Preneoplastic cells switch to Warburg metabolism from their inception exposing multiple vulnerabilities for targeted elimination

Henna Myllymaki, Lisa Kelly, Abigail Elliot, Roderick Nicholas Carter, Nicholas M Morton, Yi Feng

Research output: Contribution to journalArticlepeer-review

Abstract / Description of output

Otto Warburg described tumour cells as displaying enhanced aerobic glycolysis whilst maintaining defective oxidative phosphorylation (OXPHOS) for energy production almost 100 years ago 1,2. Since then, the ‘Warburg effect’ has been widely accepted as a key feature of rapidly proliferating cancer cells 3,4,5. What is not clear is how early “Warburg metabolism” initiates in cancer and whether changes in energy metabolism might influence tumour progression ab initio. We set out to investigate energy metabolism in HRASG12V driven preneoplastic cell (PNC) at inception, in a zebrafish skin PNC model. We find that, within 24 hours of HRASG12V induction, PNCs upregulate glycolysis and blocking glycolysis reduces PNC proliferation, whilst increasing available glucose enhances PNC proliferation and reduces apoptosis. Impaired OXPHOS accompanies enhanced glycolysis in PNCs, and a mild complex I inhibitor, metformin, selectively induces apoptosis and suppresses proliferation of PNCs. Enhanced mitochondrial fragmentation might be underlining impaired OXPHOS and block mitochondrial fragmentation triggers PNC apoptosis. Our data indicate that altered energy metabolism is one of the earliest events upon oncogene activation in somatic cells, which allows a targeted and effective PNC elimination.
Original languageEnglish
Article number7
JournalOncogenesis
Volume13
Issue number1
DOIs
Publication statusPublished - 25 Jan 2024

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