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前列腺素E合酶,一种前列腺素E2生物合成的末端酶。

Prostaglandin E synthase, a terminal enzyme for prostaglandin E2 biosynthesis.

作者信息

Kudo Ichiro, Murakami Makoto

机构信息

Department of Health Chemistry, School of Pharmaceutical Sciences, Showa University, 1-5-8 Hatanodai, Shinagawa-ku, Tokyo 142-8555, Japan.

出版信息

J Biochem Mol Biol. 2005 Nov 30;38(6):633-8. doi: 10.5483/bmbrep.2005.38.6.633.

DOI:10.5483/bmbrep.2005.38.6.633
PMID:16336776
Abstract

Biosynthesis of prostanoids is regulated by three sequential enzymatic steps, namely phospholipase A2 enzymes, cyclooxygenase (COX) enzymes, and various lineagespecific terminal prostanoid synthases. Prostaglandin E synthase (PGES), which isomerizes COX-derived PGH2 specifically to PGE2, occurs in multiple forms with distinct enzymatic properties, expressions, localizations and functions. Two of them are membrane-bound enzymes and have been designated as mPGES-1 and mPGES-2. mPGES-1 is a perinuclear protein that is markedly induced by proinflammatory stimuli, is down-regulated by antiinflammatory glucocorticoids, and is functionally coupled with COX-2 in marked preference to COX-1. Recent gene targeting studies of mPGES-1 have revealed that this enzyme represents a novel target for anti-inflammatory and anti-cancer drugs. mPGES-2 is synthesized as a Golgi membrane-associated protein, and the proteolytic removal of the N-terminal hydrophobic domain leads to the formation of a mature cytosolic enzyme. This enzyme is rather constitutively expressed in various cells and tissues and is functionally coupled with both COX-1 and COX-2. Cytosolic PGES (cPGES) is constitutively expressed in a wide variety of cells and is functionally linked to COX-1 to promote immediate PGE2 production. This review highlights the latest understanding of the expression, regulation and functions of these three PGES enzymes.

摘要

类前列腺素的生物合成由三个连续的酶促步骤调控,即磷脂酶A2、环氧化酶(COX)以及各种谱系特异性的末端类前列腺素合酶。前列腺素E合酶(PGES)可将COX衍生的PGH2特异性异构化为PGE2,它以多种形式存在,具有不同的酶学性质、表达、定位和功能。其中两种是膜结合酶,分别被命名为mPGES-1和mPGES-2。mPGES-1是一种核周蛋白,可被促炎刺激显著诱导,被抗炎糖皮质激素下调,并且在功能上与COX-2优先偶联,而非COX-1。最近针对mPGES-1的基因靶向研究表明,这种酶是抗炎和抗癌药物的新靶点。mPGES-2作为一种与高尔基体膜相关的蛋白合成,N端疏水结构域的蛋白水解去除导致成熟胞质酶的形成。这种酶在各种细胞和组织中相当组成性地表达,并且在功能上与COX-1和COX-2都偶联。胞质PGES(cPGES)在多种细胞中组成性表达,并且在功能上与COX-1相连以促进PGE2的即时产生。本综述重点介绍了对这三种PGES酶的表达、调控和功能的最新认识。

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