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通过 mRNA 运输和局部翻译调节亚细胞域中的蛋白质水平。

Regulation of protein levels in subcellular domains through mRNA transport and localized translation.

机构信息

Burke Medical Research Institute, White Plains, New York 10605, USA.

出版信息

Mol Cell Proteomics. 2010 May;9(5):952-62. doi: 10.1074/mcp.R900005-MCP200. Epub 2010 Feb 18.

Abstract

Localized protein synthesis is increasingly recognized as a means for polarized cells to modulate protein levels in subcellular regions and the distal reaches of their cytoplasm. The axonal and dendritic processes of neurons represent functional domains of cytoplasm that can be separated from their cell body by vast distances. This separation provides a biological setting where the cell uses locally synthesized proteins to both autonomously respond to stimuli and to retrogradely signal the cell body of events occurring is this distal environment. Other cell types undoubtedly take advantage of this localized mechanism, but these have not proven as amenable for isolation of functional subcellular domains. Consequently, neurons have provided an appealing experimental platform for study of mRNA transport and localized protein synthesis. Molecular biology approaches have shown both the population of mRNAs that can localize into axons and dendrites and an unexpectedly complex regulation of their transport into these processes. Several lines of evidence point to similar complexities and specificity for regulation of mRNA translation at subcellular sites. Proteomics studies are beginning to provide a comprehensive view of the protein constituents of subcellular domains in neurons and other cell types. However, these have currently fallen short of dissecting temporal regulation of new protein synthesis in subcellular sites and mechanisms used to ferry mRNAs to these sites.

摘要

局部蛋白质合成正逐渐被视为极化细胞调节亚细胞区域和细胞质远端蛋白质水平的一种手段。神经元的轴突和树突代表细胞质的功能域,可以与细胞体分离很远的距离。这种分离为细胞提供了一个生物学环境,使细胞能够利用局部合成的蛋白质来自主响应刺激,并逆行信号传递细胞体,以告知发生在远端环境中的事件。其他细胞类型无疑也利用了这种局部机制,但这些细胞类型尚未被证明能够分离出功能的亚细胞域。因此,神经元为研究 mRNA 运输和局部蛋白质合成提供了一个有吸引力的实验平台。分子生物学方法已经显示了可以定位于轴突和树突中的 mRNA 群体,以及对其运输到这些过程中的出乎意料的复杂调控。有几条证据表明,在亚细胞部位的 mRNA 翻译调控中存在类似的复杂性和特异性。蛋白质组学研究开始提供神经元和其他细胞类型中亚细胞域的蛋白质组成的全面视图。然而,这些研究目前还未能解析亚细胞部位新蛋白质合成的时间调控,以及将 mRNAs 运送到这些部位的机制。

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