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Contribution of Ebola Virus Glycoprotein Nucleoprotein and VP24 to Budding of VP40 Virus-Like Particles

机译:埃博拉病毒糖蛋白核蛋白和VP24对VP40病毒样颗粒萌发的贡献

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摘要

The VP40 matrix protein of Ebola virus buds from cells in the form of virus-like particles (VLPs) and plays a central role in virus assembly and budding. In this study, we utilized a functional budding assay and cotransfection experiments to examine the contributions of the glycoprotein (GP), nucleoprotein (NP), and VP24 of Ebola virus in facilitating release of VP40 VLPs. We demonstrate that VP24 alone does not affect VP40 VLP release, whereas NP and GP enhance release of VP40 VLPs, individually and to a greater degree in concert. We demonstrate further the following: (i) VP40 L domains are not required for GP-mediated enhancement of budding; (ii) the membrane-bound form of GP is necessary for enhancement of VP40 VLP release; (iii) NP appears to physically interact with VP40 as judged by detection of NP in VP40-containing VLPs; and (iv) the C-terminal 50 amino acids of NP may be important for interacting with and enhancing release of VP40 VLPs. These findings provide a more complete understanding of the role of VP40 and additional Ebola virus proteins during budding.
机译:埃博拉病毒的VP40基质蛋白以病毒样颗粒(VLP)的形式从细胞中萌芽,并在病毒组装和萌芽过程中发挥重要作用。在这项研究中,我们利用功能性萌芽测定和共转染实验来检查埃博拉病毒的糖蛋白(GP),核蛋白(NP)和VP24在促进VP40 VLP释放中的作用。我们证明,单独的VP24不会影响VP40 VLP的释放,而NP和GP可以单独且在更大程度上共同提高VP40 VLP的释放。我们进一步证明以下内容:(i)GP介导的出芽增强不需要VP40 L结构域; (ii)GP的膜结合形式是增强VP40 VLP释放所必需的; (iii)通过检测含VP40的VLP中的NP判断,NP似乎与VP40发生物理相互作用; (iv)NP的C末端50个氨基酸对于与VP40 VLP相互作用和增强VP40 VLP的释放可能很重要。这些发现提供了对VP40和其他埃博拉病毒蛋白在萌芽过程中的作用的更完整的了解。

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