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携带 Nano-Luciferase 表达的重组鼠样轮状病毒揭示了组织嗜性、复制动态和病毒传播。

A recombinant murine-like rotavirus with Nano-Luciferase expression reveals tissue tropism, replication dynamics, and virus transmission.

机构信息

Department of Molecular Microbiology, Washington University School of Medicine, St. Louis, MO, United States.

Veterans Affairs (VA) Palo Alto Health Care System, Department of Veterans Affairs, Palo Alto, CA, United States.

出版信息

Front Immunol. 2022 Jul 29;13:911024. doi: 10.3389/fimmu.2022.911024. eCollection 2022.

Abstract

Rotaviruses (RVs) are one of the main causes of severe gastroenteritis, diarrhea, and death in children and young animals. While suckling mice prove to be highly useful small animal models of RV infection and pathogenesis, direct visualization tools are lacking to track the temporal dynamics of RV replication and transmissibility . Here, we report the generation of the first recombinant murine-like RV that encodes a Nano-Luciferase reporter (NLuc) using a newly optimized RV reverse genetics system. The NLuc-expressing RV was replication-competent in cell culture and both infectious and virulent in neonatal mice . Strong luciferase signals were detected in the proximal and distal small intestines, colon, and mesenteric lymph nodes. We showed, a noninvasive imaging system, that RV intestinal replication peaked at days 2 to 5 post infection. Moreover, we successfully tracked RV transmission to uninoculated littermates as early as 3 days post infection, 1 day prior to clinically apparent diarrhea and 3 days prior to detectable fecal RV shedding in the uninoculated littermates. We also observed significantly increased viral replication in knockout mice that lack the host interferon signaling. Our results suggest that the NLuc murine-like RV represents a non-lethal powerful tool for the studies of tissue tropism and host and viral factors that regulate RV replication and spread, as well as provides a new tool to facilitate the testing of prophylactic and therapeutic interventions in the future.

摘要

轮状病毒(RV)是导致儿童和幼小动物严重胃肠炎、腹泻和死亡的主要原因之一。虽然哺乳期小鼠被证明是研究 RV 感染和发病机制的高度有用的小型动物模型,但缺乏直接可视化工具来跟踪 RV 复制和传染性的时间动态。在这里,我们报告了第一个使用新优化的 RV 反向遗传学系统编码 Nano-Luciferase 报告基因(NLuc)的重组鼠样 RV 的产生。该 NLuc 表达的 RV 在细胞培养中具有复制能力,并且在新生小鼠中具有感染性和毒力。在近端和远端小肠、结肠和肠系膜淋巴结中检测到强烈的荧光素酶信号。我们使用非侵入性成像系统表明,RV 肠道复制在感染后第 2 至 5 天达到峰值。此外,我们成功地跟踪了 RV 向未接种的同窝幼鼠的传播,早在感染后第 3 天,即在临床明显腹泻之前 1 天和未接种的同窝幼鼠中可检测到粪便 RV 脱落之前 3 天。我们还观察到在缺乏宿主干扰素信号的 knockout 小鼠中,病毒复制显著增加。我们的结果表明,该 NLuc 鼠样 RV 是一种非致死性的强大工具,可用于研究组织嗜性以及宿主和病毒因素,这些因素调节 RV 复制和传播,同时为未来促进预防性和治疗性干预措施的测试提供了新工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/327c/9372724/0bca88805cd4/fimmu-13-911024-g001.jpg

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