Scientific Reports (Jul 2024)

Deciphering the role of protein kinase A in the control of FoxP3 expression in regulatory T cells in health and autoimmunity

  • Maria Teresa Lepore,
  • Sara Bruzzaniti,
  • Claudia La Rocca,
  • Clorinda Fusco,
  • Fortunata Carbone,
  • Maria Mottola,
  • Bruno Zuccarelli,
  • Roberta Lanzillo,
  • Vincenzo Brescia Morra,
  • Giorgia Teresa Maniscalco,
  • Salvatore De Simone,
  • Claudio Procaccini,
  • Antonio Porcellini,
  • Veronica De Rosa,
  • Mario Galgani,
  • Silvana Cassano,
  • Giuseppe Matarese

DOI
https://doi.org/10.1038/s41598-024-68098-z
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 11

Abstract

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Abstract The molecular mechanisms that govern differential T cell development from CD4+CD25-conventional T (Tconv) into CD4+CD25+ forkhead-box-P3+ (FoxP3+) inducible regulatory T (iTreg) cells remain unclear. Herein, we investigated the relative contribution of protein kinase A (PKA) in this process. Mechanistically, we found that PKA controlled the efficiency of human iTreg cell generation through the expression of different FoxP3 splicing variants containing or not the exon 2. We found that transient PKA inhibition reduced the recruitment of cAMP-responsive element-binding protein (CREB) on regulatory regions of the FoxP3 gene, a condition that is associated with an impaired acquisition of their suppressive capacity in vitro. To corroborate our findings in a human model of autoimmunity, we measured CREB phosphorylation and FoxP3 levels in iTreg cells from treatment-naïve relapsing–remitting (RR)-multiple sclerosis (MS) subjects. Interestingly, both phospho-CREB and FoxP3 induction directly correlated and were significantly reduced in RR-MS patients, suggesting a previously unknown mechanism involved in the induction and function of human iTreg cells.