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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Age-Associated B Cells Express a Diverse Repertoire of V-H and V kappa Genes with Somatic Hypermutation
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Age-Associated B Cells Express a Diverse Repertoire of V-H and V kappa Genes with Somatic Hypermutation

机译:年龄相关的B细胞表达了具有体细胞高压的V-H和V kappa基因的各种曲目

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摘要

The origin and nature of age-associated B cells (ABCs) in mice are poorly understood. In this article, we show that their emergence required MHC class II and CD40/CD40L interactions. Young donor B cells were adoptively transferred into congenic recipients and allowed to remain for 1 mo in the absence of external Ag. B cells expressing the T-bet transcription factor, a marker for ABCs, were generated after multiple cell divisions from C57BL/6 donors but not from MHC class II- or CD40-deficient donors. Furthermore, old CD154 (CD40L)-deficient mice did not accrue ABCs, confirming that they arise primarily through T-dependent interactions. To determine what Igs ABCs express, we sequenced V-H and V kappa rearranged genes from unimmunized 22-mo-old C57BL/6 mice and showed that they had a heterogeneous repertoire, which was comparable to that seen in old follicular and marginal zone B cell subsets. However, in contrast to the follicular and marginal zone cells, ABCs displayed significant somatic hypermutation. The mutation frequency was lower than found in germinal center cells after deliberate immunization, suggesting that ABCs have undergone mild stimulation from endogenous Ags over time. These observations show that quiescent ABCs are Ag-experienced cells that accumulate during T cell-dependent responses to diverse Ags during the life of an individual.
机译:老鼠中的年龄相关的B细胞(ABC)的起源和性质是较差的。在本文中,我们表明他们的出现需要MHC II类和CD40 / CD40L相互作用。年轻的供体B细胞被用入先天受者转移,并在没有外部AG的情况下留下1 mo。在来自C57BL / 6供体的多个细胞分区之后,表达T-BET转录因子的B细胞是从C57BL / 6供体的多个细胞分裂后产生的,但不是来自MHC II类或CD40缺陷的供体。此外,旧的CD154(CD40L) - 缺少小鼠没有累积ABC,证实它们主要通过T依赖性相互作用来产生。为了确定什么IGS ABCS表达,我们测序VH和V Kappa重新排列的基因,来自无动于22-Mo-over C57bl / 6只小鼠,并显示它们具有异质的曲目,其与旧滤窗和边缘区域B细胞亚集合相当。然而,与滤饼和边缘区细胞相比,ABC显示出显着的体细胞增强次数。在故意免疫后,突变频率低于发生物细胞中发现,表明ABC随着时间的推移,ABCs对内源性AGS的轻度刺激。这些观察结果表明,静态ABC是经验丰富的细胞,其在T细胞依赖性响应期间积聚在个人的生命周期中的不同AGS。

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