Amin J, Weiss D S
Department of Physiology and Biophysics, University of South Florida College of Medicine, Tampa 33612-4799.
Nature. 1993 Dec 9;366(6455):565-9. doi: 10.1038/366565a0.
The predominant inhibitory neurotransmitter of the brain, GABA (gamma-aminobutyric acid), activates chloride-selective ion pores integral to the receptor complex. Subunits comprising the presumed hetero-pentameric GABA channel have been cloned, but little information is available on the domains important for activation. Rat wild-type or mutated alpha 1-, beta 2- and gamma 2-subunits (designated alpha, beta and gamma) were coexpressed in Xenopus oocytes and examined electrophysiologically. We report here the identification of two separate and homologous domains of the beta-subunit, each of which contributes a tyrosine and threonine essential for activation by GABA. Conservative substitution of each of these four amino acids dramatically decreased GABA channel sensitivity to activation by GABA and the GABA agonist muscimol. These substitutions, however, did not impair activation by the barbiturate pentobarbital, indicating these two different classes of agonists activate GABA channels through distinct mechanisms. We also present evidence suggesting that the two identified domains of the beta-subunit contribute a major component of the GABA receptor.
大脑中主要的抑制性神经递质γ-氨基丁酸(GABA)可激活受体复合物中不可或缺的氯离子选择性离子通道。构成假定的异源五聚体GABA通道的亚基已被克隆,但对于激活至关重要的结构域的信息却知之甚少。将大鼠野生型或突变型α1、β2和γ2亚基(分别命名为α、β和γ)在非洲爪蟾卵母细胞中共表达,并进行电生理学检测。我们在此报告β亚基中两个独立且同源的结构域的鉴定结果,每个结构域都含有一个对GABA激活至关重要的酪氨酸和苏氨酸。对这四个氨基酸中的每一个进行保守性替换,都会显著降低GABA通道对GABA及GABA激动剂蝇蕈醇激活的敏感性。然而,这些替换并不影响巴比妥类药物戊巴比妥的激活作用,这表明这两类不同的激动剂通过不同的机制激活GABA通道。我们还提供了证据表明,β亚基中鉴定出的这两个结构域构成了GABA受体的主要成分。