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Publication : FoxP3 and Ezh2 regulate Tfr cell suppressive function and transcriptional program.

First Author  Hou S Year  2019
Journal  J Exp Med Volume  216
Issue  3 Pages  605-620
PubMed ID  30705058 Mgi Jnum  J:275352
Mgi Id  MGI:6306000 Doi  10.1084/jem.20181134
Citation  Hou S, et al. (2019) FoxP3 and Ezh2 regulate Tfr cell suppressive function and transcriptional program. J Exp Med 216(3):605-620
abstractText  Follicular regulatory T (Tfr) cells are a regulatory T cell subset that controls antibody production by inhibiting T follicular helper (Tfh)-mediated help to B cells. Tfh and Tfr cells possess opposing functions suggesting unique programming. Here we elucidated the transcriptional program controlling Tfr suppressive function. We found that Tfr cells have a program for suppressive function fine-tuned by tissue microenvironment. The transcription factor FoxP3 and chromatin-modifying enzyme EZH2 are essential for this transcriptional program but regulate the program in distinct ways. FoxP3 modifies the Tfh program to induce a Tfr-like functional state, demonstrating that Tfr cells coopt the Tfh program for suppression. Importantly, we identified a Tfr cell population that loses the Tfr program to become "ex-Tfr" cells with altered functionality. These dysfunctional ex-Tfr cells may have roles in modulating pathogenic antibody responses. Taken together, our studies reveal mechanisms controlling the Tfr transcriptional program and how failure of these mechanisms leads to dysfunctional Tfr cells.
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