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H5N1 vaccine-elicited memory B cells are genetically constrained by the IGHV locus in the recognition of a neutralizing epitope in the HA stem

机译:H5N1疫苗引起的记忆B细胞受到IGHV基因座的遗传限制以识别HA茎中的中和表位

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摘要

Due to significant viral diversity, vaccines that elicit durable and broad protection against influenza have been elusive. Recent research has focused on the potential of highly conserved regions of the viral hemagglutinin (HA) as targets for broadly neutralizing antibody responses. Antibodies that bind the highly conserved stem or stalk of HA can be elicited by vaccination in humans and animal models and neutralize diverse influenza strains. However, the frequency and phenotype of HA stem-specific B cells in vivo remains unclear. Here we characterize HA stem-specific B cell responses following H5N1 vaccination and describe the re-expansion of a pre-existing population of memory B cells specific for stem epitopes. This population utilizes primarily, but not exclusively, IGHV1-69-based immunoglobulins for HA recognition. However within some subjects, allelic polymorphism at the ighv1-69 locus can limit IGHV1-69 immunodominance and may reduce circulating frequencies of stem-reactive B cells in vivo. The accurate definition of allelic selection, recombination requirements and ontogeny of neutralizing antibody responses to influenza will aid rational influenza vaccine design.
机译:由于显着的病毒多样性,难以获得针对流感的持久和广泛保护的疫苗。最近的研究集中在高度保守的病毒血凝素(HA)区域作为广泛中和抗体反应的靶标上的潜力。可以通过在人和动物模型中接种疫苗来诱导结合高度保守的HA茎或茎的抗体,并中和各种流感病毒株。但是,体内HA干特异性B细胞的频率和表型仍不清楚。在这里,我们表征接种H5N1疫苗后的HA干细胞特异性B细胞应答,并描述针对干表位的记忆B细胞种群的重新扩展。该人群主要但非唯一地使用基于IGHV1-69的免疫球蛋白进行HA识别。但是,在某些受试者中,ighv1-69基因座的等位基因多态性可以限制IGHV1-69的免疫优势,并可能降低体内干反应性B细胞的循环频率。准确定义等位基因选择,重组要求和中和抗体对流感病毒的反应,将有助于合理设计流感疫苗。

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