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A novel sequence-based antigenic distance measure for H1N1, with application to vaccine effectiveness and the selection of vaccine strains

机译:一种新型的基于序列的H1N1抗原距离测定方法,用于疫苗有效性和疫苗株的选择

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摘要

H1N1 influenza causes substantial seasonal illness and was the subtype of the 2009 influenza pandemic. Precise measures of antigenic distance between the vaccine and circulating virus strains help researchers design influenza vaccines with high vaccine effectiveness. We here introduce a sequence-based method to predict vaccine effectiveness in humans. Historical epidemiological data show that this sequence-based method is as predictive of vaccine effectiveness as hemagglutination inhibition assay data from ferret animal model studies. Interestingly, the expected vaccine effectiveness is greater against H1N1 than H3N2, suggesting a stronger immune response against H1N1 than H3N2. The evolution rate of hemagglutinin in H1N1 is also shown to be greater than that in H3N2, presumably due to greater immune selection pressure.
机译:H1N1流感导致严重的季节性疾病,是2009年流感大流行的亚型。精确测量疫苗与正在传播的病毒株之间的抗原距离,有助于研究人员设计出具有很高疫苗效力的流感疫苗。我们在这里介绍一种基于序列的方法来预测人类疫苗的有效性。历史流行病学数据表明,这种基于序列的方法与雪貂动物模型研究中的血凝抑制试验数据一样,可预测疫苗的有效性。有趣的是,针对H1N1的预期疫苗效力要比针对H3N2的效力高,这表明针对H1N1的免疫应答要强于H3N2。还显示H1N1中血凝素的进化速率比H3N2中的高,这可能是由于更高的免疫选择压力所致。

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