2012
DOI: 10.1073/pnas.1217113109
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Mouse mtDNA mutant model of Leber hereditary optic neuropathy

Abstract: An animal model of Leber hereditary optic neuropathy (LHON) was produced by introducing the human optic atrophy mtDNA ND6 P25L mutation into the mouse. Mice with this mutation exhibited reduction in retinal function by elecroretinogram (ERG), age-related decline in central smaller caliber optic nerve fibers with sparing of larger peripheral fibers, neuronal accumulation of abnormal mitochondria, axonal swelling, and demyelination. Mitochondrial analysis revealed partial complex I and respiration defects and in… Show more

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Cited by 206 publications
(208 citation statements)
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“…Moreover, therapies for disorders caused by mutated mtDNA are inadequate, in large part because of the absence of animal models with mutated mtDNA and with the same genotype and phenotype as the human disorder that would help uncover the pathogenesis of disease and test potential avenues for treatment (11)(12)(13). Current procedures for the introduction of artificially mutagenized mtDNA into mitochondria have generated optic neuropathy in mice with a gene [ND6 G14600A (P25L)] that, when homoplasmic, is responsible for Leigh syndrome in humans (14).…”
mentioning
confidence: 99%
“…Moreover, therapies for disorders caused by mutated mtDNA are inadequate, in large part because of the absence of animal models with mutated mtDNA and with the same genotype and phenotype as the human disorder that would help uncover the pathogenesis of disease and test potential avenues for treatment (11)(12)(13). Current procedures for the introduction of artificially mutagenized mtDNA into mitochondria have generated optic neuropathy in mice with a gene [ND6 G14600A (P25L)] that, when homoplasmic, is responsible for Leigh syndrome in humans (14).…”
mentioning
confidence: 99%
“…2 Complex I deficit results in reduced oxygen consumption, increased reactive oxygen species, decreased energy supply and sensitization of the mitochondrial permeability transition pore (mtPTP) to apoptosis. 3,5 The retina is uniquely vulnerable to such insults, given its high energy demands and the nonreplicating nature of mammalian retinal neurons. 2,3,5 LHON is similar in etiology to dominant optic atrophy (DOA), which has been mapped to seven loci, with three genes (OPA1, OPA3 and TMEM126A/OPA7) identified to date.…”
Section: Introductionmentioning
confidence: 99%
“…3,5 The retina is uniquely vulnerable to such insults, given its high energy demands and the nonreplicating nature of mammalian retinal neurons. 2,3,5 LHON is similar in etiology to dominant optic atrophy (DOA), which has been mapped to seven loci, with three genes (OPA1, OPA3 and TMEM126A/OPA7) identified to date. These DOA genes are nuclear encoded, but have mitochondrial functions.…”
Section: Introductionmentioning
confidence: 99%
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“…These so-called 'mito-mice' carrying a mtDNA deletion encompassing 6tRNA and seven structural genes, a mutation in the genes encoding cytochrome oxidase I (COI) or NADH dehydrogenase 4 (ND6) have been generated [56]. Recently, using a homoplasmic G14600A ND6 mutant cell line, cybrids from this cell line were fused with ES cells depleted of mtDNA to generate a mouse with a mitochondrial mutation in ND6 [57] that recapitulates many features of LHON. The model suggests that LHON is due to oxidative stress rather than to ATP deficiency, because in this model, no reduction in ATP production was evident.…”
Section: Cellular Models Of Mitochondrial Diseasementioning
confidence: 99%