Cell Reports (Oct 2013)

Protective Roles for Caspase-8 and cFLIP in Adult Homeostasis

  • Ricardo Weinlich,
  • Andrew Oberst,
  • Christopher P. Dillon,
  • Laura J. Janke,
  • Sandra Milasta,
  • John R. Lukens,
  • Diego A. Rodriguez,
  • Prajwal Gurung,
  • Chandra Savage,
  • Thirumala D. Kanneganti,
  • Douglas R. Green

DOI
https://doi.org/10.1016/j.celrep.2013.08.045
Journal volume & issue
Vol. 5, no. 2
pp. 340 – 348

Abstract

Read online

Caspase-8 or cellular FLICE-like inhibitor protein (cFLIP) deficiency leads to embryonic lethality in mice due to defects in endothelial tissues. Caspase-8−/− and receptor-interacting protein kinase-3 (RIPK3)−/−, but not cFLIP−/− and RIPK3−/−, double-knockout animals develop normally, indicating that caspase-8 antagonizes the lethal effects of RIPK3 during development. Here, we show that the acute deletion of caspase-8 in the gut of adult mice induces enterocyte death, disruption of tissue homeostasis, and inflammation, resulting in sepsis and mortality. Likewise, acute deletion of caspase-8 in a focal region of the skin induces local keratinocyte death, tissue disruption, and inflammation. Strikingly, RIPK3 ablation rescues both phenotypes. However, acute loss of cFLIP in the skin produces a similar phenotype that is not rescued by RIPK3 ablation. TNF neutralization protects from either acute loss of caspase-8 or cFLIP. These results demonstrate that caspase-8-mediated suppression of RIPK3-induced death is required not only during development but also for adult homeostasis. Furthermore, RIPK3-dependent inflammation is dispensable for the skin phenotype.