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A complex of influenza hemagglutinin with a neutralizing antibody that binds outside the virus receptor binding site

机译:流感血凝素与在病毒受体结合位点外结合的中和抗体的复合物

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The structure of a complex of influenza hemagglutinin (HA) with a neutralizing antibody shows that the antibody binds to HA at a distance from the virus receptor binding site. Comparison of the properties of this antibody and its Fab with those of an antibody that recognizes an epitope overlapping the receptor binding site leads to two main conclusions. First, inhibition of receptor binding is an important component of neutralization. Second, the efficiency of neutralization by the antibodies ranks in the same order as their avidities for HA, and their large size makes these antibodies highly efficient at neutralization, regardless of the location of their epitope in relation to the virus receptor binding site. These observations provide rationales for the range of antibody specificities that are detected in immune sera and for the distribution of sequence changes on the membrane-distal surface of influenza HAs that occur during `antigenic drift'.
机译:流感血凝素(HA)与中和抗体的复合物的结构表明,该抗体在距病毒受体结合位点一定距离处结合HA。将该抗体及其Fab的特性与识别与受体结合位点重叠的表位的抗体的特性进行比较,得出两个主要结论。首先,抑制受体结合是中和的重要组成部分。其次,抗体的中和效率与它们对HA的亲和力的排序顺序相同,并且它们的大尺寸使得这些抗体在中和时非常高效,而不论其表位相对于病毒受体结合位点的位置如何。这些观察结果为在免疫血清中检测到的抗体特异性范围和在“抗原漂移”过程中发生的流感HAs的膜远端表面上的序列变化分布提供了理论依据。

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