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结构洞察不同病毒衣壳复合物的组装和调控。

Structural insights into the assembly and regulation of distinct viral capsid complexes.

机构信息

School of Animal and Veterinary Sciences, Charles Sturt University, Boorooma Street, Wagga Wagga, New South Wales 2678, Australia.

Graham Centre for Agricultural Innovation, NSW Department of Primary Industries and Charles Sturt University, Boorooma Street, Wagga Wagga, New South Wales 2678, Australia.

出版信息

Nat Commun. 2016 Oct 4;7:13014. doi: 10.1038/ncomms13014.

Abstract

The assembly and regulation of viral capsid proteins into highly ordered macromolecular complexes is essential for viral replication. Here, we utilize crystal structures of the capsid protein from the smallest and simplest known viruses capable of autonomously replicating in animal cells, circoviruses, to establish structural and mechanistic insights into capsid morphogenesis and regulation. The beak and feather disease virus, like many circoviruses, encode only two genes: a capsid protein and a replication initiation protein. The capsid protein forms distinct macromolecular assemblies during replication and here we elucidate these structures at high resolution, showing that these complexes reverse the exposure of the N-terminal arginine rich domain responsible for DNA binding and nuclear localization. We show that assembly of these complexes is regulated by single-stranded DNA (ssDNA), and provide a structural basis of capsid assembly around single-stranded DNA, highlighting novel binding interfaces distinct from the highly positively charged N-terminal ARM domain.

摘要

病毒衣壳蛋白的组装和调节对于病毒的复制至关重要。在这里,我们利用能够在动物细胞中自主复制的最小和最简单的已知病毒——圆环病毒的衣壳蛋白的晶体结构,来建立对衣壳形态发生和调节的结构和机制见解。喙羽病病毒与许多圆环病毒一样,只编码两种基因:衣壳蛋白和复制起始蛋白。衣壳蛋白在复制过程中形成不同的大分子组装体,在这里我们以高分辨率阐明了这些结构,表明这些复合物逆转了负责 DNA 结合和核定位的 N 端富含精氨酸的结构域的暴露。我们表明,这些复合物的组装受到单链 DNA(ssDNA)的调节,并提供了围绕单链 DNA 的衣壳组装的结构基础,突出了与高度带正电荷的 N 端 ARM 结构域不同的新型结合界面。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5936/5059447/42838c28dafa/ncomms13014-f1.jpg

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