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PB2和PA突变在哺乳动物模型中对适应小鼠的pdmH1N1-金星报告基因甲型流感病毒的致病性有影响。

PB2 and PA mutations contribute to the pathogenicity of mouse-adapted pdmH1N1-Venus reporter influenza A virus in a mammalian model.

作者信息

Wu Shixiang, Yi Ruonan, Tao Yingying, Wu Huimin, Wu Li, Song Jiasheng, Zhang Xin, Yang Beibei, Wu Xing, He Yulong, Shu Jianhong, Feng Huapeng

机构信息

Department of Biopharmacy, College of Life Sciences and Medicine, Zhejiang Sci-Tech University, Hangzhou, China.

Department of Biology, College of Life Sciences, China Jiliang University, Hangzhou, China.

出版信息

Front Microbiol. 2025 Jan 7;15:1532304. doi: 10.3389/fmicb.2024.1532304. eCollection 2024.

Abstract

Influenza A viruses have been a threat to human health for the past 100 years. Understanding the dynamics and pathogenicity of the influenza viruses is of great value in controlling the influenza pandemic. Fluorescent protein-carrying recombinant influenza virus is a substantially useful tool for studying viral characteristics and high-throughput screening . In this study, we generated a recombinant pdmH1N1 CA04 influenza virus carrying a Venus reporter gene in the non-structural (NS) segment using reverse genetics. After passaging the recombinant influenza virus carrying Venus from lung to lung in mice, we found that virulence of the passaged pdmH1N1 CA04-Venus significantly increased and was lethal to the mice. We finally isolated one mouse-adapted pdmH1N1 CA04-Venus with bigger plaques expressing the amount of Venus proteins by using the ninth passage lung homogenate with plague purification. We found three different amino acids (PB2 T340K, PA I21M, and F175L) between WT-CA04-Venus and MA-CA04-Venus using whole-genome sequencing. Interestingly, the polymerase activity of MA-CA04-Venus was significantly lower than that of WT-CA04-Venus in a minigenome assay. Further investigation demonstrates that PA I21M and PA I21M + PB2 T340K significantly enhanced the polymerase activity of WT-CA04-Venus; however, PA F175L + PB2 T340K significantly decreased the polymerase activity of MA-CA04-Venus. Therefore, PA I21M mutation may determine the increased virulence in mice, and PA F175L + PB2 T340K may be involved in the stability of Venus insertion. Above all, we generated a mouse-adapted pdmH1N1 CA04-Venus virus with high virulence and stable green fluorescent Venus protein. It is a useful tool for high-throughput screening of antiviral drugs and for investigating the interaction between the influenza virus and host .

摘要

在过去的100年里,甲型流感病毒一直威胁着人类健康。了解流感病毒的动态和致病性对于控制流感大流行具有重要价值。携带荧光蛋白的重组流感病毒是研究病毒特性和高通量筛选的重要工具。在本研究中,我们利用反向遗传学技术构建了一种在非结构(NS)片段携带金星报告基因的重组pdmH1N1 CA04流感病毒。将携带金星的重组流感病毒在小鼠肺内传代后,我们发现传代后的pdmH1N1 CA04-金星的毒力显著增加,并对小鼠具有致死性。我们最终通过使用第九代肺匀浆进行噬斑纯化,分离出一株具有更大噬斑、表达金星蛋白量的适应小鼠的pdmH1N1 CA04-金星。通过全基因组测序,我们在野生型CA04-金星和适应小鼠型CA04-金星之间发现了三个不同的氨基酸(PB2 T340K、PA I21M和F175L)。有趣的是,在微型基因组试验中,适应小鼠型CA04-金星的聚合酶活性显著低于野生型CA04-金星。进一步研究表明,PA I21M和PA I21M + PB2 T340K显著增强了野生型CA04-金星的聚合酶活性;然而,PA F175L + PB2 T340K显著降低了适应小鼠型CA04-金星的聚合酶活性。因此,PA I21M突变可能决定了小鼠毒力的增加,而PA F175L + PB2 T340K可能参与了金星插入的稳定性。最重要的是,我们构建了一种具有高毒力和稳定绿色荧光金星蛋白的适应小鼠的pdmH1N1 CA04-金星病毒。它是高通量筛选抗病毒药物以及研究流感病毒与宿主相互作用的有用工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1119/11747394/3324de505f4a/fmicb-15-1532304-g001.jpg

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