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Human neutrophils drive skin autoinflammation by releasing interleukin (IL)-26.

Alessia BaldoJeremy Di DomizioAhmad YatimSophie Vandenberghe-DürrRaphael JeneltenAnissa FriesLorenzo GrizzettiFrançois KuonenCarle F PaulRobert L ModlinCurdin ConradMichel Gilliet
Published in: The Journal of experimental medicine (2024)
Autoinflammation is a sterile inflammatory process resulting from increased neutrophil infiltration and overexpression of IL-1 cytokines. The factors that trigger these events are, however, poorly understood. By investigating pustular forms of psoriasis, we show that human neutrophils constitutively express IL-26 and abundantly release it from granular stores upon activation. In pustular psoriasis, neutrophil-derived IL-26 drives the pathogenic autoinflammation process by inducing the expression of IL-1 cytokines and chemokines that further recruit neutrophils. This occurs via activation of IL-26R in keratinocytes and via the formation of complexes between IL-26 and microbiota DNA, which trigger TLR9 activation of neutrophils. Thus our findings identify neutrophils as an important source of IL-26 and point to IL-26 as the key link between neutrophils and a self-sustaining autoinflammation loop in pustular psoriasis.
Keyphrases
  • poor prognosis
  • toll like receptor
  • inflammatory response
  • wound healing
  • circulating tumor
  • long non coding rna
  • cell free
  • atopic dermatitis
  • nucleic acid