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首页> 外文期刊>Neuron >Cornichon2 Dictates the Time Course of Excitatory Transmission at Individual Hippocampal Synapses
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Cornichon2 Dictates the Time Course of Excitatory Transmission at Individual Hippocampal Synapses

机译:Cornichon2决定个别海马突触兴奋传递的时程。

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Cornichon2 (CNIH2), an integral component of AMPA receptor (AMPAR) complexes in the mammalian brain, slows deactivation and desensitization of heterologously reconstituted receptor channels. Its significance in neuronal signal transduction, however, has remained elusive. Here we show by paired recordings that CNIH2-containing AMPARs dictate the slow decay of excitatory postsynaptic currents (EPSCs) elicited in hilar mossy cells of the hippocampus by single action potentials in mossy fiber boutons (MFB). Selective knockdown of CNIH2 markedly accelerated EPSCs in individual MFB-mossy cell synapses without altering the EPSC amplitude. In contrast, the rapidly decaying EPSCs in synapses between MFBs and aspiny interneurons that lack expression of CNIH2 were unaffected by the protein knockdown but were slowed by virus-directed expression of CNIH2. These results identify CNIH2 as the molecular distinction between slow and fast EPSC phenotypes and show that CNIH2 influences the time course and, hence, the efficacy of excitatory synaptic transmission.
机译:Cornichon2(CNIH2)是哺乳动物大脑中AMPA受体(AMPAR)复合物的组成部分,可减缓异源重组受体通道的失活和减敏作用。然而,其在神经元信号转导中的意义仍然难以捉摸。在这里,我们通过成对的记录显示,含CNIH2的AMPAR决定了苔藓纤维钮扣(MFB)中的单个动作电位在海马的肺门苔藓细胞中引起的兴奋性突触后突触电流(EPSC)的缓慢衰减。在不改变EPSC振幅的情况下,单个MFB-苔藓细胞突触中CNIH2的选择性敲低显着加速了EPSC。相反,缺乏CNIH2表达的MFB和棘突间神经元之间的突触中快速衰减的EPSC不受蛋白敲低的影响,但受病毒导向的CNIH2表达的影响而减慢。这些结果确定了CNIH2是慢速和快速EPSC表型之间的分子区别,并表明CNIH2影响时间过程,从而影响兴奋性突触传递的功效。

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