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Functional interactions of ion channels with the actin cytoskeleton: does coupling to dynamic actin regulate NMDA receptors?

机译:离子通道与肌动蛋白细胞骨架的功能相互作用:是否偶联与动态肌动蛋白调节NMDA受体?

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摘要

Synapses are enriched in the cytoskeletal protein actin, which determines the shape of the pre- and postsynaptic compartments, organizes the neurotransmitter release machinery, and provides a framework for trafficking of components. In the postsynaptic compartment, interactions with actin or its associated proteins are also critical for the localization and activity of synaptic neurotransmitter receptors and ion channels. Actin binding proteins, including spectrin and alpha-actinin, serve as molecular linkages between the actin cytoskeleton and a diverse collection of receptors, including the NMDA receptor (NMDAR) and voltage-gated Na(+)channels. The actin cytoskeleton can regulate neurotransmitter receptors and ion channels by controlling their trafficking and localization at the synapse and by directly gating receptor channel opening. We highlight evidence that synaptic actin couples physically and functionally to the NMDAR and supports its activity. The molecular mechanisms by which actin regulates NMDARs are only just emerging, and recent advancements in light and electron microscopy-based imaging techniques should aide in elucidating these mechanisms.
机译:突触富含细胞骨架蛋白肌动蛋白,肌动蛋白决定突触前和突触后隔室的形状,组织神经递质释放机制,并为成分的运输提供框架。在突触后区室中,与肌动蛋白或其相关蛋白的相互作用对突触神经递质受体和离子通道的定位和活动也至关重要。肌动蛋白结合蛋白,包括光谱蛋白和α肌动蛋白,作为肌动蛋白细胞骨架和多种受体之间的分子联系,包括NMDA受体(NMDAR)和电压门控钠(+)通道。肌动蛋白细胞骨架可以通过控制神经递质受体和离子通道在突触上的运输和定位,并通过直接门控受体通道的开放来调节它们。我们强调了突触肌动蛋白在生理和功能上与NMDAR结合并支持其活动的证据。肌动蛋白调节NMDAR的分子机制才刚刚出现,基于光学和电子显微镜成像技术的最新进展应该有助于阐明这些机制。

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