Journal
CELL METABOLISM
Volume 26, Issue 2, Pages 429-+Publisher
CELL PRESS
DOI: 10.1016/j.cmet.2017.07.003
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Funding
- Max Planck Society
- Swedish Research Council [2015-00418]
- Knut and Alice Wallenberg Foundation
- Swedish Research Council [2015-00418] Funding Source: Swedish Research Council
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Mutations of mtDNA cause mitochondrial diseases and are implicated in age-associated diseases and aging. Pathogenic mtDNA mutations are often present in a fraction of all mtDNA copies, and it has been widely debated whether the proportion of mutant genomes or the absolute number of wildtype molecules determines if oxidative phosphorylation (OXPHOS) will be impaired. Here, we have studied the male infertility phenotype of mtDNA mutator mice and demonstrate that decreasing mtDNA copy number worsens mitochondrial aberrations of spermatocytes and spermatids in testes, whereas an increase in mtDNA copy number rescues the fertility phenotype and normalizes testes morphology as well as spermatocyte proteome changes. The restoration of testes function occurs in spite of unaltered total mtDNA mutation load. We thus demonstrate that increased copy number of mtDNA can efficiently ameliorate a severe disease phenotype caused by mtDNA mutations, which has important implications for developing future strategies for treatment of mitochondrial dysfunction.
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