Journal article
The NF-κB transcription factor RelA is required for the tolerogenic function of Foxp3 regulatory T cells
N Messina, T Fulford, L O'Reilly, WX Loh, JM Motyer, D Ellis, C McLean, H Naeem, A Lin, R Gugasyan, RM Slattery, RJ Grumont, S Gerondakis
Journal of Autoimmunity | ACADEMIC PRESS LTD- ELSEVIER SCIENCE LTD | Published : 2016
Abstract
The properties of CD4+ regulatory T cell (Treg) subsets are dictated by distinct patterns of gene expression determined by FOXP3 and different combinations of various transcription factors. Here we show the NF-κB transcription factor RelA is constitutively active in naïve and effector Tregs. The conditional inactivation of Rela in murine FOXP3+ cells induces a rapid onset, multi-focal autoimmune disease that depends on RelA being expressed in conventional T cells. In addition to promoting Treg lineage stability, RelA determines the size of the effector Treg population, a function influenced by the presence or absence of RelA in conventional T cells. These findings showing that RelA controls ..
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Awarded by National Health and Medical Research Council
Funding Acknowledgements
The authors thank Drs Roland Schmidt, Alexander Rudensky and John Silke for the generous provision of mouse strains used in this study. This work is supported by NHMRC program (#1016701) and project (#1029822) grant funding to SG. The authors declare they have no actual or potential conflicts of interest.