Frontiers in Immunology (Sep 2022)

SMRT and NCoR1 fine-tune inflammatory versus tolerogenic balance in dendritic cells by differentially regulating STAT3 signaling

  • Atimukta Jha,
  • Atimukta Jha,
  • Abdul Ahad,
  • Abdul Ahad,
  • Gyan Prakash Mishra,
  • Gyan Prakash Mishra,
  • Kaushik Sen,
  • Shuchi Smita,
  • Shuchi Smita,
  • Aliva Prity Minz,
  • Viplov Kumar Biswas,
  • Viplov Kumar Biswas,
  • Archana Tripathy,
  • Shantibhushan Senapati,
  • Shantibhushan Senapati,
  • Bhawna Gupta,
  • Hans Acha-Orbea,
  • Sunil Kumar Raghav,
  • Sunil Kumar Raghav

DOI
https://doi.org/10.3389/fimmu.2022.910705
Journal volume & issue
Vol. 13

Abstract

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Dendritic cell (DC) fine-tunes inflammatory versus tolerogenic responses to protect from immune-pathology. However, the role of co-regulators in maintaining this balance is unexplored. NCoR1-mediated repression of DC immune-tolerance has been recently reported. Here we found that depletion of NCoR1 paralog SMRT (NCoR2) enhanced cDC1 activation and expression of IL-6, IL-12 and IL-23 while concomitantly decreasing IL-10 expression/secretion. Consequently, co-cultured CD4+ and CD8+ T-cells depicted enhanced Th1/Th17 frequency and cytotoxicity, respectively. Comparative genomic and transcriptomic analysis demonstrated differential regulation of IL-10 by SMRT and NCoR1. SMRT depletion represses mTOR-STAT3-IL10 signaling in cDC1 by down-regulating NR4A1. Besides, Nfkbia and Socs3 were down-regulated in Ncor2 (Smrt) depleted cDC1, supporting increased production of inflammatory cytokines. Moreover, studies in mice showed, adoptive transfer of SMRT depleted cDC1 in OVA-DTH induced footpad inflammation led to increased Th1/Th17 and reduced tumor burden after B16 melanoma injection by enhancing oncolytic CD8+ T-cell frequency, respectively. We also depicted decreased Ncor2 expression in Rheumatoid Arthritis, a Th1/Th17 disease.

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