Frontiers in Immunology (May 2022)

IL-38 Gene Deletion Worsens Murine Colitis

  • Dennis M. de Graaf,
  • Dennis M. de Graaf,
  • Ruth X. Wang,
  • Ruth X. Wang,
  • Jesús Amo-Aparicio,
  • J. Scott Lee,
  • Alexander S. Dowdell,
  • Isak W. Tengesdal,
  • Carlo Marchetti,
  • Sean P. Colgan,
  • Leo A. B. Joosten,
  • Leo A. B. Joosten,
  • Charles A. Dinarello,
  • Charles A. Dinarello

DOI
https://doi.org/10.3389/fimmu.2022.840719
Journal volume & issue
Vol. 13

Abstract

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IL-38 is a recently discovered cytokine and member of the IL-1 Family. In the IL-1 Family, IL-38 is unique because the cytokine is primarily a B lymphocyte product and functions to suppress inflammation. Studies in humans with inflammatory bowel disease (IBD) suggest that IL-38 may be protective for ulcerative colitis or Crohn’s disease, and that IL-38 acts to maintain homeostasis in the intestinal tract. Here we investigated the role of endogenous IL-38 in experimental colitis in mice deficient in IL-38 by deletion of exons 1-4 in C57 BL/6 mice. Compared to WT mice, IL-38 deficient mice subjected to dextran sulfate sodium (DSS) showed greater severity of disease, more weight loss, increased intestinal permeability, and a worse histological phenotype including increased neutrophil influx in the colon. Mice lacking IL-38 exhibited elevated colonic Nlrp3 mRNA and protein levels, increased caspase-1 activation, and the concomitant increased processing of IL-1β precursor into active IL-1β. Expression of IL-1α, an exacerbator of IBD, was also upregulated. Colonic myleloperoxidase protein and Il17a, and Il17f mRNA levels were higher in the IL-38 deficient mice. Daily treatment of IL-38 deficient mice with an NLRP3 inhibitor attenuated diarrhea and weight loss during the recovery phase. These data implicate endogenous IL-38 as an anti-inflammatory cytokine that reduces DSS colitis severity. We propose that a relative deficiency of IL-38 contributes to IBD by disinhibition of the NLRP3 inflammasome.

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