甲氧氯普胺由CYP2D6代谢,是一种可逆性抑制剂而非灭活剂,可抑制CYP2D6。
Metoclopramide is metabolized by CYP2D6 and is a reversible inhibitor, but not inactivator, of CYP2D6.
作者信息
Livezey Mara R, Briggs Erran D, Bolles Amanda K, Nagy Leslie D, Fujiwara Rina, Furge Laura Lowe
机构信息
Department of Chemistry, Kalamazoo College, Kalamazoo, MI 49006 USA.
出版信息
Xenobiotica. 2014 Apr;44(4):309-319. doi: 10.3109/00498254.2013.835885. Epub 2013 Sep 6.
Abstract
- Metoclopramide is a widely used clinical drug in a variety of medical settings with rare acute dystonic events reported. The aim of this study was to assess a previous report of inactivation of CYP2D6 by metoclopramide, to determine the contribution of various CYPs to metoclopramide metabolism, and to identify the mono-oxygenated products of metoclopramide metabolism. 2. Metoclopramide interacted with CYP2D6 with Type I binding and a Ks value of 9.56 ± 1.09 µM. CYP2D6 was the major metabolizer of metoclopramide and the two major products were N-deethylation of the diethyl amine and N-hydroxylation on the phenyl ring amine. CYPs 1A2, 2C9, 2C19, and 3A4 also metabolized metoclopramide. 3. While reversible inhibition of CYP2D6 was noted, CYP2D6 inactivation by metoclopramide was not observed under conditions of varying concentration or varying time using Supersomes(TM) or pooled human liver microsomes. 4. The major metabolites of metoclopramide were N-hydroxylation and N-deethylation formed most efficiently by CYP2D6 but also formed by all CYPs examined. Also, while metoclopramide is metabolized primarily by CYP2D6, it is not a mechanism-based inactivator of CYP2D6 in vitro.
摘要
- 甲氧氯普胺是一种在多种医疗环境中广泛使用的临床药物,报告的急性肌张力障碍事件罕见。本研究的目的是评估先前关于甲氧氯普胺使CYP2D6失活的报告,确定各种细胞色素P450(CYPs)对甲氧氯普胺代谢的贡献,并鉴定甲氧氯普胺代谢的单加氧产物。2. 甲氧氯普胺与CYP2D6以I型结合相互作用,Ks值为9.56±1.09µM。CYP2D6是甲氧氯普胺的主要代谢酶,两种主要产物是二乙胺的N-去乙基化和苯环胺上的N-羟基化。CYPs 1A2、2C9、2C19和3A4也代谢甲氧氯普胺。3. 虽然注意到CYP2D6的可逆抑制,但在使用超微粒体(Supersomes(TM))或人肝微粒体池的不同浓度或不同时间条件下,未观察到甲氧氯普胺使CYP2D6失活。4. 甲氧氯普胺的主要代谢产物是N-羟基化和N-去乙基化,最有效地由CYP2D6形成,但所有检测的CYPs也能形成。此外,虽然甲氧氯普胺主要由CYP2D6代谢,但在体外它不是CYP2D6的基于机制的失活剂。
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