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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Synaptic Targeting and Functional Modulation of GluK1 Kainate Receptors by the Auxiliary Neuropilin and Tolloid-Like (NETO) Proteins.
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Synaptic Targeting and Functional Modulation of GluK1 Kainate Receptors by the Auxiliary Neuropilin and Tolloid-Like (NETO) Proteins.

机译:辅助神经菌毛蛋白和类Tolloid(NETO)蛋白对GluK1 Kainate受体的突触靶向和功能调节。

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摘要

Auxiliary proteins modify the biophysical function and pharmacological properties of ionotropic glutamate receptors and likely are important components of receptor signaling complexes in vivo. The neuropilin and tolloid-like proteins (NETO) 1 and NETO2, two closely related CUB domain-containing integral membrane proteins, were identified recently as auxiliary proteins that slowed GluK2a kainate receptor current kinetics without impacting receptor membrane localization. Here we demonstrate that NETO2 profoundly slows the desensitization rate of GluK1 kainate receptors, promotes plasma membrane localization of transfected receptors in heterologous cells and rat hippocampal neurons, and targets GluK1-containing receptors to synapses. Conversely, the closely related protein NETO1 increases the rate of GluK1 receptor desensitization. Incorporation of NETO proteins into kainate receptor-signaling complexes therefore extends the temporal range of receptor gating by over an order of magnitude. The presence of these auxiliary proteins could underlie some of the unusual aspects of kainate receptor function in the mammalian CNS.
机译:辅助蛋白修饰离子型谷氨酸受体的生物物理功能和药理特性,可能是体内受体信号复合物的重要组成部分。最近发现,两个紧密相关的含CUB结构域的整合膜蛋白Neuropilin和Tolloid-like蛋白(NETO)1和NETO2被确认为辅助蛋白,可减缓GluK2a红藻氨酸受体电流动力学,而不会影响受体膜的定位。在这里,我们证明NETO2大大减慢了GluK1海藻酸酯受体的脱敏速率,促进了异源细胞和大鼠海马神经元中转染受体的质膜定位,并靶向含有GluK1的受体进行突触。相反,密切相关的蛋白质NETO1会增加GluK1受体脱敏的速率。因此,将NETO蛋白掺入海藻酸盐受体信号复合物中可将受体门控的时间范围扩大一个数量级。这些辅助蛋白的存在可能是哺乳动物中枢神经系统中海藻酸盐受体功能异常的一些原因。

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