2012
DOI: 10.1093/hmg/dds435
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Universal heteroplasmy of human mitochondrial DNA

Abstract: Mammalian cells contain thousands of copies of mitochondrial DNA (mtDNA). At birth, these are thought to be identical in most humans. Here, we use long read length ultra-deep resequencing-by-synthesis to interrogate regions of the mtDNA genome from related and unrelated individuals at unprecedented resolution. We show that very low-level heteroplasmic variance is present in all tested healthy individuals, and is likely to be due to both inherited and somatic single base substitutions. Using this approach, we d… Show more

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Cited by 350 publications
(353 citation statements)
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“…Considering that heteroplasmy [11,40,44,45,107] and gene duplication of mitochondrial genes [46][47][48] are pervasive across taxa, the intraindividual level provides a new frontier for exploration of the evolutionary and medical significance of the mitonuclear interaction. A very striking example of the potential for intraindividual mitonuclear interaction was found in mice with artificially induced heteroplasmy between two wild-type mtDNAs, that of the Balb/cByJ mouse and that of the NZB/ BINJ mouse [108].…”
Section: Intraindividual Interactions and Biomedical Implicationsmentioning
confidence: 99%
See 1 more Smart Citation
“…Considering that heteroplasmy [11,40,44,45,107] and gene duplication of mitochondrial genes [46][47][48] are pervasive across taxa, the intraindividual level provides a new frontier for exploration of the evolutionary and medical significance of the mitonuclear interaction. A very striking example of the potential for intraindividual mitonuclear interaction was found in mice with artificially induced heteroplasmy between two wild-type mtDNAs, that of the Balb/cByJ mouse and that of the NZB/ BINJ mouse [108].…”
Section: Intraindividual Interactions and Biomedical Implicationsmentioning
confidence: 99%
“…Heteroplasmy [44,45], gene duplication of nuclear-encoded mitochondrial genes [48,116], as well as the genetic footprint of adaptive selection in mitochondrial gene trees [117][118][119] are pervasive in humans, and all of these factors have the potential to fuel mitonuclear interactions for key phenotypes, as outlined above. Thus, the coevolutionary processes underpinning the mitonuclear interaction may provide tangible insights into our understanding of the origins of mitochondrial disease, and ultimately help us to predict incidences and severity of disease expression.…”
Section: Intraindividual Interactions and Biomedical Implicationsmentioning
confidence: 99%
“…mtDNA | heteroplasmy | selection | human | tissue variation A lthough mtDNA heteroplasmy (intraindividual variability in mtDNA sequences) was initially thought to be rare in humans, studies using next-generation sequencing platforms have documented extensive heteroplasmy at low levels (<2%) (1)(2)(3)(4). Heteroplasmy is thought to represent an intermediate stage in the fixation of mtDNA mutations within an individual, and heteroplasmic mtDNA mutations have been implicated in various diseases, cancer, and aging (5)(6)(7)(8).…”
mentioning
confidence: 99%
“…Without considering these low-frequency heteroplasmy, the population prevalence of mitochondrial heteroplasmy is underestimated (12)(13)(14). Moreover, a preliminary study with ultra-deep sequencing (4,158∼20,803×) of two ∼300-bp mtDNA regions was able to find heteroplasmies with very low frequency (>0.2%) in all tested healthy samples (17). Further investigation with a large sample size and deep sequencing coverage across the whole mitochondrial genome is needed to reveal the universal prevalence of mtDNA heteroplasmy in healthy human populations.…”
mentioning
confidence: 99%