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Immunoglobulin class switching appears to be regulated by B-cell antigen receptor-specific T-cell action

机译:免疫球蛋白类切换似乎由b细胞抗原针对受体t细胞的行动

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摘要

Antigen affinity is commonly viewed as the driving force behind the selection for dominant clonotypes that can occur during the T-cell-dependent processes of class switch recombination (CSR) and immune maturation. To test this view, we analyzed the variable gene repertoires of natural monoclonal antibodies to the hapten 2-phenyloxazolone (phOx) as well as those generated after phOx protein carrier-induced thymus-dependent or Ficoll-induced thymus-independent antigen stimulation. In contrast to expectations, the extent of IgM heterogeneity proved similar and many IgM from these three populations exhibited similar or even greater affinities than the classic Ox1 clonotype that dominates only after CSR among primary and memory IgG. The population of clones that were selected during CSR exhibited a reduced VH/VL repertoire that was enriched for variable domains with shorter and more uniform CDR-H3 lengths and almost completely stripped of variable domains encoded by the large VH1 family. Thus, contrary to the current paradigm, T-cell-dependent clonal selection during CSR appeared to select for VH family and CDR-H3 loop content even when the affinity provided by alternative clones exhibited similar to increased affinity for antigen.
机译:抗原亲和力通常被视为开车背后主要的选择clonotypes期间可能发生T-cell-dependent过程类开关复合(CSR)和免疫成熟。基因测试这一观点,我们分析了变量体验自然的单克隆抗体的半抗原2-phenyloxazolone (phOx)以及那些phOx后生成的蛋白质carrier-induced thymus-dependent或Ficoll-induced thymus-independent抗原刺激。IgM异质性程度相似从这三个群体表现出许多IgM相似或更大的亲和力比之后才经典Ox1 clonotype主导CSR在小学和记忆免疫球蛋白。在企业社会责任表现出的克隆选择减少VH /重要的曲目丰富变量域较短和更均匀CDR-H3长度和几乎完全剥夺了变量域编码VH1大家庭。因此,与当前的范式,在CSR T-cell-dependent克隆选择似乎选择VH家人和CDR-H3循环内容即使提供的亲和力选择克隆表现出类似的增加抗原的亲和力。

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