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致癌物α-细辛脑在肝微粒体中的代谢

Metabolism of the carcinogen alpha-asarone in liver microsomes.

作者信息

Cartus Alexander T, Schrenk Dieter

机构信息

University of Kaiserslautern, Food Chemistry and Toxicology, Erwin-Schroedinger-Strasse 52, 67663 Kaiserslautern, Germany.

University of Kaiserslautern, Food Chemistry and Toxicology, Erwin-Schroedinger-Strasse 52, 67663 Kaiserslautern, Germany.

出版信息

Food Chem Toxicol. 2016 Jan;87:103-12. doi: 10.1016/j.fct.2015.11.021. Epub 2015 Dec 8.

DOI:10.1016/j.fct.2015.11.021
PMID:26678343
Abstract

Alpha-asarone (1) is a naturally occurring phenylpropene found in several plants, e.g. Acorus calamus. 1-containing plant materials and essential oils thereof are used for flavoring foods and in many phytopharmaceuticals. 1 has been claimed to have positive pharmacological effects, however, it is carcinogenic in male mice (liver) and probably genotoxic. Since the metabolic pathways of 1 have not been investigated and its carcinogenic mode of action is unknown, we investigated the metabolism of 1 in liver microsomes of rat, bovine, porcine, and human origin using HPLC-DAD and LC-ESI-MS/MS and derived kinetic data on the metabolite formation. The main metabolic pathway was the side-chain hydroxylation leading to (E)-3'-hydroxyasarone (2). Epoxidation of 1 presumably led to (E)-asarone-1',2'-epoxide (4) which instantly hydrolyzed to form erythro- and threo-configured diols (5b+5a). As a minor reaction O-demethylation of 1 was observed. The metabolite formation showed little species-specific differences with the exception of porcine liver microsomes for which the formation of diols 5b+5a exceeded the formation of alcohol 2. The kinetic parameters imply a dependence of the pattern of metabolite formation from substrate concentration. On the basis of our results and earlier findings we hypothesize the genotoxic epoxide 4 being the ultimate carcinogen metabolically formed from 1.

摘要

α-细辛脑(1)是一种天然存在的苯丙烯,存在于多种植物中,如菖蒲。含有1的植物材料及其精油用于食品调味和许多植物药中。1据称具有积极的药理作用,然而,它在雄性小鼠(肝脏)中具有致癌性,并且可能具有遗传毒性。由于尚未研究1的代谢途径,其致癌作用模式也未知,我们使用HPLC-DAD和LC-ESI-MS/MS研究了1在大鼠、牛、猪和人源肝脏微粒体中的代谢,并得出了代谢物形成的动力学数据。主要代谢途径是侧链羟基化生成(E)-3'-羟基细辛脑(2)。1的环氧化可能导致(E)-细辛脑-1',2'-环氧化物(4),其立即水解形成赤式和苏式构型的二醇(5b+5a)。作为次要反应,观察到了1的O-去甲基化。除猪肝微粒体外,代谢物的形成几乎没有物种特异性差异,对于猪肝微粒体,二醇5b+5a的形成超过了醇2的形成。动力学参数表明代谢物形成模式取决于底物浓度。根据我们的结果和早期发现,我们假设遗传毒性环氧化物4是由1代谢形成的最终致癌物。

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