Astbury Centre for Structural Molecular Biology, School of Molecular & Cellular Biology, Faculty of Biological Sciences, University of Leeds, Leeds, United Kingdom.
PLoS Biol. 2020 Mar 31;18(3):e3000649. doi: 10.1371/journal.pbio.3000649. eCollection 2020 Mar.
Icosahedral viral capsids must undergo conformational rearrangements to coordinate essential processes during the viral life cycle. Capturing such conformational flexibility has been technically challenging yet could be key for developing rational therapeutic agents to combat infections. Noroviruses are nonenveloped, icosahedral viruses of global importance to human health. They are a common cause of acute gastroenteritis, yet no vaccines or specific antiviral agents are available. Here, we use genetics and cryo-electron microscopy (cryo-EM) to study the high-resolution solution structures of murine norovirus as a model for human viruses. By comparing our 3 structures (at 2.9- to 3.1-Å resolution), we show that whilst there is little change to the shell domain of the capsid, the radiating protruding domains are flexible, adopting distinct states both independently and synchronously. In doing so, the capsids sample a range of conformational space, with implications for maintaining virion stability and infectivity.
二十面体病毒衣壳必须经历构象重排,以协调病毒生命周期中的重要过程。捕捉这种构象灵活性具有技术挑战性,但对于开发合理的治疗感染的药物可能是关键。诺如病毒是无包膜的二十面体病毒,对全球人类健康具有重要意义。它们是急性肠胃炎的常见病因,但目前尚无疫苗或特定的抗病毒药物。在这里,我们使用遗传学和低温电子显微镜(cryo-EM)来研究鼠诺如病毒的高分辨率溶液结构,作为人类病毒的模型。通过比较我们的 3 个结构(分辨率为 2.9 至 3.1 Å),我们表明,尽管衣壳的壳域变化很小,但辐射状突出的结构域是灵活的,无论是独立还是同步,都采用不同的状态。这样,衣壳可以在一系列构象空间中进行采样,这对维持病毒粒子的稳定性和感染力具有重要意义。
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