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培养的大鼠视网膜神经节细胞中钙离子通透的P2X受体通道

Ca2+-permeable P2X receptor channels in cultured rat retinal ganglion cells.

作者信息

Taschenberger H, Jüttner R, Grantyn R

机构信息

Developmental Physiology, Institute for Physiology, Humboldt University Medical School (Charité), D-10117 Berlin, Germany.

出版信息

J Neurosci. 1999 May 1;19(9):3353-66. doi: 10.1523/JNEUROSCI.19-09-03353.1999.

Abstract

ATP has been identified as an excitatory neurotransmitter in both the CNS and peripheral nervous system; however, little is known about the functional properties of ATP-gated channels in central neurons. Here we used a culture preparation of the postnatal rat retina to test the responsiveness of identified retinal ganglion cells (RGCs) and putative amacrines to exogenous ATP and other purinoceptor agonists. Rapidly activating ATP-induced currents (IATP) were exclusively generated in a subpopulation (approximately 65%) of RGCs. The latter were identified by Thy1.1 immunostaining, repetitive firing patterns, and activation of glutamatergic autaptic currents. None of the putative amacrine cells was ATP-sensitive. IATP could be induced with ATP, ADP, and alpha,beta-mATP but not with adenosine. It was antagonized by suramin. The current-voltage relationship of IATP showed marked inward rectification. Dose-response analysis yielded an EC50 of 14.5 microM, with a Hill coefficient of 0.9. Noise analysis of IATP suggested a mean single channel conductance of 2.3 pS. Retinal P2X purinoceptor channels exhibited a high permeability for Ca2+. PCa/PCs obtained from reversal potentials of IATP under bi-ionic conditions amounted to 2. 2 +/- 0.7. In the majority of cells, the decay of IATP was biphasic. The degree of current inactivation during the first 2 sec of agonist application was highly variable. Heterogeneity was also found with respect to the sensitivity to ADP and alpha,beta-mATP and the blocking action of suramin, suggesting expression of multiple P2X receptor subtypes. Our results indicate that activation of P2X receptor channels represents an important pathway for Ca2+ influx in postnatal RGCs.

摘要

ATP已被确定为中枢神经系统和外周神经系统中的一种兴奋性神经递质;然而,关于中枢神经元中ATP门控通道的功能特性却知之甚少。在这里,我们使用新生大鼠视网膜的培养制剂来测试已鉴定的视网膜神经节细胞(RGCs)和假定的无长突细胞对外源性ATP和其他嘌呤受体激动剂的反应性。快速激活的ATP诱导电流(IATP)仅在一部分(约65%)的RGCs中产生。后者通过Thy1.1免疫染色、重复放电模式和谷氨酸能自突触电流的激活来鉴定。所有假定的无长突细胞对ATP均不敏感。IATP可由ATP、ADP和α,β-甲基ATP诱导产生,但不能由腺苷诱导产生。它可被苏拉明拮抗。IATP的电流-电压关系表现出明显的内向整流。剂量反应分析得出EC50为14.5微摩尔,希尔系数为0.9。IATP的噪声分析表明平均单通道电导为2.3皮西门子。视网膜P2X嘌呤受体通道对Ca2+具有高通透性。在双离子条件下,从IATP的反转电位获得的PCa/PCs为2.2±0.7。在大多数细胞中,IATP的衰减是双相的。在激动剂应用的前2秒内电流失活的程度变化很大。在对ADP和α,β-甲基ATP的敏感性以及苏拉明的阻断作用方面也发现了异质性,这表明存在多种P2X受体亚型的表达。我们的结果表明,P2X受体通道的激活代表了新生RGCs中Ca2+内流的一条重要途径。

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