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Enzymes and Pathways of Kavain Bioactivation and Biotransformation.

Pengcheng Wang, Junjie Zhu, Amina I Shehu, Jie Lu, Jing Chen et al.
Other Chemical research in toxicology 2019 6 次引用
PubMed DOI
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Study Design

研究类型
In Vitro
研究人群
None
干预措施
Enzymes and Pathways of Kavain Bioactivation and Biotransformation. None
对照组
None
主要结局
None
效应方向
Mixed
偏倚风险
Unclear

Abstract

Kavain is an active and major component in Piper methysticum Forst. (kava), which is a widely used dietary supplement for the treatment of anxiety, insomnia, and stress. However, kava-containing products can cause liver toxicity, and its underlying mechanisms are understudied. Cytochrome P450s (CYPs)-mediated bioactivation and biotransformation are highly associated with drug toxicity. In the current study, we profiled the metabolic pathways of kavain in mouse liver, urine, and feces. Overall, 28 kavain metabolites were identified including 17 new ones. The metabolic pathways of kavain include glutathione (GSH) conjugation, oxidation, dehydrogenation, O-demethylation, sulfation, and glucuronidation. The identification of kavain-GSH adducts suggests the formation of reactive metabolites of kavain in the liver. We further illustrated that CYP2C19, a highly polymorphic and inducible enzyme, was the major enzyme contributing to kavain biotransformation and bioactivation. Our data can be used to guide the safe use of kava products by preventing potential herb-drug interactions and hepatotoxicity.

简要概述

It is illustrated that CYP2C19, a highly polymorphic and inducible enzyme, was the major enzyme contributing to kavain biotransformation and bioactivation and can be used to guide the safe use of kava products by preventing potential herb-drug interactions and hepatotoxicity.

Used In Evidence Reviews

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