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首页> 外文期刊>Journal of the Mechanics and Physics of Solids >Elasticity theory of the maturation of viral capsids
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Elasticity theory of the maturation of viral capsids

机译:病毒衣壳成熟的弹性理论

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摘要

Many viral capsids undergo a series of significant structural changes following assembly, a process known as maturation. The driving mechanisms for maturation usually are chemical reactions taking place inside the proteins that constitute the capsid ("subunits") that produce structural changes of the subunits. The resulting alterations of the subunits may be directly visible from the capsid structures, as observed by electron microscopy, in the form of a shear shape change and/or a rotation of groups of subunits. The existing thin shell elasticity theory for viral shells does not take account of the internal structure of the subunits and hence cannot describe displacement patterns of the capsid during maturation. Recently, it was proposed for the case of a particular virus (HK97) that thin shell elasticity theory could in fact be generalized to include transformations of the constituent proteins by including such a transformations as a change of the stress-free reference state for the deformation free energy. In this study, we adopt that approach and illustrate its validity in more generality by describing shape changes occurring during maturation across different T-numbers in terms of subunit shearing. Using phase diagrams, we determine the shear directions of the subunits that are most effective to produce capsid shape changes, such as transitions from spherical to facetted capsid shape. We further propose an equivalent stretching mechanism offering a unifying view under which capsid symmetry can be analyzed. We conclude by showing that hexamer shearing not only drives the shape change of the viral capsid during maturation but also is capable of lowering the capsid elastic energy in particular for chiral capsids (e.g., T = 7) and give rise to pre-shear patterns. These additional mechanisms may provide a driving force and an organizational principle for virus assembly.
机译:许多病毒衣壳在组装后经历了一系列显着的结构变化,这一过程称为成熟。成熟的驱动机制通常是发生在构成衣壳(“亚基”)的蛋白质内部发生的化学反应,其产生亚基的结构变化。如通过电子显微镜观察,可以通过衣壳结构以剪切形状变化和/或亚单位群的旋转的形式直接从衣壳结构中看到亚单位的所得改变。现有的用于病毒壳的薄壳弹性理论没有考虑亚基的内部结构,因此不能描述成熟过程中衣壳的位移模式。最近,对于一种特定的病毒(HK97),有人提出,薄壳弹性理论实际上可以推广到包括组成蛋白质的转化,方法是包括诸如变形的无应力参考状态的改变。自由能。在这项研究中,我们采用该方法并通过描述在亚单位剪切方面跨不同T数在成熟过程中发生的形状变化来更普遍地说明其有效性。使用相图,我们确定最有效地产生衣壳形状变化(例如从球形到多面衣壳形状的过渡)的子单元的剪切方向。我们进一步提出了一种等效的拉伸机制,该机制提供了一个统一的视图,在该视图下可以分析衣壳对称性。我们通过显示六聚体剪切不仅得出结论,不仅驱动成熟过程中病毒衣壳的形状变化,而且还能够降低衣壳的弹性能,特别是对于手性衣壳(例如T = 7)并产生预剪切模式。这些额外的机制可以为病毒组装提供动力和组织原则。

著录项

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  • 作者单位

    Mechanical and Aerospace Engineering Department, University of California, Los Angeles, CA 90095, United States;

    Mechanical and Aerospace Engineering Department, University of California, Los Angeles, CA 90095, United States,Institute for Computational Engineering & Sciences, University of Texas at Austin, TX 78712, United States;

    Physics and Astronomy Department, University of California, Los Angeles, CA 90095, United States;

    Physics and Astronomy Department, University of California, Los Angeles, CA 90095, United States;

    Mechanical and Aerospace Engineering Department, University of California, Los Angeles, CA 90095, United States;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    Conformational changes; Buckling transition; Reference configuration; Virus maturation; Virus assembly;

    机译:构象变化;屈曲过渡参考配置;病毒成熟;病毒组装;

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