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Alternative Live-Attenuated Influenza Vaccines Based on Modifications in the Polymerase Genes Protect against Epidemic and Pandemic Flu

机译:基于聚合酶基因修饰的替代性活疫苗可预防流感和大流行性流感

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摘要

Human influenza is a seasonal disease associated with significant morbidity and mortality. Influenza vaccination is the most effective means for disease prevention. We have previously shown that mutations in the PB1 and PB2 genes of the live-attenuated influenza vaccine (LAIV) from the cold-adapted (ca) influenza virus A/Ann Arbor/6/60 (H2N2) could be transferred to avian influenza viruses and produce partially attenuated viruses. We also demonstrated that avian influenza viruses carrying the PB1 and PB2 mutations could be further attenuated by stably introducing a hemagglutinin (HA) epitope tag in the PB1 gene. In this work, we wanted to determine whether these modifications would also result in attenuation of a so-called triple reassortant (TR) swine influenza virus (SIV). Thus, the TR influenza A/swine/Wisconsin/14094/99 (H3N2) virus was generated by reverse genetics and subsequently mutated in the PB1 and PB2 genes. Here we show that a combination of mutations in this TR backbone results in an attenuated virus in vitro and in vivo. Furthermore, we show the potential of our TR backbone as a vaccine that provides protection against the 2009 swine-origin pandemic influenza H1N1 virus (S-OIV) when carrying the surface of a classical swine strain. We propose that the availability of alternative backbones to the conventional ca A/Ann Arbor/6/60 LAIV strain could also be useful in epidemic and pandemic influenza and should be considered for influenza vaccine development. In addition, our data provide evidence that the use of these alternative backbones could potentially circumvent the effects of original antigenic sin (OAS) in certain circumstances.
机译:人流感是与明显的发病率和死亡率相关的季节性疾病。流感疫苗接种是预防疾病的最有效手段。我们以前已经证明,来自冷适应的(ca)流感病毒A / Ann Arbor / 6/60(H2N2)的减毒活疫苗(LAIV)的PB1和PB2基因突变可以转移到禽流感病毒中并产生部分减毒的病毒。我们还证明,通过在PB1基因中稳定引入血凝素(HA)表位标签,可以进一步减轻携带PB1和PB2突变的禽流感病毒。在这项工作中,我们想确定这些修饰是否还会导致所谓的三重重组猪流感病毒(SIV)的减毒。因此,通过反向遗传学产生了TR流感A /猪/威斯康星州/威斯康星州/ 14094/99(H3N2)病毒,随后在PB1和PB2基因中发生了突变。在这里,我们显示此TR主干中的突变组合会在体外和体内导致减毒病毒。此外,我们展示了TR主链作为疫苗的潜力,该疫苗在携带经典猪株表面时可提供针对2009年猪源性大流行性流感H1N1病毒(S-OIV)的保护。我们建议,常规ca A / Ann Arbor / 6/60 LAIV株的替代主链的可用性也可能在流行和大流行性流感中有用,应考虑用于流感疫苗的开发。此外,我们的数据提供了证据,证明在某些情况下使用这些替代主链可能会避开原始抗原性罪过(OAS)的影响。

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