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小鼠和人胆固醇25-羟化酶的cDNA克隆,这两种多结构域膜蛋白可合成一种强效的脂质代谢氧甾醇调节剂。

cDNA cloning of mouse and human cholesterol 25-hydroxylases, polytopic membrane proteins that synthesize a potent oxysterol regulator of lipid metabolism.

作者信息

Lund E G, Kerr T A, Sakai J, Li W P, Russell D W

机构信息

Department of Molecular Genetics, University of Texas Southwestern Medical Center, Dallas, Texas 75235-9046, USA.

出版信息

J Biol Chem. 1998 Dec 18;273(51):34316-27. doi: 10.1074/jbc.273.51.34316.

Abstract

Oxysterols regulate the expression of genes involved in cholesterol and lipid metabolism and serve as intermediates in cholesterol catabolism. Among the most potent of regulatory oxysterols is 25-hydroxycholesterol, whose biosynthetic enzyme has not yet been isolated. Here, we report the cloning of cholesterol 25-hydroxylase cDNAs from the mouse and human. The encoded enzymes are polytopic membrane proteins of 298 and 272 amino acids, respectively, which contain clusters of histidine residues that are essential for catalytic activity. Unlike most other sterol hydroxylases, cholesterol 25-hydroxylase is not a cytochrome P450, but rather it is a member of a small family of enzymes that utilize diiron cofactors to catalyze the hydroxylation of hydrophobic substrates. The cholesterol 25-hydroxylase gene lacks introns, and in the human it is located on chromosome 10q23. The murine gene is expressed at low levels in multiple tissues. Expression of cholesterol 25-hydroxylase in transfected cells reduces the biosynthesis of cholesterol from acetate and suppresses the cleavage of sterol regulatory element binding protein-1 and -2. The data suggest that cholesterol 25-hydroxylase has the capacity to play an important role in regulating lipid metabolism by synthesizing a co-repressor that blocks sterol regulatory element binding protein processing and ultimately leads to inhibition of gene transcription.

摘要

氧化甾醇可调节参与胆固醇和脂质代谢的基因表达,并作为胆固醇分解代谢的中间体。在最具活性的调节性氧化甾醇中,25-羟基胆固醇最为突出,其生物合成酶尚未分离出来。在此,我们报告从小鼠和人类中克隆胆固醇25-羟化酶cDNA。所编码的酶分别是由298和272个氨基酸组成的多跨膜蛋白,它们含有对催化活性至关重要的组氨酸残基簇。与大多数其他甾醇羟化酶不同,胆固醇25-羟化酶不是细胞色素P450,而是利用双铁辅因子催化疏水底物羟基化的一小类酶家族的成员。胆固醇25-羟化酶基因不含内含子,在人类中它位于10q23染色体上。小鼠基因在多个组织中低水平表达。在转染细胞中胆固醇25-羟化酶的表达可减少乙酸盐合成胆固醇,并抑制甾醇调节元件结合蛋白-1和-2的裂解。数据表明,胆固醇25-羟化酶有能力通过合成一种共抑制因子来调节脂质代谢,该共抑制因子可阻断甾醇调节元件结合蛋白的加工过程,并最终导致基因转录的抑制。

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