Frontiers in Immunology (Jan 2022)

NFATc1/αA and Blimp-1 Support the Follicular and Effector Phenotype of Tregs

  • Anika Koenig,
  • Martin Vaeth,
  • Yin Xiao,
  • Cristina M. Chiarolla,
  • Raghu Erapaneedi,
  • Matthias Klein,
  • Lena Dietz,
  • Nadine Hundhausen,
  • Snigdha Majumder,
  • Felix Schuessler,
  • Tobias Bopp,
  • Tobias Bopp,
  • Tobias Bopp,
  • Tobias Bopp,
  • Stefan Klein-Hessling,
  • Andreas Rosenwald,
  • Andreas Rosenwald,
  • Ingolf Berberich,
  • Friederike Berberich-Siebelt

DOI
https://doi.org/10.3389/fimmu.2021.791100
Journal volume & issue
Vol. 12

Abstract

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CD4+CXCR5+Foxp3+ T-follicular regulatory (TFR) cells control the germinal center responses. Like T-follicular helper cells, they express high levels of Nuclear Factor of Activated T-cells c1, predominantly its short isoform NFATc1/αA. Ablation of NFATc1 in Tregs prevents upregulation of CXCR5 and migration of TFR cells into B-cell follicles. By contrast, constitutive active NFATc1/αA defines the surface density of CXCR5, whose level determines how deep a TFR migrates into the GC and how effectively it controls antibody production. As one type of effector Treg, TFR cells express B lymphocyte-induced maturation protein-1 (Blimp-1). Blimp-1 can directly repress Cxcr5 and NFATc1/αA is necessary to overcome this Blimp-1-mediated repression. Interestingly, Blimp-1 even reinforces the recruitment of NFATc1 to Cxcr5 by protein-protein interaction and by those means cooperates with NFATc1 for Cxcr5 transactivation. On the contrary, Blimp-1 is necessary to counterbalance NFATc1/αA and preserve the Treg identity. This is because although NFATc1/αA strengthens the follicular development of Tregs, it bears the inherent risk of causing an ex-Treg phenotype.

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