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运输蛋白在腺病毒核心蛋白和DNA核输入中的作用。

A role for transportin in the nuclear import of adenovirus core proteins and DNA.

作者信息

Hindley Clemence E, Lawrence Fiona J, Matthews David A

机构信息

Department of Cellular and Molecular Medicine, School of Medical Sciences, University of Bristol, Bristol, UK.

出版信息

Traffic. 2007 Oct;8(10):1313-22. doi: 10.1111/j.1600-0854.2007.00618.x.

Abstract

Adenoviruses target their double-stranded DNA genome and its associated core proteins to the interphase nucleus; this core structure then enters through the nuclear pore complex. We have used digitonin permeabilized cell import assays to study the cellular import factors involved in nuclear entry of virus DNA and the core proteins, protein V and protein VII. We show that inhibition of transportin results in aberrant localization of protein V and that transportin is necessary for protein V to accumulate in the nucleolus. Furthermore, inhibition of transportin results in inhibition of protein VII and DNA import, whereas disruption of the classical importin alpha-importin beta import pathway has little effect. We show that mature protein VII has different import preferences from the precursor protein, preVII from which it is derived by proteolytic processing. While bacterially expressed glutathione S-transferase (GST)-preVII primarily utilizes the pathway mediated by importin alpha-importin beta, bacterially expressed GST-VII favours the transportin pathway. This is significant because while preVII is important during viral replication and assembly only mature VII is available during viral DNA import to a newly infected cell. Our results implicate transportin as a key import receptor for the nuclear localization of adenovirus core.

摘要

腺病毒将其双链DNA基因组及其相关核心蛋白靶向至间期细胞核;然后这种核心结构通过核孔复合体进入细胞核。我们利用洋地黄皂苷通透细胞导入实验来研究参与病毒DNA及核心蛋白(蛋白V和蛋白VII)核进入过程的细胞导入因子。我们发现抑制运输蛋白会导致蛋白V定位异常,且运输蛋白是蛋白V在核仁中积累所必需的。此外,抑制运输蛋白会导致蛋白VII和DNA导入受到抑制,而破坏经典的输入蛋白α-输入蛋白β导入途径影响不大。我们发现成熟的蛋白VII与前体蛋白preVII具有不同的导入偏好,preVII经蛋白水解加工后产生蛋白VII。虽然细菌表达的谷胱甘肽S-转移酶(GST)-preVII主要利用由输入蛋白α-输入蛋白β介导的途径,但细菌表达的GST-VII则倾向于运输蛋白途径。这一点很重要,因为虽然preVII在病毒复制和组装过程中很重要,但在病毒DNA导入新感染细胞期间只有成熟VII可用。我们的结果表明运输蛋白是腺病毒核心蛋白核定位的关键导入受体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d987/2171040/73342ed7d0ae/tra0008-1313-f1.jpg

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