Center for Vaccine Research, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, United States of America.
Department of Microbiology and Molecular Genetics, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, United States of America.
PLoS Biol. 2023 Dec 21;21(12):e3002415. doi: 10.1371/journal.pbio.3002415. eCollection 2023 Dec.
Antibody titers that inhibit the influenza virus hemagglutinin (HA) from engaging its receptor are the accepted correlate of protection from infection. Many potent antibodies with broad, intra-subtype specificity bind HA at the receptor binding site (RBS). One barrier to broad H1-H3 cross-subtype neutralization is an insertion (133a) between positions 133 and 134 on the rim of the H1 HA RBS. We describe here a class of antibodies that overcomes this barrier. These genetically unrestricted antibodies are abundant in the human B cell memory compartment. Analysis of the affinities of selected members of this class for historical H1 and H3 isolates suggest that they were elicited by H3 exposure and broadened or diverted by later exposure(s) to H1 HA. RBS mutations in egg-adapted vaccine strains cause the new H1 specificity of these antibodies to depend on the egg adaptation. The results suggest that suitable immunogens might elicit 133a-independent, H1-H3 cross neutralization by RBS-directed antibodies.
能够抑制流感病毒血凝素 (HA) 与受体结合的抗体滴度被认为是预防感染的可靠指标。许多具有广谱、同亚型特异性的强效抗体可以结合 HA 的受体结合位点 (RBS)。广泛的 H1-H3 跨亚型中和的一个障碍是在 H1 HA RBS 边缘的 133 位和 134 位之间的插入(133a)。我们在这里描述了一类能够克服这一障碍的抗体。这些不受基因限制的抗体在人类 B 细胞记忆区大量存在。对该类别中选定成员对历史 H1 和 H3 分离株的亲和力分析表明,它们是由 H3 暴露引起的,并通过随后(多次)暴露于 H1 HA 而得到扩展或改变。在鸡蛋适应的疫苗株中 RBS 突变导致这些抗体的新 H1 特异性取决于鸡蛋的适应。结果表明,合适的免疫原可能通过 RBS 定向抗体诱导 133a 非依赖性的 H1-H3 交叉中和。
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