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对氧代白藜芦醇(一种天然的羟基二苯乙烯)的区域选择性葡萄糖醛酸化作用,由人肝和肠微粒体及重组 UGTs 介导。

Regioselective glucuronidation of oxyresveratrol, a natural hydroxystilbene, by human liver and intestinal microsomes and recombinant UGTs.

机构信息

State Key Laboratory of Quality Research in Chinese Medicine, Institute of Chinese Medical Sciences, University of Macau.

出版信息

Drug Metab Pharmacokinet. 2014;29(3):229-36. doi: 10.2133/dmpk.dmpk-13-rg-102. Epub 2013 Nov 19.

Abstract

Oxyresveratrol (OXY) is a natural hydroxystilbene that shows similar bioactivity but better water solubility than resveratrol. This study aims to characterize its glucuronidation kinetics in human liver (HLMs) and intestinal (HIMs) microsomes and identify the main UDP-glucuronosyltransferase (UGT) isoforms involved. Three and four mono-glucuronides of OXY were generated in HIMs and HLMs, respectively, with oxyresveratrol-2-O-β-D-glucuronosyl (G4) as the major metabolite in both organs. The kinetics of G4 formation fit a sigmoidal model in HLMs and biphasic kinetics in HIMs. Multiple UGT isoforms catalyzed G4 formation with the highest activity observed with UGT1A9 followed by UGT1A1. G4 formation by both isoforms followed substrate inhibition kinetics. Propofol (UGT1A9 inhibitor) effectively blocked G4 generation in HLMs (IC50 63.7 ± 11.6 µM), whereas the UGT1A1 inhibitor bilirubin only produced partial inhibition in HLMs and HIMs. These findings shed light on the metabolic mechanism of OXY and arouse awareness of drug interactions.

摘要

氧代白藜芦醇(OXY)是一种天然的羟基二苯乙烯,其生物活性与白藜芦醇相似,但水溶性更好。本研究旨在研究其在人肝(HLMs)和肠(HIMs)微粒体中的葡萄糖醛酸化动力学,并鉴定主要涉及的 UDP-葡萄糖醛酸基转移酶(UGT)同工酶。在 HIMs 和 HLMs 中分别生成了三种和四种 OXY 的单葡萄糖醛酸化物,其中 oxyresveratrol-2-O-β-D-glucuronosyl(G4)是两种器官中的主要代谢物。G4 形成的动力学在 HLMs 中符合 S 型模型,在 HIMs 中呈双相动力学。多个 UGT 同工酶催化 G4 的形成,其中 UGT1A9 的活性最高,其次是 UGT1A1。两种同工酶的 G4 形成均遵循底物抑制动力学。丙泊酚(UGT1A9 抑制剂)可有效阻断 HLMs 中 G4 的生成(IC50 为 63.7±11.6µM),而 UGT1A1 抑制剂胆红素仅在 HLMs 和 HIMs 中产生部分抑制。这些发现阐明了 OXY 的代谢机制,并引起了对药物相互作用的关注。

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