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Specific In Vivo Deletion of B-Cell Subpopulations Expressing Human Immunoglobulins by the B-Cell Superantigen Protein L

机译:B细胞超抗原蛋白L特异性表达人免疫球蛋白的B细胞亚群的体内缺失

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摘要

Some pathogens have evolved to produce proteins, called B-cell superantigens, that can interact with human immunoglobulin variable regions, independently of the combining site, and activate B lymphocytes that express the target immunoglobulins. However, the in vivo consequences of these interactions on human B-cell numbers and function are largely unknown. Using transgenic mice expressing fully human immunoglobulins, we studied the consequences of in vivo exposure of protein L of Peptostreptococcus magnus with human immunoglobulins. In the mature pool of B cells, protein L exposure resulted in a specific reduction of splenic marginal-zone B cells and peritoneal B-1 cells. Splenic B cells exhibited a skewed light-chain repertoire consistent with the capacity of protein L to bind specific kappa gene products. Remarkably, these two B-cell subsets are implicated in innate B-cell immunity, allowing rapid clearance of pathogens. Thus, the present study reveals a novel mechanism that may be used by some infectious agents to subvert a first line of the host's immune defense.
机译:一些病原体已经进化为产生称为B细胞超抗原的蛋白质,该蛋白质可以与人免疫球蛋白可变区相互作用,而独立于结合位点,并激活表达目标免疫球蛋白的B淋巴细胞。但是,这些相互作用对人B细胞数量和功能的体内影响在很大程度上尚不清楚。使用表达完全人类免疫球蛋白的转基因小鼠,我们研究了人类免疫球蛋白在体内暴露于大肠肽链球菌蛋白L的后果。在成熟的B细胞库中,蛋白质L暴露导致脾边缘区B细胞和腹膜B-1细胞的特异性减少。脾脏B细胞显示出与蛋白质L结合特定κ基因产物的能力一致的偏斜的轻链库。值得注意的是,这两个B细胞亚群与先天B细胞免疫力有关,可以快速清除病原体。因此,本研究揭示了一种新颖的机制,该机制可被某些感染因子用来颠覆宿主免疫防御的第一线。

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