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位于小鼠13号染色体上的一组八个属于醛酮还原酶超基因家族的羟基类固醇脱氢酶基因。

A cluster of eight hydroxysteroid dehydrogenase genes belonging to the aldo-keto reductase supergene family on mouse chromosome 13.

作者信息

Vergnes Laurent, Phan Jack, Stolz Andrew, Reue Karen

机构信息

Department of Human Genetics and Medicine, David Geffen School of Medicine at UCLA, Los Angeles, CA 90095, USA.

出版信息

J Lipid Res. 2003 Mar;44(3):503-11. doi: 10.1194/jlr.M200399-JLR200. Epub 2002 Dec 1.

Abstract

A subclass of hydroxysteroid dehydrogenases (HSD) are NADP(H)-dependent oxidoreductases that belong to the aldo-keto reductase (AKR) superfamily. They are involved in prereceptor or intracrine steroid modulation, and also act as bile acid-binding proteins. The HSD family members characterized thus far in human and rat have a high degree of protein sequence similarity but exhibit distinct substrate specificity. Here we report the identification of nine murine AKR genes in a cluster on chromosome 13 by a combination of molecular cloning and in silico analysis of this region. These include four previously isolated mouse HSD genes (Akr1c18, Akr1c6, Akr1c12, Akr1c13), the more distantly related Akr1e1, and four novel HSD genes. These genes exhibit highly conserved exon/intron organization and protein sequence predictions indicate 75% amino acid similarity. The previously identified AKR protein active site residues are invariant among all nine proteins, but differences are observed in regions that have been implicated in determining substrate specificity. Differences also occur in tissue expression patterns, with expression of some genes restricted to specific tissues and others expressed at high levels in multiple tissues. Our findings dramatically expand the repertoire of AKR genes and identify unrecognized family members with potential roles in the regulation of steroid metabolism.

摘要

羟类固醇脱氢酶(HSD)的一个亚类是依赖烟酰胺腺嘌呤二核苷酸磷酸(NADP(H))的氧化还原酶,属于醛糖酮还原酶(AKR)超家族。它们参与受体前或内分泌类固醇调节,还可作为胆汁酸结合蛋白。迄今为止,在人和大鼠中鉴定出的HSD家族成员具有高度的蛋白质序列相似性,但表现出不同的底物特异性。在此,我们报告通过对该区域进行分子克隆和计算机分析相结合的方法,在13号染色体上的一个基因簇中鉴定出9个小鼠AKR基因。其中包括4个先前分离出的小鼠HSD基因(Akr1c18、Akr1c6、Akr1c12、Akr1c13)、亲缘关系较远的Akr1e1以及4个新的HSD基因。这些基因表现出高度保守的外显子/内含子结构,蛋白质序列预测显示氨基酸相似性为75%。在所有9种蛋白质中,先前鉴定出的AKR蛋白质活性位点残基是不变的,但在与底物特异性决定相关的区域观察到差异。组织表达模式也存在差异,一些基因的表达仅限于特定组织,而其他基因在多个组织中高表达。我们的研究结果极大地扩展了AKR基因库,并鉴定出在类固醇代谢调节中可能发挥潜在作用的未被认识的家族成员。

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