基金会(例如氯乙烯、丙烯腈、苯乙烯、氧化苯乙烯和苯)以及国家毒理学计划(例如环氧乙烷、1,3 - 丁二烯、异戊二烯、氯丁二烯、丙烯腈、缩水甘油和苯)进行的实验室动物研究表明,其中几种化学品具有致癌性。在小鼠中,最常见的肿瘤诱发部位是肺、肝、哈德氏腺和循环系统;在大鼠中是齐默尔氏腺和脑;在这两个物种中都是乳腺和前胃。环氧化物化学品研究之间癌症结果的差异可能与研究设计的差异(例如剂量、持续时间和暴露途径;观察期;动物品系)以及影响DNA反应性环氧化物靶器官剂量测定(毒代动力学)和组织反应(毒效动力学)的生物学因素有关。在接触这些化学品中的几种的动物和/或工人中已检测到N7 - 烷基鸟嘌呤、N1 - 烷基腺嘌呤和环乙烯加合物,以及K - ras和p53突变。国际癌症研究机构(IARC)和美国国家毒理学计划(NTP)对这些化学致癌物的分类是基于动物和人类数据以及机制研究结果。减少职业和环境中对这些化学品的接触肯定会降低人类患癌风险。

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