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抗病毒反应的强度和时机决定了感染早期严重急性呼吸综合征冠状病毒2(SARS-CoV-2)的复制情况。

Magnitude and timing of the antiviral response determine SARS-CoV-2 replication early in infection.

作者信息

Cheemarla Nagarjuna R, Watkins Timothy A, Mihaylova Valia T, Wang Bao, Zhao Dejian, Wang Guilin, Landry Marie L, Foxman Ellen F

机构信息

Department of Laboratory Medicine, Yale School of Medicine, New Haven CT, U.S.A. 06520.

Department of Immunobiology, Yale School of Medicine, New Haven CT, U.S.A. 06520.

出版信息

medRxiv. 2021 Jan 27:2021.01.22.21249812. doi: 10.1101/2021.01.22.21249812.

Abstract

The interferon response is a potent antiviral defense mechanism, but its effectiveness depends on its timing relative to viral replication. Here, we report viral replication and host response kinetics in patients at the start of SARS-CoV-2 infection and explore the impact of these kinetics experimentally. In both longitudinal patient nasopharyngeal samples and airway epithelial organoids, we found that SARS-CoV-2 initially replicated exponentially with a doubling time of ~6hr, and induced interferon stimulated genes (ISGs) with delayed timing relative to viral replication. Prior exposure to rhinovirus increased ISG levels and blocked SARS-CoV-2 replication. Conversely, inhibiting ISG induction abrogated interference by rhinovirus and enhanced SARS-CoV-2 replication rate. These results demonstrate the importance of initial interferon-mediated defenses in determining the extent to which SARS-CoV-2 can replicate at the start of infection and indicate that biological variables that alter the airway interferon response, including heterologous induction of innate immunity by other viruses, could profoundly impact SARS-CoV-2 susceptibility and transmission.

摘要

干扰素反应是一种强大的抗病毒防御机制,但其有效性取决于其相对于病毒复制的时间。在此,我们报告了SARS-CoV-2感染初期患者的病毒复制和宿主反应动力学,并通过实验探索了这些动力学的影响。在纵向采集的患者鼻咽样本和气道上皮类器官中,我们发现SARS-CoV-2最初呈指数级复制,倍增时间约为6小时,并相对于病毒复制延迟诱导干扰素刺激基因(ISG)。先前接触鼻病毒会增加ISG水平并阻断SARS-CoV-2复制。相反,抑制ISG诱导可消除鼻病毒的干扰并提高SARS-CoV-2复制率。这些结果证明了初始干扰素介导的防御在确定SARS-CoV-2在感染初期能够复制的程度方面的重要性,并表明改变气道干扰素反应的生物学变量,包括其他病毒对先天免疫的异源诱导,可能会深刻影响SARS-CoV-2的易感性和传播。

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