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外周B细胞的产生通过两条在空间和时间上不同的途径发生。

Generation of peripheral B cells occurs via two spatially and temporally distinct pathways.

作者信息

Lindsley Robert Coleman, Thomas Matthew, Srivastava Bhaskar, Allman David

机构信息

Department of Pathology and Laboratory Medicine, University of Pennsylvania School of Medicine, Philadelphia, PA 19104, USA.

出版信息

Blood. 2007 Mar 15;109(6):2521-8. doi: 10.1182/blood-2006-04-018085. Epub 2006 Nov 14.

Abstract

We have identified a population of newly formed bone marrow (BM) B cells that shares multiple characteristics with late transitional B cells in the spleen. Both late splenic transitional B cells and cells within this uncharacterized BM population expressed the cell-surface phenotype AA4(+) CD23(+), yet the developmental kinetics and the renewal rate of AA4(+) CD23(+) BM B cells mirrored recently formed BM B cells. Further, unlike the least mature B cells in the BM and spleen, AA4(+) CD23(+) BM B cells expressed the homing receptor CD62L, were dependent on the antiapoptotic cytokine receptor BR3 and the tec family kinase Btk, and proliferated in response to IL-4 plus CD40 stimulation. Finally, frequencies of lambda light chain-positive B cells declined among AA4(+) CD23(+) B cells in both the BM and spleen, suggesting that V-gene selection events correlate with CD23 expression in both compartments. These observations indicate that the first step in B-cell maturation occurs in both the BM and the periphery and suggest that recently formed B cells exit the BM as a heterogeneous pool of immature and semimature B cells.

摘要

我们已经鉴定出一群新形成的骨髓(BM)B细胞,它们与脾脏中晚期过渡性B细胞具有多个共同特征。脾脏晚期过渡性B细胞和这个未明确特征的BM群体中的细胞均表达细胞表面表型AA4(+) CD23(+),然而AA4(+) CD23(+) BM B细胞的发育动力学和更新率与最近形成的BM B细胞相似。此外,与BM和脾脏中最不成熟的B细胞不同,AA4(+) CD23(+) BM B细胞表达归巢受体CD62L,依赖抗凋亡细胞因子受体BR3和tec家族激酶Btk,并在IL-4加CD40刺激下增殖。最后,BM和脾脏中AA4(+) CD23(+) B细胞中λ轻链阳性B细胞的频率均下降,这表明V基因选择事件与两个区室中的CD23表达相关。这些观察结果表明B细胞成熟的第一步发生在BM和外周,并且表明最近形成的B细胞作为不成熟和半成熟B细胞的异质库离开BM。

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