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Discrete fracture patterns of virus shells reveal mechanical building blocks

机译:病毒壳的离散断裂模式揭示了机械构件

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摘要

Viral shells are self-assembled protein nanocontainers with remarkable material properties. They combine simplicity of construction with toughness and complex functionality. These properties make them interesting for bionanotechnology. To date we know little about how virus structure determines assembly pathways and shell mechanics. We have here used atomic force microscopy to study structural failure of the shells of the bacteriophage Φ29. We observed rigidity patterns following the symmetry of the capsid proteins. Under prolonged force exertion, we observed fracture along well-defined lines of the 2D crystal lattice. The mechanically most stable building block of the shells was a trimer. Our approach of “reverse engineering” the virus shells thus made it possible to identify stable structural intermediates. Such stable intermediates point to a hierarchy of interactions among equal building blocks correlated with distinct next-neighbor interactions. The results also demonstrate that concepts from macroscopic materials science, such as fracture, can be usefully employed in molecular engineering.
机译:病毒壳是具有出色材料特性的自组装蛋白纳米容器。它们结合了结构的简单性,韧性和复杂的功能。这些特性使它们对于生物纳米技术很有趣。迄今为止,我们对病毒结构如何决定组装途径和外壳机理的了解甚少。在这里,我们使用原子力显微镜研究了噬菌体Φ29的壳的结构破坏。我们观察到衣壳蛋白的对称性后的刚性模式。在长时间施加力的情况下,我们观察到沿2D晶格清晰定义的线的断裂。壳的机械上最稳定的组成部分是三聚体。因此,我们“逆向工程”病毒外壳的方法使鉴定稳定的结构中间体成为可能。这种稳定的中间体指向与独特的下一个邻居互动相关的相等构件之间的互动层次。结果还证明,宏观材料科学的概念(例如断裂)可以有效地应用于分子工程。

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