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UDP-糖基转移酶(UGT)超家族:新成员、新功能和新范式。

The UDP-Glycosyltransferase (UGT) Superfamily: New Members, New Functions, and Novel Paradigms.

机构信息

Department of Clinical Pharmacology and Flinders Centre for Innovation in Cancer, Flinders University College of Medicine and Public Health, Flinders Medical Centre , Bedford Park, South Australia , Australia.

出版信息

Physiol Rev. 2019 Apr 1;99(2):1153-1222. doi: 10.1152/physrev.00058.2017.

DOI:10.1152/physrev.00058.2017
PMID:30724669
Abstract

UDP-glycosyltransferases (UGTs) catalyze the covalent addition of sugars to a broad range of lipophilic molecules. This biotransformation plays a critical role in elimination of a broad range of exogenous chemicals and by-products of endogenous metabolism, and also controls the levels and distribution of many endogenous signaling molecules. In mammals, the superfamily comprises four families: UGT1, UGT2, UGT3, and UGT8. UGT1 and UGT2 enzymes have important roles in pharmacology and toxicology including contributing to interindividual differences in drug disposition as well as to cancer risk. These UGTs are highly expressed in organs of detoxification (e.g., liver, kidney, intestine) and can be induced by pathways that sense demand for detoxification and for modulation of endobiotic signaling molecules. The functions of the UGT3 and UGT8 family enzymes have only been characterized relatively recently; these enzymes show different UDP-sugar preferences to that of UGT1 and UGT2 enzymes, and to date, their contributions to drug metabolism appear to be relatively minor. This review summarizes and provides critical analysis of the current state of research into all four families of UGT enzymes. Key areas discussed include the roles of UGTs in drug metabolism, cancer risk, and regulation of signaling, as well as the transcriptional and posttranscriptional control of UGT expression and function. The latter part of this review provides an in-depth analysis of the known and predicted functions of UGT3 and UGT8 enzymes, focused on their likely roles in modulation of levels of endogenous signaling pathways.

摘要

UDP-糖基转移酶(UGTs)催化将糖共价连接到广泛的亲脂性分子上。这种生物转化在消除广泛的外源化学物质和内源性代谢产物方面起着关键作用,并且还控制许多内源性信号分子的水平和分布。在哺乳动物中,该超家族包括四个家族:UGT1、UGT2、UGT3 和 UGT8。UGT1 和 UGT2 酶在药理学和毒理学中具有重要作用,包括导致药物处置的个体差异以及癌症风险。这些 UGT 在解毒器官(如肝脏、肾脏、肠道)中高度表达,并且可以被感应解毒和内源性信号分子调节需求的途径诱导。UGT3 和 UGT8 家族酶的功能仅在最近才得到表征;这些酶对 UDP-糖的偏好与 UGT1 和 UGT2 酶不同,迄今为止,它们对药物代谢的贡献似乎相对较小。本综述总结并批判性分析了目前对所有四种 UGT 酶家族的研究现状。讨论的重点包括 UGT 在药物代谢、癌症风险和信号调节中的作用,以及 UGT 表达和功能的转录和转录后控制。本综述的后半部分对 UGT3 和 UGT8 酶的已知和预测功能进行了深入分析,重点是它们在调节内源性信号通路水平方面的可能作用。

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