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Altered virulence of Highly Pathogenic Avian Influenza (HPAI) H5N8 reassortant viruses in mammalian models

机译:哺乳动物模型中高致病性禽流感(HPAI)H5N8重配病毒的毒力改变

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ABSTRACT Recently identified highly pathogenic avian influenza (HPAI) H5N8 viruses (clade 2.3.4.4) are relatively low to moderately pathogenic in mammalian hosts compared with HPAI H5N1 viruses. In this study, we generated reassortant viruses comprised of A/MD/Korea/W452/2014(H5N8) with substitution of individual genes from A/EM/Korea/W149/2006(H5N1) to understand the contribution of each viral gene to virulence in mammals. Substituting the PB2 gene segment or the NA gene segment of the H5N8 virus by that from the H5N1 virus resulted in significantly enhanced pathogenicity compared with the parental H5N8 virus in mice. Of note, substitution of the PB2 gene segment of the H5N8 virus by that from the H5N1 virus resulted in a 1000-fold increase in virulence for mice compared with the parental virus (MLD50 decreased from 105.8 to 102.5 EID50). Further, the W452W149PB2 virus also induced the highest virus titers in lungs at all time points and the highest levels of inflammatory cytokine responses among all viruses tested. This high virulence phenotype was also confirmed by high viral titers in the respiratory tracts of infected ferrets. Further, a mini-genome assay revealed that W452W149PB2 has significantly increased polymerase activity (p < 0.001). Taken together, our study demonstrates that a single gene substitution from other avian influenza viruses can alter the pathogenicity of recent H5N8 viruses, and therefore emphasizes the need for intensive monitoring of reassortment events among co-circulating avian and mammalian viruses.
机译:摘要与HPAI H5N1病毒相比,最近鉴定出的高致病性禽流感(HPAI)H5N8病毒(2.3.4.4小节)在哺乳动物宿主中的致病性相对较低至中等。在这项研究中,我们产生了由A / MD / Korea / W452 / 2014(H5N8)组成的重配病毒,并替换了A / EM / Korea / W149 / 2006(H5N1)中的单个基因,以了解每种病毒基因对毒力的贡献在哺乳动物中。与小鼠中的亲代H5N8病毒相比,用H5N1病毒的PB2基因片段或NA基因片段替代H5N1病毒导致了更大的致病性。值得注意的是,用H5N1病毒替代PB5基因片段,与亲代病毒相比,小鼠的毒力增加了1000倍(MLD 50 从10 5.8 到10 2.5 EID 50 )。此外,在所有测试的病毒中,W452 W149PB2 病毒还在所有时间点诱导了最高的肺病毒滴度和最高的炎症细胞因子反应水平。这种高毒力表型也被感染的雪貂呼吸道中的高病毒滴度证实。此外,微型基因组分析显示W452 W149PB2 具有显着提高的聚合酶活性(p <0.001)。综上所述,我们的研究表明,从其他禽流感病毒中进行单个基因替代可以改变最近的H5N8病毒的致病性,因此强调需要对共同传播的禽和哺乳动物病毒之间的重配事件进行深入监控。

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