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Glycan receptor binding of the influenza A Virus H7N9 hemagglutinin

机译:甲型流感病毒H7N9血凝素的聚糖受体结合

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Summary The advent of H7N9 in early 2013 is of concern for a number of reasons, including its capability to infect humans, the lack of clarity in the etiology of infection, and because the human population does not have pre-existing immunity to the H7 subtype. Earlier sequence analyses of H7N9 hemagglutinin (HA) point to amino acid changes that predicted human receptor binding and impinge on the antigenic characteristics of the HA. Here, we report that the H7N9 HA shows limited binding to human receptors; however, should a single amino acid mutation occur, this would result in structural changes within the receptor binding site that allow for extensive binding to human receptors present in the upper respiratory tract. Furthermore, a subset of the H7N9 HA sequences demarcating coevolving amino acids appears to be in the antigenic regions of H7, which, in turn, could impact effectiveness of the current WHO-recommended prepandemic H7 vaccines.
机译:总结由于许多原因,H7N9的出现在2013年初引起了人们的关注,其中包括其感染人类的​​能力,感染病因缺乏明确性,以及由于人类人群对H7亚型没有预先存在的免疫力。 H7N9血凝素(HA)的早期序列分析指出了预测人类受体结合并影响HA抗原特性的氨基酸变化。在这里,我们报道了H7N9 HA对人类受体的结合有限;但是,如果发生单个氨基酸突变,则将导致受体结合位点内部发生结构变化,从而允许与上呼吸道中存在的人类受体广泛结合。此外,划定共同进化氨基酸的H7N9 HA序列的一个子集似乎在H7的抗原区域中,这反过来又可能影响当前WHO推荐的大流行前H7疫苗的有效性。

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