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Publication : RORĪ³t Promotes Foxp3 Expression by Antagonizing the Effector Program in Colonic Regulatory T Cells.

First Author  Bhaumik S Year  2021
Journal  J Immunol Volume  207
Issue  8 Pages  2027-2038
PubMed ID  34518282 Mgi Jnum  J:331158
Mgi Id  MGI:6849678 Doi  10.4049/jimmunol.2100175
Citation  Bhaumik S, et al. (2021) RORgammat Promotes Foxp3 Expression by Antagonizing the Effector Program in Colonic Regulatory T Cells. J Immunol 207(8):2027-2038
abstractText  RORgammat is the master transcription factor for the Th17 cells. Paradoxically, in the intestine, RORgammat is coexpressed in peripherally induced regulatory T cells (pTregs) together with Foxp3, the master transcription factor for Tregs. Unexpectedly, by an unknown mechanism, colonic RORgammat(+) Tregs show an enhanced suppressor function and prevent intestinal inflammation more efficiently than RORgammat-nonexpressing pTregs. Although studies have elucidated the function of RORgammat in Th17 cells, how RORgammat regulates pTreg function is not understood. In our attempt to understand the role of RORgammat in controlling Treg function, we discovered a RORgammat-driven pathway that modulates the regulatory (suppressor) function of colonic Tregs. We found that RORgammat plays an essential role in maintaining Foxp3 expression. RORgammat-deficient Tregs failed to sustain Foxp3 expression with concomitant upregulation of T-bet and IFN-gamma expressions. During colitis induced by adoptive transfer of CD45RB(hi) cells in Rag1 (-/-) mice, RORgammat-deficient colonic Tregs transitioned to a Th1-like effector phenotype and lost their suppressor function, leading to severe colitis with significant mortality. Accordingly, Foxp3-expressing, RORgammat-deficient Tregs showed impaired therapeutic efficacy in ameliorating colitis that is not due to their reduced survival. Moreover, using the Treg-specific RORgammat and T-bet double-deficient gene knockout mouse, we demonstrate that deletion of T-bet from RORgammat-deficient Tregs restored Foxp3 expression and suppression function as well as prevented onset of severe colitis. Mechanistically, our study suggests that RORgammat-mediated repression of T-bet is critical to regulating the immunosuppressive function of colonic Tregs during the inflammatory condition.
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