| Literature DB >> 33932034 |
Mónica Vara-Pérez1,2, Matteo Rossi2,3, Chris Van den Haute4,5, Hannelore Maes1, Maria Livia Sassano1,2, Vivek Venkataramani6, Bernhard Michalke7, Erminia Romano1, Kristine Rillaerts1,2, Abhishek D Garg1, Corentin Schepkens8,9, Francesca M Bosisio10, Jasper Wouters10, Ana Isabel Oliveira2,11, Peter Vangheluwe12, Wim Annaert13,14, Johannes V Swinnen8, Jean Marie Colet9, Joost J van den Oord10, Sarah-Maria Fendt2,3, Massimiliano Mazzone2,11, Patrizia Agostinis1,2.
Abstract
BNIP3 is a mitophagy receptor with context-dependent roles in cancer, but whether and how it modulates melanoma growth in vivo remains unknown. Here, we found that elevated BNIP3 levels correlated with poorer melanoma patient's survival and depletion of BNIP3 in B16-F10 melanoma cells compromised tumor growth in vivo. BNIP3 depletion halted mitophagy and enforced a PHD2-mediated downregulation of HIF-1α and its glycolytic program both in vitro and in vivo. Mechanistically, we found that BNIP3-deprived melanoma cells displayed increased intracellular iron levels caused by heightened NCOA4-mediated ferritinophagy, which fostered PHD2-mediated HIF-1α destabilization. These effects were not phenocopied by ATG5 or NIX silencing. Restoring HIF-1α levels in BNIP3-depleted melanoma cells rescued their metabolic phenotype and tumor growth in vivo, but did not affect NCOA4 turnover, underscoring that these BNIP3 effects are not secondary to HIF-1α. These results unravel an unexpected role of BNIP3 as upstream regulator of the pro-tumorigenic HIF-1α glycolytic program in melanoma cells.Entities:
Keywords: BNIP3; HIF-1α; ferritinophagy; melanoma; metabolism
Year: 2021 PMID: 33932034 DOI: 10.15252/embj.2020106214
Source DB: PubMed Journal: EMBO J ISSN: 0261-4189 Impact factor: 11.598