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小脑颗粒神经元自突触处的NMDA受体亚型

NMDA receptor subtypes at autaptic synapses of cerebellar granule neurons.

作者信息

Lu Congyi, Fu Zhanyan, Karavanov Irina, Yasuda Robert P, Wolfe Barry B, Buonanno Andres, Vicini Stefano

机构信息

Department of Physiology and Biophysics, BSB225, Georgetown University School of Medicine, 3900 Reservoir Rd., Washington, DC 20007, USA.

出版信息

J Neurophysiol. 2006 Nov;96(5):2282-94. doi: 10.1152/jn.00078.2006. Epub 2006 Aug 2.

Abstract

We studied the action potential-evoked autaptic N-methyl-d-aspartate receptor-mediated excitatory postsynaptic currents (NMDA-EPSCs) using solitary cerebellar neurons cultured in microislands from wild-type (+/+), NR2A subunit knockout (NR2A-/-), and NR2C subunit knockout (NR2C-/-) mice. The peak amplitude of autaptic NMDA-EPSCs increased for all genotypes between days in vitro 8 (DIV8) and DIV13. Compared with +/+ cells at DIV13, NR2A-/- cells had smaller and NR2C-/- cells had larger NMDA-EPSCs. The decay time of these currents were all unexpectedly fast, except in NR2A-/- neurons, and showed small but significant shortening with development. Comparison of quantal parameters during development indicated an increase in quantal content in all genotypes. The synaptic portion of NMDA receptors measured using MK-801 blockade was roughly 50% in all genotypes at DIV8, and this percentage became slightly larger in NR2A-/- and NR2C-/- neurons at DIV12. The NR2B-selective antagonists Conantokin G and CP101,606 differed in their blocking actions with development, suggesting the presence of both heterodimeric NR1/NR2B and heterotrimeric NR1/NR2A/NR2B receptors. The most striking result we obtained was the significant increase of NMDA-EPSC peak amplitude and charge transfer in NR2C-/- mice. This was mainly the result of an increase in quantal size as estimated from miniature NMDA-EPSCs. The expression of NR2C subunit containing receptors was supported by the decreased Mg(2+) sensitivity of NMDA receptors at DIV13 in +/+ but not in NR2C-/- cells. Thus solitary cerebellar granule neurons provide a novel model to investigate the role of receptor subtypes in the developmental changes of synaptic NMDA receptors.

摘要

我们使用从野生型(+/+)、NR2A亚基敲除(NR2A-/-)和NR2C亚基敲除(NR2C-/-)小鼠的微岛中培养的孤立小脑神经元,研究了动作电位诱发的自突触N-甲基-D-天冬氨酸受体介导的兴奋性突触后电流(NMDA-EPSCs)。在体外培养第8天(DIV8)至DIV13期间,所有基因型的自突触NMDA-EPSCs的峰值幅度均增加。与DIV13时的+/+细胞相比,NR2A-/-细胞的NMDA-EPSCs较小,而NR2C-/-细胞的NMDA-EPSCs较大。除了NR2A-/-神经元外,这些电流的衰减时间都出乎意料地快,并且随着发育呈现出轻微但显著的缩短。发育过程中量子参数的比较表明,所有基因型的量子含量都有所增加。在DIV8时,使用MK-801阻断测量的NMDA受体的突触部分在所有基因型中约为50%,在DIV12时,NR2A-/-和NR2C-/-神经元中的这一百分比略有增加。NR2B选择性拮抗剂芋螺毒素G和CP101,606的阻断作用随发育而不同,表明存在异二聚体NR1/NR2B和异三聚体NR1/NR2A/NR2B受体。我们获得的最显著结果是NR2C-/-小鼠中NMDA-EPSC峰值幅度和电荷转移的显著增加。这主要是由微小NMDA-EPSCs估计的量子大小增加的结果。在DIV13时,+/+细胞而非NR2C-/-细胞中NMDA受体对Mg(2+)的敏感性降低,支持了含NR2C亚基受体的表达。因此,孤立的小脑颗粒神经元为研究受体亚型在突触NMDA受体发育变化中的作用提供了一个新模型。

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