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Sequencing Antibody Repertoires Provides Evidence for Original Antigenic Sin Shaping the Antibody Response to Influenza Vaccination

机译:测序抗体库为原始抗原罪提供了对流感疫苗免疫抗体反应的证据

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摘要

We used a DNA barcoding method to enable high-throughput sequencing of the cognate heavy- and light-chain pairs of expressed antibodies. We used this approach to elucidate the plasmablast antibody response to influenza vaccination. We show that >75% of the rationally selected plasmablast antibodies bind and neutralize influenza, and that antibodies from clonal families, defined by sharing both heavy chain VJ and light chain VJ sequence usage, do so most effectively. Vaccine-induced heavy chain VJ regions contained on average >20 nucleotide mutations as compared to their predicted germline gene sequences, and some vaccine-induced antibodies exhibited higher binding affinities for hemagglutinins derived from prior years’ seasonal influenza as compared to their affinities for the immunization strains. Our results show that influenza vaccination induces the recall of memory B cells that express antibodies that previously underwent affinity maturation against prior years’ seasonal influenza, suggesting that ‘original antigenic sin’ shapes the antibody response to influenza vaccination.
机译:我们使用了一种DNA条形码方法来实现表达抗体的同源重链和轻链对的高通量测序。我们使用这种方法来阐明浆母细胞抗体对流感疫苗的反应。我们显示,超过75%的合理选择的成浆细胞抗体结合并中和了流感,并且通过共享重链VJ和轻链VJ序列使用而定义的来自克隆家族的抗体能最有效地做到这一点。疫苗诱导的重链VJ区域与其预测的种系基因序列相比平均包含> 20个核苷酸突变,并且某些疫苗诱导的抗体与前几年季节性流感衍生的血凝素相比具有更高的结合亲和力株。我们的结果表明,流感疫苗接种可诱导记忆B细胞的召回,这些细胞表达的抗体先前已针对前几年的季节性流感进行了亲和力成熟,这表明“原始抗原性罪魁祸首”决定了对流感疫苗接种的抗体反应。

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