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核畸变作为结肠遗传毒性的短期检测方法:对小鼠体内19种试剂的评估

Nuclear aberrations as a short-term test for genotoxicity to the colon: evaluation of nineteen agents in mice.

作者信息

Wargovich M J, Goldberg M T, Newmark H L, Bruce W R

出版信息

J Natl Cancer Inst. 1983 Jul;71(1):133-7.

PMID:6575200
Abstract

The genotoxicity of 16 agents including several hydrazines, nitrosamines, aromatic amines, polycyclic hydrocarbons, and other related compounds and three known inhibitors of carcinogenesis was assessed in the murine colonic nuclear aberration assay. Of the seven agents considered positive for colonic DNA damage, five were large bowel carcinogens. All structural analogues of the intestinal carcinogens that are tumorigenic for other organs, with the exception of benzo[a]pyrene, were negative in the colonic nuclear aberration assay as were all noncarcinogens tested. The metabolic inhibitor disulfiram completely inhibited 1,2-dimethylhydrazine-induced colonic nuclear damage, while inhibition was less marked for the antioxidants butylated hydroxyanisole and caffeic acid. The versatility of the assay as an indicator of colonic genotoxicity resulting from carcinogen exposure is discussed.

摘要

在小鼠结肠核畸变试验中评估了16种试剂的遗传毒性,这些试剂包括几种肼类、亚硝胺类、芳香胺类、多环烃类以及其他相关化合物,还有三种已知的致癌作用抑制剂。在被认为对结肠DNA损伤呈阳性的七种试剂中,有五种是大肠癌致癌物。除苯并[a]芘外,对其他器官具有致瘤性的肠道致癌物的所有结构类似物,在结肠核畸变试验中均为阴性,所有测试的非致癌物也是如此。代谢抑制剂双硫仑完全抑制了1,2 - 二甲基肼诱导的结肠核损伤,而抗氧化剂丁基羟基茴香醚和咖啡酸的抑制作用则不太明显。本文讨论了该试验作为致癌物暴露所致结肠遗传毒性指标的通用性。

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