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内托介导的细胞内相互作用塑造了果蝇神经肌肉接头处的突触后成分。

Neto-mediated intracellular interactions shape postsynaptic composition at the Drosophila neuromuscular junction.

作者信息

Ramos Cathy I, Igiesuorobo Oghomwen, Wang Qi, Serpe Mihaela

机构信息

Program in Cellular Regulation and Metabolism, NICHD, NIH, Bethesda, Maryland, United States of America.

出版信息

PLoS Genet. 2015 Apr 23;11(4):e1005191. doi: 10.1371/journal.pgen.1005191. eCollection 2015 Apr.

Abstract

The molecular mechanisms controlling the subunit composition of glutamate receptors are crucial for the formation of neural circuits and for the long-term plasticity underlying learning and memory. Here we use the Drosophila neuromuscular junction (NMJ) to examine how specific receptor subtypes are recruited and stabilized at synaptic locations. In flies, clustering of ionotropic glutamate receptors (iGluRs) requires Neto (Neuropillin and Tolloid-like), a highly conserved auxiliary subunit that is essential for NMJ assembly and development. Drosophila neto encodes two isoforms, Neto-α and Neto-β, with common extracellular parts and distinct cytoplasmic domains. Mutations that specifically eliminate Neto-β or its intracellular domain were generated. When Neto-β is missing or is truncated, the larval NMJs show profound changes in the subtype composition of iGluRs due to reduced synaptic accumulation of the GluRIIA subunit. Furthermore, neto-β mutant NMJs fail to accumulate p21-activated kinase (PAK), a critical postsynaptic component implicated in the synaptic stabilization of GluRIIA. Muscle expression of either Neto-α or Neto-β rescued the synaptic transmission at neto null NMJs, indicating that Neto conserved domains mediate iGluRs clustering. However, only Neto-β restored PAK synaptic accumulation at neto null NMJs. Thus, Neto engages in intracellular interactions that regulate the iGluR subtype composition by preferentially recruiting and/or stabilizing selective receptor subtypes.

摘要

控制谷氨酸受体亚基组成的分子机制对于神经回路的形成以及学习和记忆所依赖的长期可塑性至关重要。在此,我们利用果蝇神经肌肉接头(NMJ)来研究特定受体亚型是如何在突触位置被募集并稳定下来的。在果蝇中,离子型谷氨酸受体(iGluRs)的聚集需要Neto(神经纤毛蛋白和类 tolloid 蛋白),它是一种高度保守的辅助亚基,对 NMJ 的组装和发育至关重要。果蝇 neto 编码两种异构体,Neto-α 和 Neto-β,它们具有共同的细胞外部分和不同的细胞质结构域。我们产生了特异性消除 Neto-β 或其细胞内结构域的突变。当 Neto-β 缺失或被截断时,幼虫的 NMJ 由于 GluRIIA 亚基的突触积累减少而在 iGluRs 的亚型组成上显示出深刻变化。此外,neto-β 突变体的 NMJ 无法积累 p21 活化激酶(PAK),PAK 是一种关键的突触后成分,与 GluRIIA 的突触稳定有关。Neto-α 或 Neto-β 的肌肉表达挽救了 neto 基因敲除的 NMJ 处的突触传递,表明 Neto 的保守结构域介导了 iGluRs 的聚集。然而,只有 Neto-β 恢复了 neto 基因敲除的 NMJ 处 PAK 的突触积累。因此,Neto 通过优先募集和/或稳定选择性受体亚型参与细胞内相互作用,从而调节 iGluR 亚型组成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b5b1/4408064/f137b4e3dd0c/pgen.1005191.g001.jpg

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