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海人藻酸受体的突触靶向作用

Synaptic Targeting of Kainate Receptors.

作者信息

Palacios-Filardo Jon, Aller M Isabel, Lerma Juan

机构信息

Instituto de Neurociencias (CSIC-UMH), 03550 San Juan de Alicante, Spain.

出版信息

Cereb Cortex. 2016 Apr;26(4):1464-72. doi: 10.1093/cercor/bhu244. Epub 2014 Oct 14.

Abstract

When native and recombinant kainate receptors (KARs) are compared, there is a mismatch in several of their functional properties. While both generate currents, synaptic responses mediated by KARs have rarely observed in cultured hippocampal neurons. The recent discovery of auxiliary proteins for KARs, such as Netos, offers an explanation for these discrepancies. We found that the GluK5 KAR subunit and the ancillary proteins, Neto1 and Neto2, are not expressed by hippocampal neurons in culture. Therefore, we used this model to directly test whether these proteins are required for the synaptic localization of KARs. Transfection of GluK4, GluK5, Neto1, or Neto2 into hippocampal neurons was associated with the appearance of synaptic KAR-mediated EPSCs. However, GluK4 or GluK5 alone produced synaptic activity in a significant proportion of cells and with reliable event frequency. While neurons expressing GluK4 or GluK5 subunits displayed synaptic responses with rapid kinetics, the expression of Neto proteins conferred these synaptic responses with their characteristic slow onset and decay rates. These data reveal some requirements for KAR targeting to the synapse, indicating a fundamental role of high affinity KAR subunits in this process.

摘要

当对天然型和重组型红藻氨酸受体(KARs)进行比较时,它们的几种功能特性存在不匹配之处。虽然两者都会产生电流,但在培养的海马神经元中很少观察到由KARs介导的突触反应。最近发现的KARs辅助蛋白,如Netos,为这些差异提供了解释。我们发现,培养的海马神经元不表达GluK5 KAR亚基以及辅助蛋白Neto1和Neto2。因此,我们利用这个模型直接测试这些蛋白是否是KARs突触定位所必需的。将GluK4、GluK5、Neto1或Neto2转染到海马神经元中与突触KAR介导的兴奋性突触后电流(EPSCs)的出现相关。然而,单独的GluK4或GluK5在相当比例的细胞中产生了突触活性,且事件频率可靠。虽然表达GluK4或GluK5亚基的神经元表现出具有快速动力学的突触反应,但Neto蛋白的表达赋予了这些突触反应其特征性的缓慢起始和衰减速率。这些数据揭示了KAR靶向突触的一些要求,表明高亲和力KAR亚基在这一过程中起基本作用。

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