Nature Communications (Oct 2024)

Reverse hierarchical DED assembly in the cFLIP-procaspase-8 and cFLIP-procaspase-8-FADD complexes

  • Chao-Yu Yang,
  • Yi-Chun Tseng,
  • Yi-Fan Tu,
  • Bai-Jiun Kuo,
  • Li-Chung Hsu,
  • Chia-I Lien,
  • You-Sheng Lin,
  • Yin-Ting Wang,
  • Yen-Chen Lu,
  • Tsung-Wei Su,
  • Yu-Chih Lo,
  • Su-Chang Lin

DOI
https://doi.org/10.1038/s41467-024-53306-1
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 17

Abstract

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Abstract cFLIP, a master anti-apoptotic regulator, targets the FADD-induced DED complexes of procaspase-8 in death receptor and ripoptosome signaling pathways. Several tumor cells maintain relatively high levels of cFLIP in achieving their immortality. However, understanding the three-dimensional regulatory mechanism initiated or mediated by elevated levels of cFLIP has been limited by the absence of the atomic coordinates for cFLIP-induced DED complexes. Here we report the crystal plus cryo-EM structures to uncover an unconventional mechanism where cFLIP and procaspase-8 autonomously form a binary tandem DED complex, independent of FADD. This complex gains the ability to recruit FADD, thereby allosterically modulating cFLIP assembly and partially activating caspase-8 for RIPK1 cleavage. Our structure-guided mutagenesis experiments provide critical insights into these regulatory mechanisms, elucidating the resistance to apoptosis and necroptosis in achieving immortality. Finally, this research offers a unified model for the intricate bidirectional hierarchy-based processes using multiprotein helical assembly to govern cell fate decisions.