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腺病毒核心蛋白pVII通过多种输入受体途径转运至细胞核。

Adenovirus core protein pVII is translocated into the nucleus by multiple import receptor pathways.

作者信息

Wodrich Harald, Cassany Aurelia, D'Angelo Maximiliano A, Guan Tinglu, Nemerow Glen, Gerace Larry

机构信息

Institut de Génétique Moléculaire de Montpellier, UMR 5535 CNRS, 1919 Route de Mende, 34293 Montpellier Cedex 05, France.

出版信息

J Virol. 2006 Oct;80(19):9608-18. doi: 10.1128/JVI.00850-06.

Abstract

Adenoviruses are nonenveloped viruses with an approximately 36-kb double-stranded DNA genome that replicate in the nucleus. Protein VII, an abundant structural component of the adenovirus core that is strongly associated with adenovirus DNA, is imported into the nucleus contemporaneously with the adenovirus genome shortly after virus infection and may promote DNA import. In this study, we evaluated whether protein VII uses specific receptor-mediated mechanisms for import into the nucleus. We found that it contains potent nuclear localization signal (NLS) activity by transfection of cultured cells with protein VII fusion constructs and by microinjection of cells with recombinant protein VII fusions. We identified three NLS-containing regions in protein VII by deletion mapping and determined important NLS residues by site-specific mutagenesis. We found that recombinant protein VII and its NLS-containing domains strongly and specifically bind to importin alpha, importin beta, importin 7, and transportin, which are among the most abundant cellular nuclear import receptors. Moreover, these receptors can mediate the nuclear import of protein VII fusions in vitro in permeabilized cells. Considered together, these data support the hypothesis that protein VII is a major NLS-containing adaptor for receptor-mediated import of adenovirus DNA and that multiple import pathways are utilized to promote efficient nuclear entry of the viral genome.

摘要

腺病毒是无包膜病毒,其基因组为约36kb的双链DNA,在细胞核中复制。蛋白质VII是腺病毒核心中一种丰富的结构成分,与腺病毒DNA紧密相关,在病毒感染后不久与腺病毒基因组同时被导入细胞核,可能促进DNA的导入。在本研究中,我们评估了蛋白质VII是否利用特定的受体介导机制导入细胞核。我们通过用蛋白质VII融合构建体转染培养细胞以及用重组蛋白质VII融合物显微注射细胞,发现它具有强大的核定位信号(NLS)活性。我们通过缺失图谱分析在蛋白质VII中鉴定出三个含NLS的区域,并通过位点特异性诱变确定了重要的NLS残基。我们发现重组蛋白质VII及其含NLS的结构域能强烈且特异性地与输入蛋白α、输入蛋白β、输入蛋白7和运输蛋白结合,这些是细胞中最丰富的细胞核输入受体。此外,这些受体在体外可介导通透细胞中蛋白质VII融合物的细胞核输入。综合考虑,这些数据支持以下假说:蛋白质VII是一种主要的含NLS的衔接蛋白,用于受体介导的腺病毒DNA导入,并且利用多种输入途径来促进病毒基因组高效进入细胞核。

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