克隆内竞争抑制高亲和力抗体分泌细胞的形成。
Intraclonal competition inhibits the formation of high-affinity antibody-secreting cells.
作者信息
Le Thuc-vy L, Kim Tea Hyun, Chaplin David D
机构信息
Department of Microbiology, University of Alabama at Birmingham, Birmingham, AL 35294, USA.
出版信息
J Immunol. 2008 Nov 1;181(9):6027-37. doi: 10.4049/jimmunol.181.9.6027.
Abstract
Protective immunity requires a diverse, polyclonal B cell repertoire. We demonstrate that affinity maturation of the humoral response to a hapten is impaired when preexisting clonally restricted cells recognizing the hapten are dominant in the B cell repertoire. B1-8i(+/-) mice, which feature a high frequency of B cells with nitrophenyl (NP)-binding specificity, respond to NP-haptenated proteins with the production of NP-specific Abs, but affinity maturation is impaired due to insufficient generation of high-affinity Ab-producing cells. We manipulated the frequency of NP-specific B cells by adoptive transfer of B1-8 B cells into naive, wild-type recipients. Remarkably, when 10(4) B1-8 B cells were transferred, these cells supported efficient affinity maturation and plasma cell differentiation. In contrast, when 10(6) B1-8 cells were transferred, affinity maturation did not occur. These data indicate that restricting the frequency of clonally related B cells is required to support affinity maturation.
摘要
保护性免疫需要多样化的多克隆B细胞库。我们证明,当预先存在的识别半抗原的克隆受限细胞在B细胞库中占主导地位时,对半抗原的体液反应的亲和力成熟会受到损害。B1-8i(+/-)小鼠具有高频率的具有硝基苯基(NP)结合特异性的B细胞,对NP-半抗原化蛋白产生NP特异性抗体,但由于高亲和力抗体产生细胞的生成不足,亲和力成熟受到损害。我们通过将B1-8 B细胞过继转移到幼稚的野生型受体中来操纵NP特异性B细胞的频率。值得注意的是,当转移10^4个B1-8 B细胞时,这些细胞支持有效的亲和力成熟和浆细胞分化。相反,当转移10^6个B1-8细胞时,未发生亲和力成熟。这些数据表明,限制克隆相关B细胞的频率是支持亲和力成熟所必需的。
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