Cell Reports (Feb 2016)

Neutrophil-Derived Proteases Escalate Inflammation through Activation of IL-36 Family Cytokines

  • Conor M. Henry,
  • Graeme P. Sullivan,
  • Danielle M. Clancy,
  • Inna S. Afonina,
  • Dagmar Kulms,
  • Seamus J. Martin

DOI
https://doi.org/10.1016/j.celrep.2015.12.072
Journal volume & issue
Vol. 14, no. 4
pp. 708 – 722

Abstract

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Recent evidence has strongly implicated the IL-1 family cytokines IL-36α, IL-36β, and IL-36γ as key initiators of skin inflammation. Similar to the other members of the IL-1 family, IL-36 cytokines are expressed as inactive precursors and require proteolytic processing for activation; however, the responsible proteases are unknown. Here, we show that IL-36α, IL-36β, and IL-36γ are activated differentially by the neutrophil granule-derived proteases cathepsin G, elastase, and proteinase-3, increasing their biological activity ∼500-fold. Active IL-36 promoted a strong pro-inflammatory signature in primary keratinocytes and was sufficient to perturb skin differentiation in a reconstituted 3D human skin model, producing features resembling psoriasis. Furthermore, skin eluates from psoriasis patients displayed significantly elevated cathepsin G-like activity that was sufficient to activate IL-36β. These data identify neutrophil granule proteases as potent IL-36-activating enzymes, adding to our understanding of how neutrophils escalate inflammatory reactions. Inhibition of neutrophil-derived proteases may therefore have therapeutic benefits in psoriasis.

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