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. 2025 Jul;27(7):1098-1113.
doi: 10.1038/s41556-025-01689-8. Epub 2025 Jun 27.

Autophagy-targeted NBR1-p62/SQSTM1 complexes promote breast cancer metastasis by sequestering ITCH

Gourish Mondal  1 Hugo Gonzalez  2   3 Timothy Marsh  1 Andrew M Leidal  1 Ariadne Vlahakis  1 Pravin R Phadatare  1 Sofı́a Bustamante Eguiguren  1 Michael Bruck  4 Akul Naik  5 Mark Jesus M Magbanua  5   6 Laura A Huppert  4   6 Arun P Wiita  5   6   7   8 Jeroen P Roose  2   6 Jennifer M Rosenbluth  4   6   8 Jayanta Debnath  9   10
Affiliations

Autophagy-targeted NBR1-p62/SQSTM1 complexes promote breast cancer metastasis by sequestering ITCH

Gourish Mondal et al. Nat Cell Biol. 2025 Jul.

Abstract

Autophagy deficiency in breast cancer promotes metastasis through the accumulation of the autophagy cargo receptor NBR1. Here we show that autophagy normally suppresses breast cancer metastasis by enabling the clearance of NBR1-p62/SQSTM1 complexes that instruct p63-mediated pro-metastatic basal differentiation programmes. When autophagy is inhibited, the autophagy cargo receptors NBR1 and p62/SQSTM1 accumulate within biomolecular condensates in cells, which drives basal differentiation in both mouse and human breast cancer models. Mechanistically, these NBR1-p62/SQSTM1 complexes sequester ITCH, a ubiquitin ligase that degrades and negatively regulates p63 in breast cancer cells, thereby stabilizing and activating p63. Accordingly, mutant forms of NBR1 unable to sequester ITCH into NBR1-p62/SQSTM1 complexes do not promote basal differentiation and metastasis in vivo. Overall, our findings illuminate how proteostatic defects arising in the setting of therapeutic autophagy inhibition modulate epithelial lineage fidelity and metastatic progression.

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Conflict of interest statement

Competing interests: J.D. is a former member of the SAB of Vescor Therapeutics (concluded January 2022). The other authors declare no competing interests.

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