化学
毒性
细胞毒性
CYP3A型
药理学
新陈代谢
急性毒性
诱导剂
代谢途径
去甲基化
生物化学
细胞色素P450
体外
生物
基因表达
DNA甲基化
有机化学
基因
作者
Wei Zhang,Kun Ren,Shuangfeng Wu,Jing-yan Guo,Shumeng Ren,Yingni Pan,Dongmei Wang,Toshio Morikawa,Huiming Hua,Xiaoqiu Liu
标识
DOI:10.1016/j.jchromb.2021.123040
摘要
Euodiae Fructus (EF), the dried unripe scented fruit of Euodia rutaecarpa (Juss.) Benth., was reported to show anti-hypertensive, antitumor, and anti-obesity effects. The main alkaloids of EF were reported as the reason for toxicity of EF by metabolic activation majority through CYP3A. Up till the present moment, the cytotoxicity mechanisms of EF have not yet to be fully clarified. For the purposes of this article, the influence of CYP3A inducer and inhibitor on cytotoxicity of EF and metabolism in L02 cells of five alkaloids related to toxicity of EF were evaluated. The results indicated that CYP3A inducer aggravated the toxicity and CYP3A inhibitor alleviated the toxicity. UPLC-Q-Exactive-MS was used for the identification of five alkaloids of EF in L02 cells. A total of 13 metabolites were detected in L02 cells. In general, five alkaloids were widely metabolized in L02 cells such as oxygenation, demethylation, dehydrogenation, and etc. In addition, oxygenation was the main metabolic pathway. It was inferred that the toxicity of EF was closely related to the CYP3A and the metabolic intermediate might be one of the reasons for the toxicity of EF. Hence, the choice of optimal dose might be critical to avoid the adverse reactions owing to combination of EF and CYP3A inducer.
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