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首页> 外文期刊>Mucosal immunology >Spatiotemporal interplay of severe acute respiratory syndrome coronavirus and respiratory mucosal cells drives viral dissemination in rhesus macaques
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Spatiotemporal interplay of severe acute respiratory syndrome coronavirus and respiratory mucosal cells drives viral dissemination in rhesus macaques

机译:严重急性呼吸系统综合症冠状病毒和呼吸道粘膜细胞的时空相互作用驱动猕猴的病毒传播

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Innate immune responses have a critical role in the control of early virus replication and dissemination. It remains unknown, however, how severe acute respiratory syndrome coronavirus (SARS-CoV) evades respiratory innate immunity to establish a systemic infection. Here we show in Chinese macaques that SARS-CoV traversed the mucosa through the respiratory tract within 2 days, resulting in extensive mucosal infiltration by T cells, MAC387(+), and CD163(+) monocytes/macrophages followed by limited viral replication in the lung but persistent viral shedding into the upper airway. Mucosal monocytes/macrophages sequestered virions in intracellular vesicles together with infected Langerhans cells and migrated into the tonsils and/or draining lymph nodes within 2 days. In lymphoid tissues, viral RNA and proteins were detected in infected monocytes upon differentiation into dendritic cells (DCs) within 3 days. Systemic viral dissemination was observed within 7 days. This study provides a comprehensive overview of the spatiotemporal interactions of SARS-CoV, monocytes/macrophages, and the DC network in mucosal tissues and highlights the fact that, while these innate cells contribute to viral clearance, they probably also serve as shelters and vehicles to provide a mechanism for the virus to escape host mucosal innate immunity and disseminate systemically.
机译:先天免疫应答在早期病毒复制和传播的控制中起着关键作用。但是,严重的急性呼吸系统综合症冠状病毒(SARS-CoV)如何逃避呼吸系统先天免疫以建立全身性感染仍是未知的。在这里,我们在中国的猕猴中显示,SARS-CoV在2天之内穿过呼吸道穿过粘膜,导致T细胞,MAC387(+)和CD163(+)单核细胞/巨噬细胞广泛地进入粘膜浸润,然后在病毒中复制受限肺,但病毒持续脱落进入上呼吸道。粘膜单核细胞/巨噬细胞与感染的朗格汉斯细胞一起隔离在细胞内囊泡中的病毒粒子,并在2天内迁移到扁桃体和/或引流淋巴结中。在淋巴样组织中,感染的单核细胞在3天内分化为树突状细胞(DC)后就检测到病毒RNA和蛋白质。在7天内观察到全身性病毒传播。这项研究全面概述了SARS-CoV,单核细胞/巨噬细胞和粘膜组织中DC网络的时空相互作用,并着重指出了以下事实:尽管这些先天细胞有助于病毒清除,但它们也可能充当避难所和媒介提供了一种病毒逃避宿主粘膜固有免疫力并全身传播的机制。

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