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埃博拉病毒和雷斯顿病毒 VP35 寡聚化结构域及其在所有埃博拉病毒种属中的比较生物物理特征。

Structures of Ebola and Reston Virus VP35 Oligomerization Domains and Comparative Biophysical Characterization in All Ebolavirus Species.

机构信息

The Max-Planck Institute of Biochemistry, Department of Molecular Structural Biology, Am Klopferspitz 18, 82152 Martinsried, Germany.

Istituto Zooprofilattico dell'Abruzzo e del Molise, Campo Boario, 64100 Teramo, Italy.

出版信息

Structure. 2019 Jan 2;27(1):39-54.e6. doi: 10.1016/j.str.2018.09.009. Epub 2018 Oct 25.

Abstract

The multifunctional virion protein 35 (VP35) of ebolaviruses is a critical determinant of virulence and pathogenesis indispensable for viral replication and host innate immune evasion. Essential for VP35 function is homo-oligomerization via a coiled-coil motif. Here we report crystal structures of VP35 oligomerization domains from the prototypic Ebola virus (EBOV) and the non-pathogenic Reston virus (RESTV), together with a comparative biophysical characterization of the domains from all known species of the Ebolavirus genus. EBOV and RESTV VP35 oligomerization domains form bipartite parallel helix bundles with a canonical coiled coil in the N-terminal half and increased plasticity in the highly conserved C-terminal half. The domain assembles into trimers and tetramers in EBOV, whereas it exclusively forms tetramers in all other ebolavirus species. Substitution of coiled-coil leucine residues critical for immune antagonism leads to aberrant oligomerization. A conserved arginine involved in inter-chain salt bridges stabilizes the VP35 oligomerization domain and modulates between coiled-coil oligomeric states.

摘要

埃博拉病毒的多功能病毒蛋白 35(VP35)是病毒复制和宿主固有免疫逃避所必需的毒力和发病机制的关键决定因素。VP35 的功能必需通过卷曲螺旋基序进行同源寡聚化。在这里,我们报告了来自原型埃博拉病毒(EBOV)和非致病性 Reston 病毒(RESTV)的 VP35 寡聚化结构域的晶体结构,以及对所有已知埃博拉病毒属物种的结构域的比较生物物理特性。EBOV 和 RESTV VP35 寡聚化结构域形成双部分平行螺旋束,N 端的半胱氨酸残基具有典型的卷曲螺旋,而高度保守的 C 端半胱氨酸残基具有更高的可塑性。该结构域在 EBOV 中组装成三聚体和四聚体,而在所有其他埃博拉病毒物种中,它仅形成四聚体。卷曲螺旋中对免疫拮抗至关重要的亮氨酸残基的取代会导致异常寡聚化。参与链间盐桥的保守精氨酸稳定 VP35 寡聚化结构域并调节卷曲螺旋寡聚状态。

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