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Influenza hemagglutinin protein stability activation and pandemic risk

机译:流感血凝素蛋白的稳定性活化性和大流行风险

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摘要

For decades, hemagglutinin (HA) protein structure and its refolding mechanism have served as a paradigm for understanding protein-mediated membrane fusion. HA trimers are in a high-energy state and are functionally activated by low pH. Over the past decade, HA stability (or the pH at which irreversible conformational changes are triggered) has emerged as an important determinant in influenza virus host range, infectivity, transmissibility, and human pandemic potential. Here, we review HA protein structure, assays to measure its stability, measured HA stability values, residues and mutations that regulate its stability, the effect of HA stability on interspecies adaptation and transmissibility, and mechanistic insights into this process. Most importantly, HA stabilization appears to be necessary for adapting emerging influenza viruses to humans.
机译:数十年来,血凝素(HA)的蛋白质结构及其重折叠机制已成为理解蛋白质介导的膜融合的范例。 HA三聚体处于高能状态,并被低pH值功能激活。在过去的十年中,HA稳定性(或引发不可逆构象变化的pH值)已成为流感病毒宿主范围,传染性,传播性和人类大流行潜力的重要决定因素。在这里,我们审查了HA蛋白质的结构,测定其稳定性的方法,测得的HA稳定性值,调节其稳定性的残基和突变,HA稳定性对种间适应性和可传递性的影响以及对该过程的机理性见解。最重要的是,HA稳定似乎是使新兴流感病毒适应人类所必需的。

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