Mitochondrial DNA mutations drive aerobic glycolysis to enhance checkpoint blockade response in melanoma.
Mahnoor MahmoodEric Minwei LiuAmy L ShergoldElisabetta TollaJacqueline Tait-MulderAlejandro Huerta-UribeEngy ShokryAlex L YoungSergio LillaMinsoo KimTricia ParkSonia BoscencoJavier L ManchonCrístina Rodríguez-AntonaRowan C WaltersRoger J SpringettJames N BlazaLouise MitchellKaren BlythSara ZanivanDavid SumptonEdward W RobertsEd ReznikPayam A GammagePublished in: Nature cancer (2024)
The mitochondrial genome (mtDNA) encodes essential machinery for oxidative phosphorylation and metabolic homeostasis. Tumor mtDNA is among the most somatically mutated regions of the cancer genome, but whether these mutations impact tumor biology is debated. We engineered truncating mutations of the mtDNA-encoded complex I gene, Mt-Nd5, into several murine models of melanoma. These mutations promoted a Warburg-like metabolic shift that reshaped tumor microenvironments in both mice and humans, consistently eliciting an anti-tumor immune response characterized by loss of resident neutrophils. Tumors bearing mtDNA mutations were sensitized to checkpoint blockade in a neutrophil-dependent manner, with induction of redox imbalance being sufficient to induce this effect in mtDNA wild-type tumors. Patient lesions bearing >50% mtDNA mutation heteroplasmy demonstrated a response rate to checkpoint blockade that was improved by ~2.5-fold over mtDNA wild-type cancer. These data nominate mtDNA mutations as functional regulators of cancer metabolism and tumor biology, with potential for therapeutic exploitation and treatment stratification.
Keyphrases
- mitochondrial dna
- copy number
- wild type
- genome wide
- papillary thyroid
- immune response
- dna damage
- squamous cell
- cell cycle
- dna methylation
- gene expression
- oxidative stress
- childhood cancer
- lymph node metastasis
- squamous cell carcinoma
- metabolic syndrome
- patient safety
- risk assessment
- skin cancer
- toll like receptor
- high intensity
- climate change
- data analysis
- dendritic cells