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从 pUL7:pUL51 复合物的结构中洞察疱疹病毒的组装。

Insights into herpesvirus assembly from the structure of the pUL7:pUL51 complex.

机构信息

Department of Pathology, University of Cambridge, Cambridge, United Kingdom.

European Molecular Biology Laboratory (EMBL) Hamburg Site, Hamburg, Germany.

出版信息

Elife. 2020 May 11;9:e53789. doi: 10.7554/eLife.53789.

Abstract

Herpesviruses acquire their membrane envelopes in the cytoplasm of infected cells via a molecular mechanism that remains unclear. Herpes simplex virus (HSV)-1 proteins pUL7 and pUL51 form a complex required for efficient virus envelopment. We show that interaction between homologues of pUL7 and pUL51 is conserved across human herpesviruses, as is their association with -Golgi membranes. We characterized the HSV-1 pUL7:pUL51 complex by solution scattering and chemical crosslinking, revealing a 1:2 complex that can form higher-order oligomers in solution, and we solved the crystal structure of the core pUL7:pUL51 heterodimer. While pUL7 adopts a previously-unseen compact fold, the helix-turn-helix conformation of pUL51 resembles the cellular endosomal complex required for transport (ESCRT)-III component CHMP4B and pUL51 forms ESCRT-III-like filaments, suggesting a direct role for pUL51 in promoting membrane scission during virus assembly. Our results provide a structural framework for understanding the role of the conserved pUL7:pUL51 complex in herpesvirus assembly.

摘要

疱疹病毒通过一种尚未明确的分子机制在感染细胞的细胞质中获得其膜包膜。单纯疱疹病毒 (HSV)-1 蛋白 pUL7 和 pUL51 形成了一个复合物,该复合物对于病毒的有效包裹是必需的。我们发现,pUL7 和 pUL51 的同源物之间的相互作用在人类疱疹病毒中是保守的,它们与 -高尔基体膜的结合也是如此。我们通过溶液散射和化学交联来表征 HSV-1 pUL7:pUL51 复合物,揭示了一种 1:2 的复合物,该复合物可以在溶液中形成更高阶的寡聚物,我们还解决了核心 pUL7:pUL51 异源二聚体的晶体结构。虽然 pUL7 采用了以前未见的紧凑折叠,但 pUL51 的螺旋-转角-螺旋构象类似于细胞内体运输所必需的复合物 (ESCRT)-III 成分 CHMP4B,并且 pUL51 形成 ESCRT-III 样纤维,这表明 pUL51 在促进病毒组装过程中的膜分裂中发挥直接作用。我们的研究结果为理解保守的 pUL7:pUL51 复合物在疱疹病毒组装中的作用提供了结构框架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b8fe/7289601/6b9767a605ed/elife-53789-fig1.jpg

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