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一种新型GABAA受体亚基对苯二氮䓬药理学的重要性。

Importance of a novel GABAA receptor subunit for benzodiazepine pharmacology.

作者信息

Pritchett D B, Sontheimer H, Shivers B D, Ymer S, Kettenmann H, Schofield P R, Seeburg P H

机构信息

ZMBH, Universität Heidelberg, FRG.

出版信息

Nature. 1989 Apr 13;338(6216):582-5. doi: 10.1038/338582a0.

Abstract

Neurotransmission effected by GABA (gamma-aminobutyric acid) is predominantly mediated by a gated chloride channel intrinsic to the GABAA receptor. This heterooligomeric receptor exists in most inhibitory synapses in the vertebrate central nervous system (CNS) and can be regulated by clinically important compounds such as benzodiazepines and barbiturates. The primary structures of GABAA receptor alpha- and beta-subunits have been deduced from cloned complementary DNAs. Co-expression of these subunits in heterologous systems generates receptors which display much of the pharmacology of their neural counterparts, including potentiation by barbiturates. Conspicuously, however, they lack binding sites for, and consistent electrophysiological responses to, benzodiazepines. We now report the isolation of a cloned cDNA encoding a new GABAA receptor subunit, termed gamma 2, which shares approximately 40% sequence identity with alpha- and beta-subunits and whose messenger RNA is prominently localized in neuronal subpopulations throughout the CNS. Importantly, coexpression of the gamma 2 subunit with alpha 1 and beta 1 subunits produces GABAA receptors displaying high-affinity binding for central benzodiazepine receptor ligands.

摘要

由γ-氨基丁酸(GABA)介导的神经传递主要由GABAA受体固有的门控氯离子通道介导。这种异源寡聚体受体存在于脊椎动物中枢神经系统(CNS)的大多数抑制性突触中,并且可受临床上重要的化合物如苯二氮䓬类和巴比妥类药物的调节。GABAA受体α和β亚基的一级结构已从克隆的互补DNA中推导出来。在异源系统中共同表达这些亚基会产生具有其神经对应物许多药理学特性的受体,包括巴比妥类药物的增强作用。然而,明显的是,它们缺乏苯二氮䓬类药物的结合位点以及对其一致的电生理反应。我们现在报告分离出一种克隆的cDNA,其编码一种新的GABAA受体亚基,称为γ2,它与α和β亚基具有约40%的序列同一性,并且其信使RNA在整个CNS的神经元亚群中显著定位。重要的是,γ2亚基与α1和β1亚基的共表达产生了对中枢苯二氮䓬受体配体具有高亲和力结合的GABAA受体。

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