Altered propionate metabolism contributes to tumour progression and aggressiveness.
Ana P GomesDidem IlterVivien LowStanislav DrapelaTanya SchildEdouard MullarkyJulie HanIlaria EliaDorien BroekaertAdam RosenzweigMichal NagiecJoana B NunesBethany E SchafferAnders P MutveiJohn M AsaraLewis C CantleySarah-Maria FendtJohn BlenisPublished in: Nature metabolism (2022)
The alteration of metabolic pathways is a critical strategy for cancer cells to attain the traits necessary for metastasis in disease progression. Here, we find that dysregulation of propionate metabolism produces a pro-aggressive signature in breast and lung cancer cells, increasing their metastatic potential. This occurs through the downregulation of methylmalonyl coenzyme A epimerase (MCEE), mediated by an extracellular signal-regulated kinase 2-driven transcription factor Sp1/early growth response protein 1 transcriptional switch driven by metastatic signalling at its promoter level. The loss of MCEE results in reduced propionate-driven anaplerotic flux and intracellular and intratumoral accumulation of methylmalonic acid, a by-product of propionate metabolism that promotes cancer cell invasiveness. Altogether, we present a previously uncharacterized dysregulation of propionate metabolism as an important contributor to cancer and a valuable potential target in the therapeutic treatment of metastatic carcinomas.
Keyphrases
- transcription factor
- squamous cell carcinoma
- small cell lung cancer
- gene expression
- cell proliferation
- dna methylation
- genome wide
- papillary thyroid
- signaling pathway
- dna binding
- human health
- high grade
- risk assessment
- squamous cell
- combination therapy
- young adults
- lymph node metastasis
- anti inflammatory
- smoking cessation
- childhood cancer