PLoS ONE (Jan 2017)

Th17 micro-milieu regulates NLRP1-dependent caspase-5 activity in skin autoinflammation.

  • Stephanie Zwicker,
  • Eva Hattinger,
  • Daniela Bureik,
  • Aleksandra Batycka-Baran,
  • Andreas Schmidt,
  • Peter-Arne Gerber,
  • Simon Rothenfusser,
  • Michel Gilliet,
  • Thomas Ruzicka,
  • Ronald Wolf

DOI
https://doi.org/10.1371/journal.pone.0175153
Journal volume & issue
Vol. 12, no. 4
p. e0175153

Abstract

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IL-1β is a potent player in cutaneous inflammation and central for the development of a Th17 micro-milieu in autoinflammatory diseases including psoriasis. Its production is controlled at the transcriptional level and by subsequent posttranslational processing via inflammatory caspases. In this study, we detected inflammatory caspase-5 active in epidermal keratinocytes and in psoriatic skin lesions. Further, interferon-γ and interleukin-17A synergistically induced caspase-5 expression in cultured keratinocytes, which was dependent on the antimicrobial peptide psoriasin (S100A7). However, diseases-relevant triggers for caspase-5 activity and IL-1β production remain unknown. Recently, extranuclear DNA has been identified as danger-signals abundant in the psoriatic epidermis. Here, we could demonstrate that cytosolic double-stranded (ds) DNA transfected into keratinocytes triggered the activation of caspase-5 and the release of IL-1β. Further, interleukin-17A promoted caspase-5 function via facilitation of the NLRP1-inflammasome. Anti-inflammatory vitamin D interfered with the IL-1β release and suppressed caspase-5 in keratinocytes and in psoriatic skin lesions. Our data link the disease-intrinsic danger signals psoriasin (S100A7) and dsDNA for NLPR1-dependent caspase-5 activity in psoriasis providing potential therapeutic targets in Th17-mediated skin autoinflammation.