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前列腺素途径中以花生四烯酸衍生的底物和产物与二十碳五烯酸衍生的底物和产物的酶和受体。

Enzymes and receptors of prostaglandin pathways with arachidonic acid-derived versus eicosapentaenoic acid-derived substrates and products.

作者信息

Wada Masayuki, DeLong Cynthia J, Hong Yu H, Rieke Caroline J, Song Inseok, Sidhu Ranjinder S, Yuan Chong, Warnock Mark, Schmaier Alvin H, Yokoyama Chieko, Smyth Emer M, Wilson Stephen J, FitzGerald Garret A, Garavito R Michael, Sui De Xin, Regan John W, Smith William L

机构信息

Department of Biological Chemistry, University of Michigan, Ann Arbor, Michigan 48109, USA.

出版信息

J Biol Chem. 2007 Aug 3;282(31):22254-66. doi: 10.1074/jbc.M703169200. Epub 2007 May 22.

DOI:10.1074/jbc.M703169200
PMID:17519235
Abstract

Dietary fish oil containing omega 3 highly unsaturated fatty acids has cardioprotective and anti-inflammatory effects. Prostaglandins (PGs) and thromboxanes are produced in vivo both from the omega 6 fatty acid arachidonic acid (AA) and the omega 3 fatty acid eicosapentaenoic acid (EPA). Certain beneficial effects of fish oil may result from altered PG metabolism resulting from increases in the EPA/AA ratios of precursor phospholipids. Here we report in vitro specificities of prostanoid enzymes and receptors toward EPA-derived, 3-series versus AA-derived, 2-series prostanoid substrates and products. The largest difference was seen with PG endoperoxide H synthase (PGHS)-1. Under optimal conditions purified PGHS-1 oxygenates EPA with only 10% of the efficiency of AA, and EPA significantly inhibits AA oxygenation by PGHS-1. Two- to 3-fold higher activities or potencies with 2-series versus 3-series compounds were observed with PGHS-2, PGD synthases, microsomal PGE synthase-1 and EP1, EP2, EP3, and FP receptors. Our most surprising observation was that AA oxygenation by PGHS-2 is only modestly inhibited by EPA (i.e. PGHS-2 exhibits a marked preference for AA when EPA and AA are tested together). Also unexpectedly, TxA(3) is about equipotent to TxA(2) at the TP alpha receptor. Our biochemical data predict that increasing phospholipid EPA/AA ratios in cells would dampen prostanoid signaling with the largest effects being on PGHS-1 pathways involving PGD, PGE, and PGF. Production of 2-series prostanoids from AA by PGHS-2 would be expected to decrease in proportion to the compensatory decrease in the AA content of phospholipids that would result from increased incorporation of omega 3 fatty acids such as EPA.

摘要

富含ω-3高度不饱和脂肪酸的膳食鱼油具有心脏保护和抗炎作用。前列腺素(PGs)和血栓素在体内可由ω-6脂肪酸花生四烯酸(AA)和ω-3脂肪酸二十碳五烯酸(EPA)产生。鱼油的某些有益作用可能源于前体磷脂中EPA/AA比值增加导致的PG代谢改变。在此,我们报告了类前列腺素酶和受体对EPA衍生的3-系列与AA衍生的2-系列类前列腺素底物及产物的体外特异性。PG内过氧化物H合酶(PGHS)-1的差异最为显著。在最佳条件下,纯化的PGHS-1氧化EPA的效率仅为AA的10%,且EPA可显著抑制PGHS-1对AA的氧化。与3-系列化合物相比,PGHS-2、PGD合酶、微粒体PGE合酶-1以及EP1、EP2、EP3和FP受体对2-系列化合物的活性或效力高2至3倍。我们最令人惊讶的发现是,PGHS-2对AA的氧化仅受到EPA的适度抑制(即当同时检测EPA和AA时,PGHS-2对AA表现出明显的偏好)。同样出乎意料的是,TxA(3)在TPα受体上与TxA(2)的效力相当。我们的生化数据预测,细胞中磷脂EPA/AA比值的增加会减弱类前列腺素信号传导,其中对涉及PGD、PGE和PGF的PGHS-1途径影响最大。由于ω-3脂肪酸(如EPA)掺入增加导致磷脂中AA含量代偿性减少,预计PGHS-2由AA产生的2-系列类前列腺素产量将相应降低。

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