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神经元中极化膜运输的机制——聚焦于内体。

Mechanisms of polarized membrane trafficking in neurons -- focusing in on endosomes.

机构信息

Department of Neuroscience, University of Virginia Medical School, 409 Lane Rd. Extension, MR4-6116, Charlottesville, VA 22908, USA.

出版信息

Mol Cell Neurosci. 2011 Dec;48(4):278-87. doi: 10.1016/j.mcn.2011.06.013. Epub 2011 Jul 2.

Abstract

Neurons are polarized cells that have a complex and unique morphology: long processes (axons and dendrites) extending far from the cell body. In addition, the somatodendritic and axonal domains are further divided into specific subdomains, such as synapses (pre- and postsynaptic specializations), proximal and distal dendrites, axon initial segments, nodes of Ranvier, and axon growth cones. The striking asymmetry and complexity of neuronal cells are necessary for their function in receiving, processing and transferring electrical signals, with each domain playing a precise function in these processes. In order to establish and maintain distinct neuronal domains, mechanisms must exist for protein delivery to specific neuronal compartments, such that each compartment has the correct functional molecular composition. How polarized membrane domains are established and maintained is a long-standing question. Transmembrane proteins, such as receptors and adhesion molecules, can be transported to their proper membrane domains by several pathways. The biosynthetic secretory system delivers newly synthesized transmembrane proteins from the ER via the Golgi and trans-Golgi-network (TGN) to the plasma membrane. In addition, the endosomal system is critically involved in many instances in ensuring proper (re)targeting of membrane components because it can internalize and degrade mislocalized proteins, or recycle proteins from one domain to another. The endosomal system is thus crucial for establishing and maintaining neuronal polarity. In this review, we focus mainly on the intracellular compartments that serve as sorting stations for polarized transport, with particular emphasis on the emerging roles of endosomes.

摘要

神经元是具有复杂而独特形态的极化细胞

它们的长突起(轴突和树突)从细胞体延伸得很远。此外,体树突和轴突域进一步分为特定的亚域,如突触(前突触和后突触特化)、近端和远端树突、轴突起始段、Ranvier 结和轴突生长锥。神经元细胞的显著不对称性和复杂性是其接收、处理和传递电信号功能的必要条件,每个域在这些过程中都发挥着精确的作用。为了建立和维持独特的神经元域,必须存在将蛋白质递送到特定神经元区室的机制,以使每个区室具有正确的功能分子组成。极化膜域是如何建立和维持的,这是一个长期存在的问题。跨膜蛋白,如受体和粘附分子,可以通过几种途径被运输到它们适当的膜域。生物合成分泌系统将新合成的跨膜蛋白从内质网通过高尔基体和反式高尔基体网络(TGN)运送到质膜。此外,内体系统在许多情况下都参与了确保膜成分正确(再)靶向的过程,因为它可以内化和降解定位错误的蛋白质,或者将蛋白质从一个域循环到另一个域。因此,内体系统对于建立和维持神经元极性至关重要。在这篇综述中,我们主要关注作为极化运输分拣站的细胞内区室,特别强调内体的新兴作用。

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