Nature Communications (Jan 2025)

Heterochromatic gene silencing controls CD4+ T cell susceptibility to regulatory T cell-mediated suppression in a murine allograft model

  • Julie Noguerol,
  • Karl Laviolette,
  • Margot Zahm,
  • Adeline Chaubet,
  • Ambrine Sahal,
  • Claire Détraves,
  • Romain Torres,
  • Clothilde Demont,
  • Véronique Adoue,
  • Carine Joffre,
  • Florence Cammas,
  • Joost PM van Meerwijk,
  • Olivier P. Joffre

DOI
https://doi.org/10.1038/s41467-025-55848-4
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 18

Abstract

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Abstract Protective immune responses require close interactions between conventional (Tconv) and regulatory T cells (Treg). The extracellular mediators and signaling events that regulate the crosstalk between these CD4+ T cell subsets have been extensively characterized. However, how Tconv translate Treg-dependent suppressive signals at the chromatin level remains largely unknown. Here we show, using a murine bone marrow allograft model in which graft rejection is coordinated by CD4+ T cells and can be inhibited by Treg, that Treg-mediated T cell suppression involves Heterochromatin Protein 1 α (HP1α)-dependent gene silencing. Unexpectedly, our screen also reveals that T cells deficient for HP1γ or the methyltransferase SUV39H1 are better repressed by Treg than their wild-type counterparts. Mechanistically, our transcriptional and epigenetic profiling identifies HP1γ as a negative regulator of a gene network functionally associated with T-cell exhaustion, including those encoding the inhibitory receptors PD-1 and LAG-3. In conclusion, we identify HP1 variants as rheostats that finely tune the balance between tolerance and immunity. While HP1α converts immunosuppressive signals into heterochromatin-dependent gene silencing mechanisms, HP1γ adjusts Tconv sensitivity to inhibitory environmental signals.