c-Rel Controls Multiple Discrete Steps in the Thymic Development of Foxp3+ CD4 Regulatory T Cells
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Grigoriadis, George
Vasanthakumar, Ajithkumar
Banerjee, Ashish
Grumont, Raelene
Overall, Sarah
Gleeson, Paul
Shannon, Frances
Gerondakis, Steve
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Public Library of Science
Abstract
The development of natural Foxp3(+) CD4 regulatory T cells (nTregs) proceeds via two steps that involve the initial antigen dependent generation of CD25(+)GITR(hi)Foxp3(-)CD4(+) nTreg precursors followed by the cytokine induction of Foxp3. Using mutant mouse models that lack c-Rel, the critical NF-κB transcription factor required for nTreg differentiation, we establish that c-Rel regulates both of these developmental steps. c-Rel controls the generation of nTreg precursors via a haplo-insufficient mechanism, indicating that this step is highly sensitive to c-Rel levels. However, maintenance of c-Rel in an inactive state in nTreg precursors demonstrates that it is not required for a constitutive function in these cells. While the subsequent IL-2 induction of Foxp3 in nTreg precursors requires c-Rel, this developmental transition does not coincide with the nuclear expression of c-Rel. Collectively, our results support a model of nTreg differentiation in which c-Rel generates a permissive state for foxp3 transcription during the development of nTreg precursors that influences the subsequent IL-2 dependent induction of Foxp3 without a need for c-Rel reactivation.
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animals, cell nucleus, cell survival, forkhead transcription factors, haploinsufficiency, interleukin-15, interleukin-2, mice, phosphorylation, protein multimerization, proto-oncogene proteins c-bcl-2, proto-oncogene proteins c-rel, receptors, interleukin-2, stat5 transcription factor, signal transduction, t-lymphocytes, regulatory, thymus gland
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PLoS ONE
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