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Structural basis for biologically relevant mechanical stiffening of a virus capsid by cavity-creating or spacefilling mutations

机译:通过空洞形成或空间填充突变对病毒衣壳进行生物学相关的机械加固的结构基础

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摘要

Recent studies reveal that the mechanical properties of virus particles may have been shaped by evolution to facilitate virus survival. Manipulation of the mechanical behavior of virus capsids is leading to a better understanding of viral infection, and to the development of virus-based nanoparticles with improved mechanical properties for nanotechnological applications. In the minute virus of mice (MVM), deleterious mutations around capsid pores involved in infection-related translocation events invariably increased local mechanical stiffness and interfered with pore-associated dynamics. To provide atomic-resolution insights into biologically relevant changes in virus capsid mechanics, we have determined by X-ray crystallography the structural effects of deleterious, mechanically stiffening mutations around the capsid pores. Data show that the cavity-creating N170A mutation at the pore wall does not induce any dramatic structural change around the pores, but instead generates subtle rearrangements that propagate throughout the capsid, resulting in a more compact, less flexible structure. Analysis of the spacefilling L172W mutation revealed the same relationship between increased stiffness and compacted capsid structure. Implications for understanding connections between virus mechanics, structure, dynamics and infectivity, and for engineering modified virus-based nanoparticles, are discussed.
机译:最近的研究表明,病毒颗粒的机械特性可能已经通过进化形成,以促进病毒的生存。对病毒衣壳的机械行为的操纵导致人们对病毒感染有了更好的了解,并导致了具有改进的机械性能的基于病毒的纳米颗粒在纳米技术中的应用。在小鼠微小病毒(MVM)中,与感染相关的移位事件有关的衣壳孔周围的有害突变始终会增加局部机械刚度并干扰与孔相关的动力学。为了提供关于病毒衣壳力学中生物学相关变化的原子分辨率见解,我们通过X射线晶体学确定了衣壳孔周围有害的,机械变硬的突变的结构效应。数据显示,在孔壁处产生空腔的N170A突变不会引起孔周围任何显着的结构变化,而是会产生细微的重排,这些重排会传播到整个衣壳中,从而导致结构更紧凑,柔韧性更低。对空间填充的L172W突变的分析表明,增加的刚度和紧密的衣壳结构之间存在相同的关系。讨论了理解病毒力学,结构,动力学和感染性之间的联系以及工程改造基于病毒的纳米颗粒的意义。

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