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首页> 外文期刊>Emerging Infectious Diseases >Association of Increased Receptor-Binding Avidity of Influenza A(H9N2) Viruses with Escape from Antibody-Based Immunity and Enhanced Zoonotic Potential
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Association of Increased Receptor-Binding Avidity of Influenza A(H9N2) Viruses with Escape from Antibody-Based Immunity and Enhanced Zoonotic Potential

机译:甲型H9N2流感病毒受体结合亲和力增加与基于抗体的免疫逃逸和人畜共患病潜力的关联

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We characterized 55 influenza A(H9N2) viruses isolated in Pakistan during 2014–2016 and found that the hemagglutinin gene is of the G1 lineage and that internal genes have differentiated into a variety of novel genotypes. Some isolates had up to 4-fold reduction in hemagglutination inhibition titers compared with older viruses. Viruses with hemagglutinin A180T/V substitutions conveyed this antigenic diversity and also caused up to 3,500-fold greater binding to avian-like and 20-fold greater binding to human-like sialic acid receptor analogs. This enhanced binding avidity led to reduced virus replication in primary and continuous cell culture. We confirmed that altered receptor-binding avidity of H9N2 viruses, including enhanced binding to human-like receptors, results in antigenic variation in avian influenza viruses. Consequently, current vaccine formulations might not induce adequate protective immunity in poultry, and emergence of isolates with marked avidity for human-like receptors increases the zoonotic risk.
机译:我们对2014-2016年在巴基斯坦分离出的55种甲型H9N2流感病毒进行了特征分析,发现血凝素基因属于G1谱系,内部基因已分化为多种新基因型。与旧病毒相比,某些分离株的血凝抑制效价降低了多达4倍。具有血凝素A180T / V取代的病毒传达了这种抗原多样性,并且还导致与禽样结合的结合力提高了3,500倍,与人样唾液酸受体类似物的结合力提高了20倍以上。这种增强的结合亲和力导致病毒在原代和连续细胞培养物中的复制减少。我们证实,H9N2病毒的受体结合亲和力发生了变化,包括与人样受体的结合增强,导致禽流感病毒发生抗原变异。因此,当前的疫苗制剂可能无法在家禽中诱导足够的保护性免疫力,并且对人样受体具有明显亲和力的分离株的出现增加了人畜共患病的风险。

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