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横向扩散驱动树突棘处AMPA受体的组成性交换,并受棘形态调控。

Lateral diffusion drives constitutive exchange of AMPA receptors at dendritic spines and is regulated by spine morphology.

作者信息

Ashby Michael C, Maier Susie R, Nishimune Atsushi, Henley Jeremy M

机构信息

Medical Research Council Centre for Synaptic Plasticity, Department of Anatomy, University of Bristol, Medical School, Bristol BS8 1TD, United Kingdom.

出版信息

J Neurosci. 2006 Jun 28;26(26):7046-55. doi: 10.1523/JNEUROSCI.1235-06.2006.

Abstract

Synapse specificity is a basic feature of synaptic plasticity, but it remains unclear how synapse-specific signaling is achieved if postsynaptic membrane proteins can diffuse laterally between synapses. We monitored movements of AMPA receptors (AMPARs) on the surface of mature neurons to investigate the role of lateral diffusion in constitutive AMPAR trafficking and to assess the influence of membrane architecture on the surface distribution of synaptic proteins. Our data show that lateral diffusion is responsible for the continual exchange of a substantial pool of AMPARs at the spine surface. Furthermore, we found that a general characteristic of membrane proteins is that their movement into and out of spines is slow compared with that in nonspiny membrane. This shows that lateral diffusion is dependent on spine morphology and is restricted at the spine neck. These results demonstrate the importance of lateral diffusion in trafficking of AMPAR protein population and provide new insight into how spine structure can maintain synapse specificity by compartmentalizing lateral diffusion and therefore increasing the residence time of membrane proteins near individual synapses.

摘要

突触特异性是突触可塑性的一个基本特征,但如果突触后膜蛋白能够在突触之间进行侧向扩散,那么突触特异性信号是如何实现的仍不清楚。我们监测了成熟神经元表面AMPA受体(AMPARs)的运动,以研究侧向扩散在组成型AMPAR转运中的作用,并评估膜结构对突触蛋白表面分布的影响。我们的数据表明,侧向扩散导致了大量AMPARs在棘突表面的持续交换。此外,我们发现膜蛋白的一个普遍特征是,与非棘突膜相比,它们进出棘突的运动较慢。这表明侧向扩散依赖于棘突形态,并在棘突颈部受到限制。这些结果证明了侧向扩散在AMPAR蛋白群体转运中的重要性,并为棘突结构如何通过分隔侧向扩散来维持突触特异性从而增加膜蛋白在单个突触附近的停留时间提供了新的见解。

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