Literature DB >> 31225793

The quantity of CD40 signaling determines the differentiation of B cells into functionally distinct memory cell subsets.

Takuya Koike1, Koshi Harada1, Shu Horiuchi1, Daisuke Kitamura1.   

Abstract

In mice, memory B (Bmem) cells can be divided into two subpopulations: CD80hi Bmem cells, which preferentially differentiate into plasma cells; and CD80lo Bmem cells, which become germinal center (GC) B cells during a recall response. We demonstrate that these distinct responses can be B-cell-intrinsic and essentially independent of B-cell receptor (BCR) isotypes. Furthermore, we find that the development of CD80hi Bmem cells in the primary immune response requires follicular helper T cells, a relatively strong CD40 signal and a high-affinity BCR on B cells, whereas the development of CD80lo Bmem cells does not. Quantitative differences in CD40 stimulation were enough to recapitulate the distinct B cell fate decisions in an in vitro culture system. The quantity of CD40 signaling appears to be translated into NF-κB activation, followed by BATF upregulation that promotes Bmem cell differentiation from GC B cells.
© 2019, Koike et al.

Entities:  

Keywords:  germinal center; immune response; immunology; inflammation; memory B cells; mouse; plasma cells; recall response

Mesh:

Substances:

Year:  2019        PMID: 31225793      PMCID: PMC6636905          DOI: 10.7554/eLife.44245

Source DB:  PubMed          Journal:  Elife        ISSN: 2050-084X            Impact factor:   8.140


  65 in total

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