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大鼠脑σ受体的克隆及功能特性研究

Cloning and functional characterization of a sigma receptor from rat brain.

作者信息

Seth P, Fei Y J, Li H W, Huang W, Leibach F H, Ganapathy V

机构信息

Department of Biochemistry and Molecular Biology, Medical College of Georgia, Augusta 30912-2100, USA.

出版信息

J Neurochem. 1998 Mar;70(3):922-31. doi: 10.1046/j.1471-4159.1998.70030922.x.

Abstract

We have cloned a sigma receptor from rat brain and established its functional identity using a heterologous expression system. The cloned cDNA (1,582 bp long) codes for a protein of 223 amino acids that possesses a single putative transmembrane domain. The amino acid sequence of the rat brain sigma receptor is highly homologous to that of the sigma receptor recently cloned from guinea pig liver and a human placental cell line but is not related to any other known mammalian receptors. When expressed in HeLa cells, the rat brain sigma receptor cDNA leads to a two- to threefold increase in haloperidol binding, and this cDNA-induced binding is sensitive to inhibition by several sigma receptor-specific ligands. Kinetic analysis using the heterologous expression system has revealed that the rat brain sigma receptor interacts with haloperidol with an apparent dissociation constant (K(D)) of 3 nM. Functional expression of the cloned rat brain sigma receptor in HeLa cells also leads to an increase in the binding of two other sigma ligands, namely, (+)-pentazocine and (+)-3-(3-hydroxyphenyl)-N-(1-propyl)piperidine (PPP). Pharmacological characterization of the cloned rat brain sigma receptor reveals that it exhibits severalfold higher affinity for clorgyline than for 1 ,3-di(2-tolyl)guanidine, it interacts with progesterone and testosterone, and its interaction with PPP is markedly enhanced by phenytoin. In addition, transfection of MCF-7 cells, which do not express type 1 sigma receptor mRNA or activity, with the cloned rat brain cDNA leads to the appearance of haloperidol-sensitive binding of (+)-pentazocine, a selective type 1 sigma receptor ligand. These data show that the cloned rat brain cDNA codes for a functional type 1 sigma receptor. Northern blot analysis with poly(A)+ RNA isolated from various rat tissues has indicated that the sigma receptor-specific transcript, 1.6 kb in size, is expressed abundantly in liver and moderately in intestine, kidney, brain, and lung.

摘要

我们从大鼠脑中克隆了一种σ受体,并使用异源表达系统确定了其功能特性。克隆的cDNA(1582bp长)编码一个由223个氨基酸组成的蛋白质,该蛋白质具有一个单一的推定跨膜结构域。大鼠脑σ受体的氨基酸序列与最近从豚鼠肝脏和人胎盘细胞系克隆的σ受体高度同源,但与任何其他已知的哺乳动物受体无关。当在HeLa细胞中表达时,大鼠脑σ受体cDNA导致氟哌啶醇结合增加两到三倍,并且这种cDNA诱导的结合对几种σ受体特异性配体的抑制敏感。使用异源表达系统的动力学分析表明,大鼠脑σ受体与氟哌啶醇相互作用的表观解离常数(K(D))为3 nM。克隆的大鼠脑σ受体在HeLa细胞中的功能表达还导致另外两种σ配体,即(+)-喷他佐辛和(+)-3-(3-羟基苯基)-N-(1-丙基)哌啶(PPP)的结合增加。克隆的大鼠脑σ受体的药理学特性表明,它对氯吉灵的亲和力比对1,3-二(2-甲苯基)胍高几倍,它与孕酮和睾酮相互作用,并且苯妥英明显增强其与PPP的相互作用。此外,用克隆的大鼠脑cDNA转染不表达1型σ受体mRNA或活性的MCF-7细胞,导致选择性1型σ受体配体(+)-喷他佐辛出现对氟哌啶醇敏感的结合。这些数据表明,克隆的大鼠脑cDNA编码一种功能性1型σ受体。用从各种大鼠组织中分离的聚腺苷酸加尾RNA进行的Northern印迹分析表明,大小为1.6kb的σ受体特异性转录本在肝脏中大量表达,在肠道、肾脏、大脑和肺中中度表达。

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