PLoS Biology (Feb 2007)

Epigenetic control of the foxp3 locus in regulatory T cells.

  • Stefan Floess,
  • Jennifer Freyer,
  • Christiane Siewert,
  • Udo Baron,
  • Sven Olek,
  • Julia Polansky,
  • Kerstin Schlawe,
  • Hyun-Dong Chang,
  • Tobias Bopp,
  • Edgar Schmitt,
  • Stefan Klein-Hessling,
  • Edgar Serfling,
  • Alf Hamann,
  • Jochen Huehn

DOI
https://doi.org/10.1371/journal.pbio.0050038
Journal volume & issue
Vol. 5, no. 2
p. e38

Abstract

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Compelling evidence suggests that the transcription factor Foxp3 acts as a master switch governing the development and function of CD4(+) regulatory T cells (Tregs). However, whether transcriptional control of Foxp3 expression itself contributes to the development of a stable Treg lineage has thus far not been investigated. We here identified an evolutionarily conserved region within the foxp3 locus upstream of exon-1 possessing transcriptional activity. Bisulphite sequencing and chromatin immunoprecipitation revealed complete demethylation of CpG motifs as well as histone modifications within the conserved region in ex vivo isolated Foxp3(+)CD25(+)CD4(+) Tregs, but not in naïve CD25(-)CD4(+) T cells. Partial DNA demethylation is already found within developing Foxp3(+) thymocytes; however, Tregs induced by TGF-beta in vitro display only incomplete demethylation despite high Foxp3 expression. In contrast to natural Tregs, these TGF-beta-induced Foxp3(+) Tregs lose both Foxp3 expression and suppressive activity upon restimulation in the absence of TGF-beta. Our data suggest that expression of Foxp3 must be stabilized by epigenetic modification to allow the development of a permanent suppressor cell lineage, a finding of significant importance for therapeutic applications involving induction or transfer of Tregs and for the understanding of long-term cell lineage decisions.