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Geometric Mismatches within the Concentric Layers of Rotavirus Particles: a Potential Regulatory Switch of Viral Particle Transcription Activity

机译:轮状病毒颗粒同心层内的几何不匹配:病毒颗粒转录活性的潜在监管开关。

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摘要

Rotaviruses are prototypical double-stranded RNA viruses whose triple-layered icosahedral capsid constitutes transcriptional machinery activated by the release of the external layer. To understand the molecular basis of this activation, we studied the structural interplay between the three capsid layers by electron cryo-microscopy and digital image processing. Two viral particles and four virus-like particles containing various combinations of inner (VP2)-, middle (VP6)-, and outer (VP7)-layer proteins were studied. We observed that the absence of the VP2 layer increases the particle diameter and changes the type of quasi-equivalent icosahedral symmetry, as described by the shift in triangulation number (T) of the VP6 layer (from T = 13 to T = 19 or more). By fitting X-ray models of VP6 into each reconstruction, we determined the quasi-atomic structures of the middle layers. These models showed that the VP6 lattices, i.e., curvature and trimer contacts, are characteristic of the particle composition. The different functional states of VP6 thus appear as being characterized by trimers having similar conformations but establishing different intertrimeric contacts. Remarkably, the external protein VP7 reorients the VP6 trimers located around the fivefold axes of the icosahedral capsid, thereby shrinking the channel through which mRNA exits the transcribing rotavirus particle. We conclude that the constraints arising from the different geometries imposed by the external and internal layers of the rotavirus capsid constitute a potential switch regulating the transcription activity of the viral particles.
机译:轮状病毒是典型的双链RNA病毒,其三层二十面体衣壳构成了通过释放外层而激活的转录机制。为了了解这种激活的分子基础,我们通过电子冷冻显微镜和数字图像处理研究了三个衣壳层之间的结构相互作用。研究了两个病毒颗粒和四个病毒样颗粒,它们分别包含内层(VP2),中间层(VP6)和外层(VP7)蛋白的各种组合。我们观察到缺少VP2层会增加粒径并改变准等二十面体对称性的类型,如VP6层的三角剖分数(T)的变化(从T = 13到T = 19或更大)所描述)。通过将VP6的X射线模型拟合到每个重建中,我们确定了中间层的准原子结构。这些模型表明,VP6晶格,即曲率和三聚体接触是颗粒组成的特征。 VP6的不同功能状态因此表现为具有相似构象但建立了不同的三聚体接触的三聚体。值得注意的是,外部蛋白VP7重新定位了位于二十面体衣壳五倍轴周围的VP6三聚体,从而缩小了mRNA从转录轮状病毒颗粒中流出的通道。我们得出的结论是,由轮状病毒衣壳的外层和内层施加的不同几何形状引起的约束条件构成了调节病毒颗粒转录活性的潜在开关。

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