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SARS-CoV-2 variants with NSP12 P323L/G671S mutations display enhanced virus replication in ferret upper airways and higher transmissibility

机译:具有 NSP12 P323L/G671S 突变的 SARS-CoV-2 变体在雪貂上呼吸道中的病毒复制增强,传播性更高

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With the emergence of multiple predominant SARS-CoV-2 variants, it becomes important to have a comprehensive assessment of their viral fitness and transmissibility. Here, we demonstrate that natural temperature differences between the upper (33 DEG;C) and lower (37 DEG;C) respiratory tract have profound effects on SARS-CoV2 replication and transmissibility. Specifically, SARS-CoV-2 variants containing the NSP12 mutations P323L or P323L/G671S exhibit enhanced RNA-dependent RNA polymerase (RdRp) activity at 33 DEG;C compared with 37 DEG;C and high transmissibility. Molecular dynamics simulations and microscale thermophoresis demonstrate that the NSP12 P323L and P323L/G671S mutations stabilize the NSP12-NSP7-NSP8 complex through hydrophobic effects, leading to increased viral RdRp activity. Furthermore, competitive transmissibility assay reveals that reverse genetic (RG)-P323L or RG-P323L/G671S NSP12 outcompetes RG-WT (wild-type) NSP12 for replication in the upper respiratory tract, allowing markedly rapid transmissibility. This suggests that NSP12 P323L or P323L/G671S mutation of SARS-CoV-2 is associated with increased RdRp complex stability and enzymatic activity, promoting efficient transmissibility.
机译:随着多种主要 SARS-CoV-2 变体的出现,对其病毒适应性和传播性进行全面评估变得非常重要。在这里,我们证明了上部(33&°C;C)及以下(37°C;C)呼吸道对SARS-CoV2的复制和传播有深远的影响。具体来说,含有 NSP12 突变 P323L 或 P323L/G671S 的 SARS-CoV-2 变体在 33 和 DEG 时表现出增强的 RNA 依赖性 RNA 聚合酶 (RdRp) 活性;C与37&DEG相比;C、传播性高。分子动力学模拟和微尺度热泳表明,NSP12、P323L和P323L/G671S突变通过疏水效应稳定NSP12-NSP7-NSP8复合物,导致病毒RdRp活性增加。此外,竞争性传播性测定表明,反向遗传 (RG)-P323L 或 RG-P323L/G671S NSP12 在上呼吸道复制方面优于 RG-WT(野生型)NSP12,从而实现显着快速的传播性。这表明 SARS-CoV-2 的 NSP12 P323L 或 P323L/G671S 突变与 RdRp 复合物稳定性和酶活性增加有关,从而促进有效的传播性。

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