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Positive and negative selection shape the human naive B cell repertoire

机译:正面和负选择形状人类天真的B细胞曲目

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摘要

Although negative selection of developing B cells in the periphery is well described, yet poorly understood, evidence of naive B cell positive selection remains elusive. Using 2 humanized mouse models, we demonstrate that there was strong skewing of the expressed immunoglobulin repertoire upon transit into the peripheral naive B cell pool. This positive selection of expanded naive B cells in humanized mice resembled that observed in healthy human donors and was independent of autologous thymic tissue. In contrast, negative selection of autoreactive B cells required thymus-derived Tregs and MHC class II–restricted self-antigen presentation by B cells. Indeed, both defective MHC class II expression on B cells of patients with rare bare lymphocyte syndrome and prevention of self-antigen presentation via HLA-DM inhibition in humanized mice resulted in the production of autoreactive naive B cells. These latter observations suggest that Tregs repressed autoreactive naive B cells continuously produced by the bone marrow. Thus, a model emerged, in which both positive and negative selection shaped the human naive B cell repertoire and that each process was mediated by fundamentally different molecular and cellular mechanisms.
机译:虽然外围中的发育B细胞的阴性选择很好地描述,但尚未理解,朴素B细胞阳性选择的证据仍然难以捉摸。使用2种人源化的小鼠模型,我们证明在将表达的免疫球蛋白曲目中越强烈偏离进入外周幼稚B细胞库。这种在人源化小鼠中的扩增幼稚B细胞的阳性选择类似于在健康的人类供体中观察并与自体胸腺组织无关。相反,自身反应性B细胞的阴性选择需要B细胞所需的胸腺衍生的Tregs和MHC类II限制的自抗原呈递。实际上,在稀有裸淋巴细胞综合征的患者的B细胞上表达缺陷MHC II类表达和通过HLA-DM抑制在人源化的小鼠中预防自抗原呈递导致自身反应性幼稚B细胞的产生。后一种观察结果表明,通过骨髓连续产生的压抑自身反应性幼稚B细胞。因此,出现了一种模型,其中正和阴性选择成形为人幼稚B细胞曲目,并且每种方法是通过基本上不同的分子和细胞机制介导的。

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