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In silico 3D structure analysis accelerates the solution of a real viral structure and antibodies docking mechanism

机译:In silico 3D结构分析加速了真正病毒结构和抗体对接机制的解决方案

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摘要

Norwalk virus (NoV) is responsible for most outbreaks of non-bacterial gastroenteritis. NoV is genetically diverse and show antigenically variable. Recently, we produced a monoclonal antibody called 5B-18 that reacts broadly with NoV genogroup II (GII). We suspected the 5B-18 binds to a conformational epitope on 3D structure of virion. X-ray crystallography showed us that 5B-18 binds to NoV at the P domain, which protrudes from the capsid surface of the virion. However, there seems to be no space that would allow the IgG to approach the virion. To solve this problem, we used cryo-electron microscopy to examine NoV GII virus-like particles (VLPs). The P domain rises up higher in NoV GII than in NoV GI, and it seems to form an outer layer around the virion. Finally, using in silico modeling we found the 5B-18 Fab arms and NoV P region are quite flexible, so that 5B-18 can bind the NoV virion from bottom of P domain. This study demonstrates the shortcomings of studying biological phenomenon by only one technique. Each method has limitations. Multiple methods and modeling in silico are the keys to solving structural problems.
机译:诺沃克病毒(NoV)是大多数非细菌性胃肠炎的爆发原因。 NoV具有遗传多样性,并显示出抗原可变性。最近,我们生产了一种名为5B-18的单克隆抗体,可与NoV基因组II(GII)广泛反应。我们怀疑5B-18与病毒体3D结构上的构象表位结合。 X射线晶体学表明,5B-18在病毒颗粒的衣壳表面突出的P结构域与NoV结合。但是,似乎没有空间允许IgG接近病毒粒子。为了解决此问题,我们使用了冷冻电子显微镜检查了NoV GII病毒样颗粒(VLP)。在NoV GII中,P域的升高高于在NoV GI中,并且似乎在病毒体周围形成了外层。最后,通过计算机模拟,我们发现5B-18 Fab臂和NoV P区域非常灵活,因此5B-18可以从P结构域的底部结合NoV病毒体。这项研究表明仅通过一种技术来研究生物学现象的缺点。每种方法都有局限性。计算机上的多种方法和建模是解决结构问题的关键。

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