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输入蛋白α亚型在细胞运输和疾病状态中的多样化。

Diversification of importin-α isoforms in cellular trafficking and disease states.

作者信息

Pumroy Ruth A, Cingolani Gino

机构信息

*Department of Biochemistry and Molecular Biology, Thomas Jefferson University, Philadelphia, PA 19107, U.S.A.

出版信息

Biochem J. 2015 Feb 15;466(1):13-28. doi: 10.1042/BJ20141186.

DOI:10.1042/BJ20141186
PMID:25656054
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4405237/
Abstract

The human genome encodes seven isoforms of importin α which are grouped into three subfamilies known as α1, α2 and α3. All isoforms share a fundamentally conserved architecture that consists of an N-terminal, autoinhibitory, importin-β-binding (IBB) domain and a C-terminal Arm (Armadillo)-core that associates with nuclear localization signal (NLS) cargoes. Despite striking similarity in amino acid sequence and 3D structure, importin-α isoforms display remarkable substrate specificity in vivo. In the present review, we look at key differences among importin-α isoforms and provide a comprehensive inventory of known viral and cellular cargoes that have been shown to associate preferentially with specific isoforms. We illustrate how the diversification of the adaptor importin α into seven isoforms expands the dynamic range and regulatory control of nucleocytoplasmic transport, offering unexpected opportunities for pharmacological intervention. The emerging view of importin α is that of a key signalling molecule, with isoforms that confer preferential nuclear entry and spatiotemporal specificity on viral and cellular cargoes directly linked to human diseases.

摘要

人类基因组编码7种 importin α 亚型,它们被分为3个亚家族,即α1、α2和α3。所有亚型都具有基本保守的结构,包括一个N端自抑制性的importin-β结合(IBB)结构域和一个与核定位信号(NLS)货物相关的C端臂(犰狳)核心。尽管氨基酸序列和三维结构有显著相似性,但importin-α亚型在体内表现出显著的底物特异性。在本综述中,我们探讨了importin-α亚型之间的关键差异,并提供了已知病毒和细胞货物的综合清单,这些货物已被证明优先与特定亚型相关联。我们说明了衔接蛋白importin α多样化为7种亚型如何扩大核质运输的动态范围和调控控制,为药物干预提供了意想不到的机会。importin α的新观点是它是一种关键信号分子,其亚型赋予病毒和细胞货物优先的核进入以及与人类疾病直接相关的时空特异性。

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