MYCN-driven fatty acid uptake is a metabolic vulnerability in neuroblastoma.
Ling TaoMahmoud A MohammadGiorgio MilazzoMyrthala Moreno-SmithTajhal D PatelBarry ZormanAndrew BadachhapeBlanca E HernandezAmber B WolfZihua ZengJennifer H FosterSara AloisiPavel SumazinYouli ZuJohn HicksKetan B GhaghadaNagireddy PutluriGiovanni PeriniCristian CoarfaEveline BarbieriPublished in: Nature communications (2022)
Neuroblastoma (NB) is a childhood cancer arising from sympatho-adrenal neural crest cells. MYCN amplification is found in half of high-risk NB patients; however, no available therapies directly target MYCN. Using multi-dimensional metabolic profiling in MYCN expression systems and primary patient tumors, we comprehensively characterized the metabolic landscape driven by MYCN in NB. MYCN amplification leads to glycerolipid accumulation by promoting fatty acid (FA) uptake and biosynthesis. We found that cells expressing amplified MYCN depend highly on FA uptake for survival. Mechanistically, MYCN directly upregulates FA transport protein 2 (FATP2), encoded by SLC27A2. Genetic depletion of SLC27A2 impairs NB survival, and pharmacological SLC27A2 inhibition selectively suppresses tumor growth, prolongs animal survival, and exerts synergistic anti-tumor effects when combined with conventional chemotherapies in multiple preclinical NB models. This study identifies FA uptake as a critical metabolic dependency for MYCN-amplified tumors. Inhibiting FA uptake is an effective approach for improving current treatment regimens.
Keyphrases
- fatty acid
- induced apoptosis
- end stage renal disease
- chronic kidney disease
- signaling pathway
- childhood cancer
- stem cells
- genome wide
- newly diagnosed
- ejection fraction
- poor prognosis
- prognostic factors
- climate change
- free survival
- young adults
- single cell
- peritoneal dialysis
- endoplasmic reticulum stress
- cell therapy
- cell proliferation
- bone marrow
- cancer therapy
- amino acid
- pi k akt