Species-specific cleavage of the autophagy adaptor p62 dictates responses to TNF
- Mol Cell. 2026 Apr 16;86(8):1574-1586.e11. doi: 10.1016/j.molcel.2026.03.013.
- 1. Tumour Cell Death and Autophagy Laboratory, Cancer Research UK Scotland Institute, Garscube Estate, Switchback Road, Glasgow G61 1BD, UK; School of Cancer Sciences, University of Glasgow, Garscube Estate, Switchback Road, Glasgow G61 1QH, UK. Electronic address: [email protected].
- 2. Tumour Cell Death and Autophagy Laboratory, Cancer Research UK Scotland Institute, Garscube Estate, Switchback Road, Glasgow G61 1BD, UK.
- 3. MRC Toxicology Unit, University of Cambridge, Tennis Court Road, Cambridge CB2 1QR, UK.
- 4. Tumour Cell Death and Autophagy Laboratory, Cancer Research UK Scotland Institute, Garscube Estate, Switchback Road, Glasgow G61 1BD, UK; School of Cancer Sciences, University of Glasgow, Garscube Estate, Switchback Road, Glasgow G61 1QH, UK.
- 5. Tumour Cell Death and Autophagy Laboratory, Cancer Research UK Scotland Institute, Garscube Estate, Switchback Road, Glasgow G61 1BD, UK; School of Cancer Sciences, University of Glasgow, Garscube Estate, Switchback Road, Glasgow G61 1QH, UK. Electronic address: [email protected].
Inflammation can affect many diseases. We report here that inflammatory cytokines invoke caspase-8-mediated cleavage of the Autophagy adaptor p62/SQSTM1 at aspartic acid 329 in human cells, producing a previously described truncated form, which we term tr-p62. We show that TNF-driven cell death is tr-p62 dependent and that Autophagy inhibition promotes death via tr-p62 accumulation. Mechanistically, p62 cleavage is receptor-interacting serine/threonine-protein kinase 1 (RIPK1) dependent, and tr-p62 stabilizes Caspase-8 activating complex-IIb. tr-p62-driven cell death downstream of TNF is also RIPK1 and Caspase dependent, promoting feedforward Caspase-8 activation. p62 cleavage does not, however, affect Necroptosis. Surprisingly, this Caspase-8 cleavage site in p62 is absent in mice, and introduction of cleavable forms of p62 into mouse cells causes sensitization to TNF-induced death. Moreover, mice with CRISPR-Cas9-generated cleavable p62 exhibit TNF hypersensitivity and intestinal inflammation in vivo. These findings provide significant insights into TNF-induced cell death and introduce a mouse model that may provide better clarity for human-related studies of inflammatory disease.
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