| Literature DB >> 30174309 |
Meagan J McManus1, Martin Picard2, Hsiao-Wen Chen1, Hans J De Haas3, Prasanth Potluri1, Jeremy Leipzig1, Atif Towheed1, Alessia Angelin1, Partho Sengupta3, Ryan M Morrow1, Brett A Kauffman4, Marc Vermulst1, Jagat Narula3, Douglas C Wallace5.
Abstract
Nuclear-encoded mutations causing metabolic and degenerative diseases have highly variable expressivity. Patients sharing the homozygous mutation (c.523delC) in the adenine nucleotide translocator 1 gene (SLC25A4, ANT1) develop cardiomyopathy that varies from slowly progressive to fulminant. This variability correlates with the mitochondrial DNA (mtDNA) lineage. To confirm that mtDNA variants can modulate the expressivity of nuclear DNA (nDNA)-encoded diseases, we combined in mice the nDNA Slc25a4-/- null mutation with a homoplasmic mtDNA ND6P25L or COIV421A variant. The ND6P25L variant significantly increased the severity of cardiomyopathy while the COIV421A variant was phenotypically neutral. The adverse Slc25a4-/- and ND6P25L combination was associated with impaired mitochondrial complex I activity, increased oxidative damage, decreased l-Opa1, altered mitochondrial morphology, sensitization of the mitochondrial permeability transition pore, augmented somatic mtDNA mutation levels, and shortened lifespan. The strikingly different phenotypic effects of these mild mtDNA variants demonstrate that mtDNA can be an important modulator of autosomal disease.Entities:
Keywords: F(1)F(o)-ATPase; OPA1; adenine nucleotide translocator; aging; cardiomyopathy; complex I; complex IV; mitochondrial DNA; mitochondrial-nuclear interaction; mtDNA instability
Mesh:
Substances:
Year: 2018 PMID: 30174309 PMCID: PMC6717513 DOI: 10.1016/j.cmet.2018.08.002
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287