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首页> 外文期刊>Cancer letters >Integration of toxicological approaches with 'omic' and related technologies to elucidate mechanisms of carcinogenic action: Propiconazole, an example
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Integration of toxicological approaches with 'omic' and related technologies to elucidate mechanisms of carcinogenic action: Propiconazole, an example

机译:将毒理学方法与“ omic”及相关技术相结合以阐明致癌作用的机制:丙哌唑,一个例子

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摘要

The field of mechanistic chemical carcinogenesis has evolved with the advent and advances in genomic, proteomic and metabolomic technologies. These advances allow mechanistic events along the process of exposure to frank tumors to be studied in great detail. Herein is reviewed an example of this approach using, propiconazole, a triazole-containing antifungal agent that is a mouse hepatocarcinogen. This review will highlight those toxicological, genomic, proteomic and metabolomic findings in mice that were used to describe a set of linked events that lead to propiconazole-induced hepatocarcinogenesis. Independent experimental proof of many of these events is presented that solidified this proposed mechanism of carcinogenic action for propiconazole.
机译:机械化学致癌的领域随着基因组学,蛋白质组学和代谢组学技术的出现和发展而发展。这些进展允许对暴露于坦率肿瘤的过程中的机械事件进行详细研究。本文回顾了使用丙环唑的方法的一个例子,丙环唑是一种含三唑的抗真菌剂,是小鼠肝癌的致癌剂。这篇综述将重点介绍小鼠中的毒理学,基因组学,蛋白质组学和代谢组学发现,这些发现被用来描述一系列导致丙环唑诱导的肝癌发生的相关事件。提供了许多此类事件的独立实验证据,这些证据巩固了拟议的丙环唑致癌作用机理。

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