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Mitochondrial genetic variation in human bioenergetics, adaptation, and adult disease.

Volney K FriedrichMeagan A RubelTheodore G Schurr
Published in: American journal of human biology : the official journal of the Human Biology Council (2021)
Our review suggests that the mitochondrial research field would benefit from independently replicating mtDNA haplogroup-phenotype associations across global populations, incorporating potentially confounding environmental, demographic, and disease covariates into studies of mtDNA variation, and extending association-based studies to include analyses of complete mitogenomes and assays of mitochondrial function.
Keyphrases
  • mitochondrial dna
  • oxidative stress
  • copy number
  • endothelial cells
  • case control
  • gene expression
  • induced pluripotent stem cells
  • risk assessment
  • young adults
  • human health
  • life cycle
  • childhood cancer