HK97 主要衣壳蛋白的三角洲结构域对衣壳组装是必需的。
The delta domain of the HK97 major capsid protein is essential for assembly.
机构信息
Department of Biological Sciences, University of Pittsburgh, Pittsburgh, PA 15260, USA.
Department of Biological Sciences, University of Pittsburgh, Pittsburgh, PA 15260, USA.
出版信息
Virology. 2014 May;456-457:171-8. doi: 10.1016/j.virol.2014.03.022. Epub 2014 Apr 10.
Abstract
The 102 residue N-terminal extension of the HK97 major capsid protein, the delta domain, is normally present during the assembly of immature HK97 procapsids, but it is removed during maturation like well-known internal scaffolding proteins of other tailed phages and herpesviruses. The delta domain also shares other unusual properties usually found in other viral and phage scaffolding proteins, including its location on the inside of the capsid, a high predicted and measured α-helical content, and an additional prediction for the ability to form parallel coiled-coils. Viral scaffolding proteins are essential for capsid assembly and phage viability, so we tested whether the HK97 delta domain was essential for capsid assembly. We studied the effects of deleting all or parts of the delta domain on capsid assembly and on complementation of capsid-protein-defective phage, and our results demonstrate that the delta domain is required for HK97 capsid assembly.
摘要
HK97 主要衣壳蛋白的 102 残基 N 端延伸部分,即 δ 结构域,在不成熟的 HK97 原衣壳组装过程中通常存在,但与其他有尾噬菌体和疱疹病毒中众所周知的内部支架蛋白一样,在成熟过程中会被去除。δ 结构域还具有其他通常在其他病毒和噬菌体支架蛋白中发现的不寻常特性,包括其位于衣壳内部、高预测和测量的α-螺旋含量,以及形成平行卷曲螺旋的额外预测能力。病毒支架蛋白对于衣壳组装和噬菌体存活至关重要,因此我们测试了 HK97 的 δ 结构域是否对衣壳组装至关重要。我们研究了删除 δ 结构域的全部或部分对衣壳组装和衣壳蛋白缺陷噬菌体的互补的影响,结果表明 δ 结构域是 HK97 衣壳组装所必需的。
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