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The Dynamic Life of Virus Capsids

机译:病毒衣壳的动态寿命

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摘要

Protein-shelled viruses have been thought as “tin cans” that merely carry the genomic cargo from cell to cell. However, through the years, it has become clear that viruses such as rhinoviruses and caliciviruses are active and dynamic structures waiting for the right environmental cues to deliver their genomic payload to the host cell. In the case of human rhinoviruses, the capsid has empty cavities that decrease the energy required to cause conformational changes, resulting in the capsids “breathing”, waiting for the moment when the receptor binds for it to release its genome. Most strikingly, the buried N-termini of VP1 and VP4 are transiently exposed during this process. A more recent example of a “living” protein capsid is mouse norovirus (MNV). This family of viruses have a large protruding (P) domain that is loosely attached to the shell via a single-polypeptide tether. Small molecules found in the gut, such as bile salts, cause the P domains to rotate and collapse onto the shell surface. Concomitantly, bile alters the conformation of the P domain itself from one that binds antibodies to one that recognizes receptors. In this way, MNV appears to use capsid flexibility to present one face to the immune system and a completely different one to attack the host tissue. Therefore, it appears that even protein-shelled viruses have developed an impressive array of tricks to dodge our immune system and efficiently attack the host.
机译:蛋白质壳病毒被认为是“锡罐”,其仅将基因组货物从细胞中携带到细胞。然而,经过多年,已经清楚地清楚的是,鼻病毒和裂殖病毒等病毒是等待正确的环境提示的活性和动态结构,以将其基因组有效载荷传递给宿主细胞。在人鼻病毒的情况下,衣壳具有空洞,减少引起构象变化所需的能量,导致衣壳“呼吸”,当受体结合它以释放其基因组时等待衣壳。最引人注目的是,在此过程中,VP1和VP4的埋地N-Termini是瞬时暴露的。更新的“活”蛋白质衣壳的例子是小鼠诺罗病毒(MNV)。这种病毒系具有大的突出(P)结构域,通过单多肽系绳松散地连接到壳体上。在肠道中发现的小分子,例如胆汁盐,导致p域旋转和塌陷到壳表面上。同时,胆汁改变了P域本身与识别受体抗体的抗体的构象。以这种方式,MNV似乎使用衣壳的柔韧性来向免疫系统呈现一个面部和完全不同的,以攻击宿主组织。因此,似乎甚至蛋白质 - 壳病毒已经开发出令人印象深刻的技巧,以躲避我们的免疫系统并有效地攻击主机。

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