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Breaking Symmetry in Viral Icosahedral Capsids as Seen through the Lenses of X-ray Crystallography and Cryo-Electron Microscopy

机译:通过X射线晶体学和低温电子显微镜观察打破病毒二十面体衣壳的对称性

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摘要

The majority of viruses on Earth form capsids built by multiple copies of one or more types of a coat protein arranged with 532 symmetry, generating an icosahedral shell. This highly repetitive structure is ideal to closely pack identical protein subunits and to enclose the nucleic acid genomes. However, the icosahedral capsid is not merely a passive cage but undergoes dynamic events to promote packaging, maturation and the transfer of the viral genome into the host. These essential processes are often mediated by proteinaceous complexes that interrupt the shell’s icosahedral symmetry, providing a gateway through the capsid. In this review, we take an inventory of molecular structures observed either internally, or at the 5-fold vertices of icosahedral DNA viruses that infect bacteria, archea and eukaryotes. Taking advantage of the recent revolution in cryo-electron microscopy (cryo-EM) and building upon a wealth of crystallographic structures of individual components, we review the design principles of non-icosahedral structural components that interrupt icosahedral symmetry and discuss how these macromolecules play vital roles in genome packaging, ejection and host receptor-binding.
机译:地球上的大多数病毒形成衣壳,该衣壳由一种或多种类型的外壳蛋白(具有532个对称性)的多个副本构建而成,从而生成二十面体壳。这种高度重复的结构非常适合紧密包装相同的蛋白质亚基并封闭核酸基因组。然而,二十面体衣壳不仅是被动的笼子,而且还经历动态事件以促进包装,成熟以及病毒基因组向宿主的转移。这些基本过程通常是由蛋白质复合物介导的,这些蛋白质复合物中断了壳的二十面体对称性,为通过衣壳提供了通道。在这篇综述中,我们对在内部或在感染细菌,古细菌和真核生物的二十面体DNA病毒的5倍顶点处观察到的分子结构进行了清点。利用最新的低温电子显微镜(cryo-EM)革命,并利用大量单个成分的晶体结构,我们回顾了中断二十面体对称性的非二十面体结构成分的设计原理,并讨论了这些大分子如何发挥重要作用在基因组包装,弹射和宿主受体结合中的作用。

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