The mtDNA Mutation Spectrum of the Progeroid Polg Mutator Mouse Includes Abundant Control Region Multimers

Williams, Steve K.; Huang, Jian; Edwards, Yvonne J. K.; Ulloa, Rick H.; Dillon, Lloye M.; Prolla, Tomas A.; Vance, Jeffery M.; Moraes, Carlos T.; Züchner, Stephan

doi:10.1016/j.cmet.2010.11.012

Cited by 89 publications

(112 citation statements)

References 32 publications

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“…The mtDNA mutator mice are homozygous for a knock-in mutation that leads to the expression of a proofreading-deficient catalytic subunit of mtDNA polymerase (PolgA mut ). The expression of PolgA mut causes extensive mtDNA mutagenesis with the formation of three different forms of mtDNA mutations: random point mutations, linear molecules with large deletions, and, in certain tissues, molecules containing multimers of the control region (an area of the mitochondrial genome that contains noncoding mtDNA) (58,60,61). Furthermore, a single report has argued that a fourth type of mtDNA mutation, consisting of circular mtDNA molecules with large deletions, is prevalent and even drives the premature aging phenotype (60).…”

Section: Are Mtdna Mutations a Driving Force In Aging?mentioning

confidence: 99%

The role of mitochondria in aging

Bratić¹,

Larsson²

2013

J. Clin. Invest.

853

670

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Over the last decade, accumulating evidence has suggested a causative link between mitochondrial dysfunction and major phenotypes associated with aging. Somatic mitochondrial DNA (mtDNA) mutations and respiratory chain dysfunction accompany normal aging, but the first direct experimental evidence that increased mtDNA mutation levels contribute to progeroid phenotypes came from the mtDNA mutator mouse. Recent evidence suggests that increases in aging-associated mtDNA mutations are not caused by damage accumulation, but rather are due to clonal expansion of mtDNA replication errors that occur during development. Here we discuss the caveats of the traditional mitochondrial free radical theory of aging and highlight other possible mechanisms, including insulin/IGF-1 signaling (IIS) and the target of rapamycin pathways, that underlie the central role of mitochondria in the aging process.

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Section: Are Mtdna Mutations a Driving Force In Aging?mentioning

confidence: 99%

The role of mitochondria in aging

Bratić¹,

Larsson²

2013

J. Clin. Invest.

853

670

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“…These mice express a proofreading-deficient version of the nuclear-encoded mitochondrial DNA polymerase gamma and, consequently, accumulate point mutations and deletions in their mitochondrial genome (7). These mice display a premature aging phenotype that substantially manifests around 9 mo of age with symptoms such as weight loss, s.c. lipodystrophy, alopecia, infertility, and anemia, ultimately resulting in death around 12 mo (6).…”

mentioning

confidence: 99%

High-fat diet and FGF21 cooperatively promote aerobic thermogenesis in mtDNA mutator mice

Wall

Whyte

Suh

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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Mitochondria are highly adaptable organelles that can facilitate communication between tissues to meet the energetic demands of the organism. However, the mechanisms by which mitochondria can nonautonomously relay stress signals remain poorly understood. Here we report that mitochondrial mutations in the young, preprogeroid polymerase gamma mutator (POLG) mouse produce a metabolic state of starvation. As a result, these mice exhibit signs of metabolic imbalance including thermogenic defects in brown adipose tissue (BAT). An unexpected benefit of this adaptive response is the complete resistance to diet-induced obesity when POLG mice are placed on a high-fat diet (HFD). Paradoxically, HFD further increases oxygen consumption in part by inducing thermogenesis and mitochondrial biogenesis in BAT along with enhanced expression of fibroblast growth factor 21 (FGF21). Collectively, these findings identify a mechanistic link between FGF21, a long-known marker of mitochondrial disease, and systemic metabolic adaptation in response to mitochondrial stress.

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“…There has been one study arguing that a third type of mutation, circular mtDNA molecules with deletions, drives the phenotype of mtDNA mutator mice (Vermulst et al, 2008). However, this study has been refuted in several independent studies, in which sensitive PCR assays (Edgar et al, 2009;Kraytsberg et al, 2009) or deep sequencing (Williams et al, 2010;Ameur et al, 2011) could not detect any significant levels of circular mtDNA molecules with deletions in various tissues of mtDNA mutator mice. In addition, the biochemical phenotype in mtDNA mutator mice is fully consistent with the idea that point mutations of mtDNA create amino acid substitutions of respiratory chain subunits, which explains the observed decline in the stability of the respiratory chain complexes (Edgar et al, 2009).…”

Section: Principles For Maternal Inheritance Of Mtdnamentioning

confidence: 77%