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球形病毒颗粒组装的限制因素。

Constraints on the assembly of spherical virus particles.

作者信息

Rossmann M G

出版信息

Virology. 1984 Apr 15;134(1):1-11. doi: 10.1016/0042-6822(84)90267-8.

Abstract

Examination of protein structure shows that it is not possible to deform protein domains to the extent required by the Caspar-Klug quasi-symmetry surface lattices for the description of viral capsids (D. L. D. Caspar and A. Klug (1962). Cold Spring Harbor Symp. Quant. Biol. 27, 1-24). However, flexibility in proteins can be achieved by a number of ligand-induced events. One type of alteration is that of quaternary structural changes in oligomers. This strategy has been used by southern bean mosaic virus and tomato bushy stunt virus where dimers attain two different states in the assembled capsid. Alterations of subunit interactions can be induced by association with RNA, cations, or other oligomeric units and, hence, successful assembly results from a stepwise aggregation. The nature of the oligomers (dimers, trimers, or pentamers) must be the underlying reason for the occurrence of the Caspar-Klug lattices and the organization into icosahedra. An analysis of the surface lattices shows which types of oligomers will be necessary for assembly.

摘要

对蛋白质结构的研究表明,不可能将蛋白质结构域变形到卡斯帕 - 克卢格准对称表面晶格所要求的程度,以用于描述病毒衣壳(D. L. D. 卡斯帕和A. 克卢格(1962年)。《冷泉港定量生物学研讨会》27卷,第1 - 24页)。然而,蛋白质中的灵活性可以通过多种配体诱导事件来实现。一种类型的改变是寡聚体中四级结构的变化。南方菜豆花叶病毒和番茄丛生矮化病毒采用了这种策略,在组装好的衣壳中,二聚体达到两种不同的状态。亚基相互作用的改变可以由与RNA、阳离子或其他寡聚体单元的结合诱导,因此,成功的组装是由逐步聚集产生的。寡聚体(二聚体、三聚体或五聚体)的性质必定是卡斯帕 - 克卢格晶格出现以及形成二十面体结构的根本原因。对表面晶格的分析表明组装需要哪些类型的寡聚体。

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