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The influence of BCR density on the differentiation of natural poly-reactive B cells begins at an early stage of B cell development.

机译:BCR密度对天然多反应性B细胞分化的影响始于B细胞发育的早期阶段。

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B cell antigen receptor (BCR) density plays a role in the differentiation of immature B cells to their mature compartments; however, the exact strategy of its influence on the development of natural autoreactive B cells is still unclear. In the present study, we explored the role of BCR surface density in autoreactive B cell development by studying two lines of mice containing distinct copy numbers of an IgH transgene with V(H) derived from a poly-reactive natural antibody 3B4. Surface BCR levels were found to be related to the transgene copy number in these mice. In mice with higher copy numbers of the transgene, the BCRs were found to promote the remaining of autoreactive B cells into marginal zone (MZ) and B-1a subsets; meanwhile, elevated surface BCR levels were correlated with a significant decrease of follicular (Fo) B cell numbers and a reduction in the number of multiple stages of immature B cells both in spleen and bone marrow (BM). Interestingly, no difference in the ratio of cell apoptosis and proliferation was found in all stages of B cell development between two lines, except that more severely aberrant proliferation of pro/pre-B cells in BM was found in mice with higher transgene copies. This data supports the idea that natural poly-reactive B cells can be positively selected into MZ and B-1 cells, and high BCR surface density favors this selection. More importantly, our data suggests that the influence by receptor expression on the differentiation of natural poly-reactive B cells begins at an early stage of B cell development.
机译:B细胞抗原受体(BCR)的密度在未成熟B细胞向成熟区室的分化中起作用;然而,其对天然自身反应性B细胞发育的影响的确切策略仍不清楚。在本研究中,我们通过研究两行含有IgH转基因的不同拷贝数和源自多反应性天然抗体3B4的V(H)的小鼠系,探索了BCR表面密度在自身反应性B细胞发育中的作用。发现在这些小鼠中表面BCR水平与转基因拷贝数有关。在转基因拷贝数较高的小鼠中,发现BCR可以促进自身反应性B细胞的剩余进入边缘区(MZ)和B-1a子集。同时,升高的表面BCR水平与脾脏和骨髓(BM)中卵泡(Fo)B细胞数量的显着减少以及未成熟B细胞的多阶段数量的减少相关。有趣的是,在两个系之间的B细胞发育的所有阶段中,均未发现细胞凋亡与增殖比率的差异,只是在转基因拷贝数较高的小鼠中,发现BM中pro / pre-B细胞的异常异常增殖更为严重。该数据支持这样的想法,即可以将天然的多反应性B细胞正确地选择为MZ和B-1细胞,并且高BCR表面密度有利于这种选择。更重要的是,我们的数据表明受体表达对天然多反应性B细胞分化的影响始于B细胞发育的早期阶段。

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