Cell Reports (Aug 2024)

Non-canonical autophosphorylation of RIPK1 drives timely pyroptosis to control Yersinia infection

  • David Jetton,
  • Hayley I. Muendlein,
  • Wilson M. Connolly,
  • Zoie Magri,
  • Irina Smirnova,
  • Rebecca Batorsky,
  • Joan Mecsas,
  • Alexei Degterev,
  • Alexander Poltorak

Journal volume & issue
Vol. 43, no. 8
p. 114641

Abstract

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Summary: Caspase-8-dependent pyroptosis has been shown to mediate host protection from Yersinia infection. For this mode of cell death, the kinase activity of receptor-interacting protein kinase 1 (RIPK1) is required, but the autophosphorylation sites required to drive caspase-8 activation have not been determined. Here, we show that non-canonical autophosphorylation of RIPK1 at threonine 169 (T169) is necessary for caspase-8-mediated pyroptosis. Mice with alanine in the T169 position are highly susceptible to Yersinia dissemination. Mechanistically, the delayed formation of a complex containing RIPK1, ZBP1, Fas-associated protein with death domain (FADD), and caspase-8 abrogates caspase-8 maturation in T169A mice and leads to the eventual activation of RIPK3-dependent necroptosis in vivo; however, this is insufficient to protect the host, suggesting that timely pyroptosis during early response is specifically required to control infection. These results position RIPK1 T169 phosphorylation as a driver of pyroptotic cell death critical for host defense.

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