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一种新的标记策略表明肌球蛋白 Va 和肌球蛋白 Vb 结合相同的树突极化囊泡群体。

A novel labeling strategy reveals that myosin Va and myosin Vb bind the same dendritically polarized vesicle population.

机构信息

Department of Biological Sciences and the Center for Biotechnology and Interdisciplinary Studies, Rensselaer Polytechnic Institute, Troy, New York, USA.

出版信息

Traffic. 2020 Nov;21(11):689-701. doi: 10.1111/tra.12764.

Abstract

Neurons are specialized cells with a polarized geometry and several distinct subdomains that require specific complements of proteins. Delivery of transmembrane proteins requires vesicle transport, which is mediated by molecular motor proteins. The myosin V family of motor proteins mediates transport to the barbed end of actin filaments, and little is known about the vesicles bound by myosin V in neurons. We developed a novel strategy to visualize myosin V-labeled vesicles in cultured hippocampal neurons and systematically characterized the vesicle populations labeled by myosin Va and Vb. We find that both myosins bind vesicles that are polarized to the somatodendritic domain where they undergo bidirectional long-range transport. A series of two-color imaging experiments showed that myosin V specifically colocalized with two different vesicle populations: vesicles labeled with the transferrin receptor and vesicles labeled by low-density lipoprotein receptor. Finally, coexpression with Kinesin-3 family members found that myosin V binds vesicles concurrently with KIF13A or KIF13B, supporting the hypothesis that coregulation of kinesins and myosin V on vesicles is likely to play an important role in neuronal vesicle transport. We anticipate that this new assay will be applicable in a broad range of cell types to determine the function of myosin V motor proteins.

摘要

神经元是具有极化几何形状和几个不同亚域的特化细胞,需要特定的蛋白质补充。跨膜蛋白的输送需要囊泡运输,这是由分子马达蛋白介导的。肌球蛋白 V 家族的马达蛋白介导运输到肌动蛋白丝的游离端,而关于神经元中肌球蛋白 V 结合的囊泡知之甚少。我们开发了一种新策略来可视化培养的海马神经元中肌球蛋白 V 标记的囊泡,并系统地表征了肌球蛋白 Va 和 Vb 标记的囊泡群体。我们发现,两种肌球蛋白都结合了极化到树突状区域的囊泡,在那里它们进行双向长程运输。一系列双色成像实验表明,肌球蛋白 V 特异性地与两种不同的囊泡群体共定位:转铁蛋白受体标记的囊泡和低密度脂蛋白受体标记的囊泡。最后,与 Kinesin-3 家族成员的共表达表明,肌球蛋白 V 与 KIF13A 或 KIF13B 结合囊泡,支持这样的假设,即囊泡上的驱动蛋白和肌球蛋白 V 的核心调控可能在神经元囊泡运输中发挥重要作用。我们预计,这种新的测定方法将适用于广泛的细胞类型,以确定肌球蛋白 V 马达蛋白的功能。

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