PLoS ONE (Sep 2009)

miR-155 inhibition sensitizes CD4+ Th cells for TREG mediated suppression.

  • Heiko F Stahl,
  • Tanja Fauti,
  • Nina Ullrich,
  • Tobias Bopp,
  • Jan Kubach,
  • Werner Rust,
  • Paul Labhart,
  • Vassili Alexiadis,
  • Christian Becker,
  • Mathias Hafner,
  • Andreas Weith,
  • Martin C Lenter,
  • Helmut Jonuleit,
  • Edgar Schmitt,
  • Detlev Mennerich

DOI
https://doi.org/10.1371/journal.pone.0007158
Journal volume & issue
Vol. 4, no. 9
p. e7158

Abstract

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BackgroundIn humans and mice naturally occurring CD4(+)CD25(+) regulatory T cells (nTregs) are a thymus-derived subset of T cells, crucial for the maintenance of peripheral tolerance by controlling not only potentially autoreactive T cells but virtually all cells of the adaptive and innate immune system. Recent work using Dicer-deficient mice irrevocably demonstrated the importance of miRNAs for nTreg cell-mediated tolerance.Principal findingsDNA-Microarray analyses of human as well as murine conventional CD4(+) Th cells and nTregs revealed a strong up-regulation of mature miR-155 (microRNA-155) upon activation in both populations. Studying miR-155 expression in FoxP3-deficient scurfy mice and performing FoxP3 ChIP-Seq experiments using activated human T lymphocytes, we show that the expression and maturation of miR-155 seem to be not necessarily regulated by FoxP3. In order to address the functional relevance of elevated miR-155 levels, we transfected miR-155 inhibitors or mature miR-155 RNAs into freshly-isolated human and mouse primary CD4(+) Th cells and nTregs and investigated the resulting phenotype in nTreg suppression assays. Whereas miR-155 inhibition in conventional CD4(+) Th cells strengthened nTreg cell-mediated suppression, overexpression of mature miR-155 rendered these cells unresponsive to nTreg cell-mediated suppression.ConclusionInvestigation of FoxP3 downstream targets, certainly of bound and regulated miRNAs revealed the associated function between the master regulator FoxP3 and miRNAs as regulators itself. miR-155 is shown to be crucially involved in nTreg cell mediated tolerance by regulating the susceptibility of conventional human as well as murine CD4(+) Th cells to nTreg cell-mediated suppression.