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豇豆花叶病毒运动蛋白C端的研究

Studies on the C-terminus of the Cowpea mosaic virus movement protein.

作者信息

Bertens P, Heijne W, van der Wel N, Wellink J, van Kammen A

机构信息

Laboratory of Molecular Biology, Wageningen University, Wageningen, The Netherlands.

出版信息

Arch Virol. 2003 Feb;148(2):265-79. doi: 10.1007/s00705-002-0918-z.

Abstract

Cowpea mosaic virus (CPMV) spreads from cell-to-cell as virus particles through tubular structures in modified plasmodesmata which are composed of viral movement protein (MP). Mutational analysis of the MP has revealed that the N-terminal and central regions of the MP are involved in tubule formation and that the C-terminal domain probably has a role in the interactions with virus particles. By constructing C-terminal deletion mutants and comoviral hybrid MPs, it was possible to delineate the C-terminal border of the tubule-forming domain to a small region between amino acids 292 and 298. Experiments with tripartite viruses in protoplasts indicated that the C-terminus of the MP is involved in the incorporation of virus particles in the tubule and that for efficient incorporation of virus particles all MP molecules incorporated in a tubule need to contain a functional C-terminus. A mutant virus coding for a MP in which the last 10 C-terminal amino acids were replaced by the green fluorescent protein (GFP) was able to form tubules in protoplasts. These tubules did not contain virus particles, probably because the GFP interferes with the incorporation of virions into the tubule. These results suggest a model for the structure of the tubule in which the C-terminus of the MP is located inside the tubular structure, where it is able to interact with virus particles.

摘要

豇豆花叶病毒(CPMV)作为病毒粒子通过修饰的胞间连丝中的管状结构在细胞间传播,这些管状结构由病毒运动蛋白(MP)组成。对MP的突变分析表明,MP的N端和中央区域参与小管形成,而C端结构域可能在与病毒粒子的相互作用中发挥作用。通过构建C端缺失突变体和共病毒杂交MP,有可能将小管形成结构域的C端边界划定到氨基酸292和298之间的一个小区域。原生质体中三方病毒的实验表明,MP的C端参与病毒粒子在小管中的掺入,并且为了有效掺入病毒粒子,掺入小管中的所有MP分子都需要包含一个功能性C端。一种编码MP的突变病毒,其中最后10个C端氨基酸被绿色荧光蛋白(GFP)取代,能够在原生质体中形成小管。这些小管不包含病毒粒子,可能是因为GFP干扰了病毒粒子掺入小管。这些结果提示了一种小管结构模型,其中MP的C端位于管状结构内部,在那里它能够与病毒粒子相互作用。

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