CREB/ATF-dependent T cell receptor-induced FoxP3 gene expression: a role for DNA methylation

doi:10.1084/jem.20070109

Published online June 25, 2007
doi:10.1084/jem.20070109
The Journal of Experimental Medicine, Vol. 204, No. 7, 1543-1551
The Rockefeller University Press, 0022-1007 $30.00
© 2007 Kim et al.

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BRIEF DEFINITIVE REPORT

CREB/ATF-dependent T cell receptor–induced FoxP3 gene expression: a role for DNA methylation

Hyoung-Pyo Kim and Warren J. Leonard

Laboratory of Molecular Immunology, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, MD 20892

CORRESPONDENCE Warren J. Leonard: wjl{at}helix.nih.gov

Regulatory T cells (T reg cells) are a population of CD4⁺ Tcells that limit immune responses. FoxP3 is a master controltranscription factor for development and function of these cells,but its regulation is poorly understood. We have identifieda T cell receptor–responsive enhancer in the FoxP3 firstintron that is dependent on a cyclic-AMP response element bindingprotein (CREB)/activating transcription factor (ATF) site overlappinga CpG island. Methylation of this island inversely correlateswith CREB binding and FoxP3 expression. Interestingly, transforminggrowth factor-ß, which induces T reg cell formation,decreases methylation of the CpG island and increases FoxP3expression. Similarly, inhibiting methylation with 5-azacytidineor knocking down the DNA methyltransferase Dnmt1 also inducesFoxP3 expression. Conversely, methylation of the CpG island,which decreases CREB binding or expression of dominant-negativeCREB, decreases FoxP3 gene expression. Thus, T cell receptor–inducedFoxP3 expression in T reg cells is controlled both by sequence-specificbinding of CREB/ATF and by DNA methylation of a CpG island.

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