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含有α4亚基的GABA(A)受体:原位的发生率、分布、药理学及亚基结构

GABA(A) receptors containing the alpha4-subunit: prevalence, distribution, pharmacology, and subunit architecture in situ.

作者信息

Benke D, Michel C, Mohler H

机构信息

Institute of Pharmacology, ETH and University of Zurich, Switzerland.

出版信息

J Neurochem. 1997 Aug;69(2):806-14. doi: 10.1046/j.1471-4159.1997.69020806.x.

Abstract

Recombinant GABA(A) receptors, expressed from alpha-, beta-, and gamma2-subunits, are diazepam-insensitive when the alpha-subunit is either alpha4 or alpha6. In situ, diazepam-insensitive receptors containing the alpha6-subunit are almost exclusively expressed in the granule cell layer of the cerebellum. However, diazepam-insensitive receptors are also expressed in forebrain areas. Here, we report on the presence of diazepam-insensitive GABA(A) receptors in various brain areas containing the alpha4-subunit. GABA(A) receptors immunoprecipitated with a newly developed alpha4-subunit-specific antiserum displayed a drug binding profile that was indistinguishable from those of alpha4beta2gamma2-recombinant receptors and diazepam-insensitive [3H]Ro 15-4513 binding sites in rat brain membranes. In addition, alpha4-subunit containing receptors and forebrain diazepam-insensitive receptors are present at comparably low abundance in rat brain and exhibit virtually identical patterns of distribution. Analysis of the subunit architecture of alpha4-subunit containing receptors revealed that the alpha4-subunit contributes to several receptor subtypes. Depending on the brain region, the alpha4-subunit can be coassembled with a second type of alpha-subunit variant being alpha1, alpha2, or alpha3. The data demonstrate that native receptors containing the alpha4-subunit are structurally heterogeneous, expressed at very low abundance in the brain, and display the drug binding profile of diazepam-insensitive [3H]Ro 15-4513 binding sites. Pharmacologically, these receptors may contribute to the actions of nonclassical ligands such as Ro 15-4513 and bretazenil.

摘要

由α、β和γ2亚基表达的重组GABA(A)受体,当α亚基为α4或α6时,对安定不敏感。在原位,含有α6亚基的对安定不敏感的受体几乎只在小脑颗粒细胞层表达。然而,对安定不敏感的受体也在前脑区域表达。在此,我们报告在含有α4亚基的各种脑区中存在对安定不敏感的GABA(A)受体。用新开发的α4亚基特异性抗血清免疫沉淀的GABA(A)受体显示出与大鼠脑膜中α4β2γ2重组受体和对安定不敏感的[3H]Ro 15-4513结合位点的药物结合谱无法区分的药物结合谱。此外,含有α4亚基的受体和前脑对安定不敏感的受体在大鼠脑中的丰度相当低,并且表现出几乎相同的分布模式。对含有α4亚基的受体的亚基结构分析表明,α4亚基有助于几种受体亚型的形成。根据脑区的不同,α4亚基可以与第二种类型的α亚基变体α1、α2或α3共同组装。数据表明,含有α4亚基的天然受体在结构上是异质的,在脑中以非常低的丰度表达,并显示出对安定不敏感的[3H]Ro 15-4513结合位点的药物结合谱。在药理学上,这些受体可能有助于非经典配体如Ro 15-4513和布雷替奈的作用。

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