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首页> 外文期刊>Scientific reports. >Amino acid substitutions V63I or A37S/I61T/V63I/V100A in the PA N-terminal domain increase the virulence of H7N7 influenza A virus
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Amino acid substitutions V63I or A37S/I61T/V63I/V100A in the PA N-terminal domain increase the virulence of H7N7 influenza A virus

机译:PA N末端结构域中的氨基酸取代V63I或A37S / I61T / V63I / V100A可提高H7N7甲型流感病毒的毒力

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摘要

The PA N-terminal domain (PA-Nter) is essential for viral transcription and replication. Here we identified PA-Nter substitutions A37S, I61T, V63I and V100A in recently emerged avian influenza A viruses (IAVs) with potential effect on virus pathogenicity and/or host adaptation. We introduced the identified PA-Nter substitutions into avian H7N7 IAV by reverse genetics. Our results showed that single substitution V63I and combined substitutions, I61T/V63I and A37S/I61T/V63I/V100A (Mfour), significantly increased virus growth capacity in mammalian cells. Meanwhile, these substitutions conferred higher virus transcription/replication capacity by producing more mRNA, cRNA and vRNA. Consistently, the polymerase activity and the endonuclease activity were enhanced by these PA-Nter substitutions. Notably, substitutions V63I and Mfour strongly increased virus replication and virulence in mice. Collectively, our findings demonstrated that the PA-Nter substitutions V63I and Mfour enhanced IAV pathogenicity through modification of the polymerase activity and the endonuclease activity, which added to the evolving knowledge of IAV virulence determinants.
机译:PA N末端结构域(PA-Nter)对于病毒转录和复制至关重要。在这里,我们在新近出现的禽流感A病毒(IAV)中鉴定了PA-Nter替代品A37S,I61T,V63I和V100A,它们对病毒的致病性和/或宿主适应性具有潜在影响。我们通过反向遗传学将鉴定出的PA-Nter取代引入禽类H7N7 IAV中。我们的结果表明,单取代V63I和组合取代I61T / V63I和A37S / I61T / V63I / V100A(Mfour),显着提高了哺乳动物细胞中的病毒生长能力。同时,这些替代通过产生更多的mRNA,cRNA和vRNA赋予更高的病毒转录/复制能力。一致地,通过这些PA-Nter取代增强了聚合酶活性和核酸内切酶活性。值得注意的是,取代V63I和Mfour大大增强了小鼠中的病毒复制和毒力。总的来说,我们的研究结果表明,PA-Nter取代V63I和Mfour通过修饰聚合酶活性和核酸内切酶活性增强了IAV的致病性,这增加了IAV毒力决定簇的知识。

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