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

机译:从脉冲结构的结构中洞察疱疹病毒组件:刮浆件复合物

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摘要

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 trans-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.
机译:Herpesviruses通过持续不清楚的分子机制获取受感染细胞的细胞质中的膜包膜。单纯疱疹病毒(HSV)-1蛋白质浆浆和刮浆蛋白脉冲脉冲脉冲型脉冲型脉冲率为有效的病毒包膜所需的复合物。我们表明,脉冲疱疹和刮浆物质之间的相互作用在人疱疹病毒中保守,与其与反式高尔基膜的关系。通过溶液散射和化学交联,表征HSV-1脉冲滤波器7:脉冲51复合物,揭示了可以在溶液中形成高阶低聚物的1:2络合物,并且我们解决了芯浆7:脉冲晶片的晶体结构。虽然纸浆采用以前看不见的紧凑型折叠,但是脉冲螺旋螺旋构象的脉冲螺旋构象类似于转运所需的细胞内体复合物(ESCRT)-III组分CHMP4B和脉冲液体形成ESCRT-III样细丝,表明普拉斯普拉斯(ESCRT-III)的长丝,表明刮浆液的直接作用在促进病毒组件期间的膜群。我们的结果提供了一种结构框架,用于了解保守脉冲浆系统的作用:普拉斯维尔组件中的脉冲脉冲脉冲滤波器。

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