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γ-氨基丁酸(GABA)受体的三种亚型对大鼠暗适应视网膜电图成分的调节作用

Modulation of the components of the rat dark-adapted electroretinogram by the three subtypes of GABA receptors.

作者信息

Möller Anna, Eysteinsson Thor

机构信息

Department of Physiology, University of Iceland IS-101 Reykjavik, Iceland.

出版信息

Vis Neurosci. 2003 Sep-Oct;20(5):535-42. doi: 10.1017/s0952523803205071.

DOI:10.1017/s0952523803205071
PMID:14977332
Abstract

The separate components of the dark-adapted electroretinogram (ERG) are believed to reflect the electric activity of neurones in both the inner and the outer layers of the retina, although their precise origin still remains unclear. The purpose of this study was to examine whether selective blockage or stimulation of the different subtypes of GABA receptors might help further elucidate the cellular origin of the components of the dark-adapted ERG. The rat retina is of interest since the localization and physiology of GABA receptors in that retina have been examined in great detail. GABA agonists and antagonists, known to affect the responses of neurons in the inner plexiform layer, were injected into the vitreous of one eye while ERG responses evoked by flashes of white light were recorded. GABA and the GABAa agonist isoguvacine completely removed the oscillatory potentials (OPs) and reduced the amplitude of the a- and b-waves. TPMPA, a GABAC antagonist, reduced the a- and b-waves but had no significant effect on the OPs. Baclofen, a GABAb agonist, reduced the amplitude of the a- and b-waves, without having any effects on the amplitude of the OPs. The GABAb antagonist CGP35348 increased the amplitudes of the a- and b-wave without having an effect on the amplitudes of the OPs. The GABAb receptor ligands had significant and opposite effect on the latency of the OPs. These results indicate that retinal neurons, presumably a subpopulation of amacrine cells, that have GABAb receptors are not the source of the OPs of the ERG, although they may modulate these wavelets in some manner, while contributing to the generation of the dark-adapted a- and b-waves. OPs are modified by stimulation of GABAa receptors, and the a- and b-waves by stimulation of all GABA receptor subtypes.

摘要

暗适应视网膜电图(ERG)的各个组成部分被认为反映了视网膜内层和外层神经元的电活动,尽管它们的确切起源仍不清楚。本研究的目的是探讨选择性阻断或刺激不同亚型的GABA受体是否有助于进一步阐明暗适应ERG各组成部分的细胞起源。大鼠视网膜备受关注,因为该视网膜中GABA受体的定位和生理学已得到详细研究。已知影响内网状层神经元反应的GABA激动剂和拮抗剂被注入一只眼睛的玻璃体中,同时记录白光闪光诱发的ERG反应。GABA和GABAa激动剂异鹅肌肽完全消除了振荡电位(OPs)并降低了a波和b波的振幅。GABAC拮抗剂TPMPA降低a波和b波,但对OPs无显著影响。GABAb激动剂巴氯芬降低a波和b波的振幅,但对OPs的振幅无任何影响。GABAb拮抗剂CGP35348增加a波和b波的振幅,但对OPs的振幅无影响。GABAb受体配体对OPs的潜伏期有显著且相反的影响。这些结果表明,具有GABAb受体的视网膜神经元,可能是无长突细胞的一个亚群,不是ERG中OPs的来源,尽管它们可能以某种方式调节这些小波,同时参与暗适应a波和b波的产生。OPs通过刺激GABAa受体而改变,a波和b波则通过刺激所有GABA受体亚型而改变。

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