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大鼠α6β2δ GABAA受体表现出两种不同且可分离的激动剂亲和力。

Rat alpha6beta2delta GABAA receptors exhibit two distinct and separable agonist affinities.

作者信息

Hadley Stephen H, Amin Jahanshah

机构信息

Department of Molecular Pharmacology and Physiology, College of Medicine, University of South Florida, Tampa, FL 33612, USA.

出版信息

J Physiol. 2007 Jun 15;581(Pt 3):1001-18. doi: 10.1113/jphysiol.2007.132886. Epub 2007 Mar 29.

Abstract

The onset of motor learning in rats coincides with exclusive expression of GABAA receptors containing alpha6 and delta subunits in the granule neurons of the cerebellum. This development temporally correlates with the presence of a spontaneously active chloride current through alpha6-containing GABAA receptors, known as tonic inhibition. Here we report that the coexpression of alpha6, beta2, and delta subunits produced receptor-channels which possessed two distinct and separable states of agonist affinity, one exhibiting micromolar and the other nanomolar affinities for GABA. The high-affinity state was associated with a significant level of spontaneous channel activity. Increasing the level of expression or the ratio of beta2 to alpha6 and delta subunits increased the prevalence of the high-affinity state. Comparative studies of alpha6beta2delta, alpha1beta2delta, alpha6beta2gamma2, alpha1beta2gamma2 and alpha4beta2delta receptors under equivalent levels of expression demonstrated that the significant level of spontaneous channel activity is uniquely attributable to alpha6beta2delta receptors. The pharmacology of spontaneous channel activity arising from alpha6beta2delta receptor expression corresponded to that of tonic inhibition. For example, GABAA receptor antagonists, including furosemide, blocked the spontaneous current. Further, the neuroactive steroid 5alpha-THDOC and classical glycine receptor agonists beta-alanine and taurine directly activated alpha6beta2delta receptors with high potency. Specific mutation within the GABA-dependent activation domain (betaY157F) impaired both low- and high-affinity components of GABA agonist activity in alpha6betaY157Fdelta receptors, but did not attenuate the spontaneous current. In comparison, a mutation located between the second and third transmembrane segments of the delta subunit (deltaR287M) significantly diminished the nanomolar component and the spontaneous activity. The possibility that the high affinity state of the alpha6beta2delta receptor modulates the granule neuron activity as well as potential mechanisms affecting its expression are discussed.

摘要

大鼠运动学习的开始与小脑颗粒神经元中含有α6和δ亚基的GABAA受体的特异性表达相吻合。这一发育过程在时间上与通过含α6的GABAA受体的自发激活氯离子电流(即张力性抑制)的存在相关。在此,我们报告α6、β2和δ亚基的共表达产生了受体通道,该通道具有两种不同且可分离的激动剂亲和力状态,一种对GABA表现出微摩尔亲和力,另一种表现出纳摩尔亲和力。高亲和力状态与显著水平的自发通道活性相关。增加β2与α6和δ亚基的表达水平或比例会增加高亲和力状态的发生率。在同等表达水平下对α6β2δ、α1β2δ、α6β2γ2、α1β2γ2和α4β2δ受体进行的比较研究表明,显著水平的自发通道活性唯一地归因于α6β2δ受体。由α6β2δ受体表达产生的自发通道活性的药理学与张力性抑制的药理学相对应。例如,包括速尿在内的GABAA受体拮抗剂可阻断自发电流。此外,神经活性类固醇5α-四氢脱氧皮质酮以及经典的甘氨酸受体激动剂β-丙氨酸和牛磺酸可高效直接激活α6β2δ受体。GABA依赖性激活结构域内的特异性突变(βY157F)损害了α6βY157Fδ受体中GABA激动剂活性的低亲和力和高亲和力成分,但并未减弱自发电流。相比之下,位于δ亚基的第二和第三跨膜段之间的突变(δR287M)显著降低了纳摩尔成分和自发活性。讨论了α6β2δ受体的高亲和力状态调节颗粒神经元活性的可能性以及影响其表达的潜在机制。

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