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Pten controls B-cell responsiveness and germinal center reaction by regulating the expression of IgD BCR.


ABSTRACT: In contrast to other B-cell antigen receptor (BCR) classes, the function of IgD BCR on mature B cells remains largely elusive as mature B cells co-express IgM, which is sufficient for development, survival, and activation of B cells. Here, we show that IgD expression is regulated by the forkhead box transcription factor FoxO1, thereby shifting the responsiveness of mature B cells towards recognition of multivalent antigen. FoxO1 is repressed by phosphoinositide 3-kinase (PI3K) signaling and requires the lipid phosphatase Pten for its activation. Consequently, Pten-deficient B cells expressing knock-ins for BCR heavy and light chain genes are unable to upregulate IgD. Furthermore, in the presence of autoantigen, Pten-deficient B cells cannot eliminate the autoreactive BCR specificity by secondary light chain gene recombination. Instead, Pten-deficient B cells downregulate BCR expression and become unresponsive to further BCR-mediated stimulation. Notably, we observed a delayed germinal center (GC) reaction by IgD-deficient B cells after immunization with trinitrophenyl-ovalbumin (TNP-Ova), a commonly used antigen for T-cell-dependent antibody responses. Together, our data suggest that the activation of IgD expression by Pten/FoxO1 results in mature B cells that are selectively responsive to multivalent antigen and are capable of initiating rapid GC reactions and T-cell-dependent antibody responses.

SUBMITTER: Setz CS 

PROVIDER: S-EPMC6545559 | biostudies-literature | 2019 Jun

REPOSITORIES: biostudies-literature

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Pten controls B-cell responsiveness and germinal center reaction by regulating the expression of IgD BCR.

Setz Corinna S CS   Khadour Ahmad A   Renna Valerio V   Iype Joseena J   Gentner Eva E   He Xiaocui X   Datta Moumita M   Young Marc M   Nitschke Lars L   Wienands Jürgen J   Maity Palash C PC   Reth Michael M   Jumaa Hassan H  

The EMBO journal 20190423 11


In contrast to other B-cell antigen receptor (BCR) classes, the function of IgD BCR on mature B cells remains largely elusive as mature B cells co-express IgM, which is sufficient for development, survival, and activation of B cells. Here, we show that IgD expression is regulated by the forkhead box transcription factor FoxO1, thereby shifting the responsiveness of mature B cells towards recognition of multivalent antigen. FoxO1 is repressed by phosphoinositide 3-kinase (PI3K) signaling and requ  ...[more]

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