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婴儿和成人人类B细胞对轮状病毒的反应共享常见的免疫显性可变基因库。

Infant and adult human B cell responses to rotavirus share common immunodominant variable gene repertoires.

作者信息

Weitkamp Jörn-Hendrik, Kallewaard Nicole, Kusuhara Koichi, Bures Elizabeth, Williams John V, LaFleur Bonnie, Greenberg Harry B, Crowe James E

机构信息

Department of Pediatrics, Vanderbilt University Medical Center, Nashville, TN 37232-2581, USA.

出版信息

J Immunol. 2003 Nov 1;171(9):4680-8. doi: 10.4049/jimmunol.171.9.4680.

DOI:10.4049/jimmunol.171.9.4680
PMID:14568943
Abstract

Ab repertoires exhibit marked restrictions during fetal life characterized by biases of variable gene usage and lack of junctional diversity. We tested the hypothesis that Ab repertoire restriction contributes to the observed poor quality of specific Ab responses made by infants to viral infections. We analyzed the molecular determinants of B cell responses in humans to two Ags of rotavirus (RV), a common and clinically important infection of human infants. We sequenced Ab H and L chain V region genes (V(H) and V(L)) of clones expanded from single B cells responding to RV virus protein 6 or virus protein 7. We found that adults exhibited a distinct bias in use of gene segments in the V(H)1 and V(H)4 families, for example, V(H)1-46, V(H)4-31, and V(H)4-61. This gene segment bias differed markedly from the V(H)3 dominant bias seen in randomly selected adult B cells. Recombinant Abs incorporating any of those three immunodominant V(H) segments bound to RV-infected cells and also to purified RV particles. The RV-specific B cell repertoires of infants aged 2-11 mo and those of adults were highly related when compared by V(H), D, J(H), V(L), and J(L) segment selection, extent of junctional diversity, and mean H chain complementarity determining region 3 length. These data suggest that residual fetal bias of the B cell repertoire is not a limiting determinant of the quality of Ab responses to viruses of infants beyond the neonatal period.

摘要

在胎儿期,抗体库表现出明显的限制,其特征为可变基因使用的偏差和连接多样性的缺乏。我们检验了这样一个假说,即抗体库限制导致了婴儿对病毒感染产生的特异性抗体反应质量较差这一现象。我们分析了人类B细胞对两种轮状病毒(RV)抗原的反应的分子决定因素,RV是人类婴儿常见且具有临床重要性的感染源。我们对从响应RV病毒蛋白6或病毒蛋白7的单个B细胞扩增出的克隆的抗体重链和轻链V区基因(V(H)和V(L))进行了测序。我们发现,成年人在V(H)1和V(H)4家族的基因片段使用上表现出明显的偏差,例如V(H)1-46、V(H)4-31和V(H)4-61。这种基因片段偏差与在随机选择的成年B细胞中看到的V(H)3主导偏差明显不同。包含这三个免疫显性V(H)片段中任何一个的重组抗体都能与RV感染的细胞以及纯化的RV颗粒结合。通过V(H)、D基因、J(H)、V(L)和J(L)片段选择、连接多样性程度以及平均重链互补决定区3长度进行比较时,2至11个月大婴儿的RV特异性B细胞库与成年人的高度相关。这些数据表明,B细胞库的残留胎儿期偏差并不是新生儿期之后婴儿对病毒抗体反应质量的限制因素。

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