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Direct linkage of mitochondrial genome variation to risk factors for type 2 diabetes in conplastic strains
Pravenec M, Hyakukoku M, Houstek J, Zidek V, Landa V, Mlejnek P, Miksik I, Dudová-Mothejzikova K, Pecina P, Vrbacky M, Drahota Z, Vojtiskova A, Mracek T, Kazdova L, Oliyarnyk O, Wang J, Ho C, Qi N, Sugimoto K, Kurtz T
Language English Country United States
NLK
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from 1991 to 6 months ago
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from 1991-08-01 to 1 year ago
PubMed Central
from 1997 to 6 months ago
Europe PubMed Central
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Open Access Digital Library
from 1991-08-01
- MeSH
- Diabetes Mellitus, Type 2 genetics MeSH
- Financing, Organized MeSH
- Genetic Variation MeSH
- Genome MeSH
- Gene Dosage MeSH
- Haplotypes MeSH
- Rats MeSH
- DNA, Mitochondrial genetics MeSH
- Mitochondria enzymology genetics MeSH
- Polymorphism, Genetic MeSH
- Rats, Inbred BN MeSH
- Rats, Inbred SHR MeSH
- Electron Transport Complex IV genetics MeSH
- Risk Factors MeSH
- Base Sequence MeSH
- Sequence Analysis, DNA MeSH
- Amino Acid Substitution MeSH
- Animals MeSH
- Check Tag
- Rats MeSH
- Male MeSH
- Animals MeSH
Recently, the relationship of mitochondrial DNA (mtDNA) variants to metabolic risk factors for diabetes and other common diseases has begun to attract increasing attention. However, progress in this area has been limited because (1) the phenotypic effects of variation in the mitochondrial genome are difficult to isolate owing to confounding variation in the nuclear genome, imprinting phenomena, and environmental factors; and (2) few animal models have been available for directly investigating the effects of mtDNA variants on complex metabolic phenotypes in vivo. Substitution of different mitochondrial genomes on the same nuclear genetic background in conplastic strains provides a way to unambiguously isolate effects of the mitochondrial genome on complex traits. Here we show that conplastic strains of rats with identical nuclear genomes but divergent mitochondrial genomes that encode amino acid differences in proteins of oxidative phosphorylation exhibit differences in major metabolic risk factors for type 2 diabetes. These results (1) provide the first direct evidence linking naturally occurring variation in the mitochondrial genome, independent of variation in the nuclear genome and other confounding factors, to inherited variation in known risk factors for type 2 diabetes; and (2) establish that spontaneous variation in the mitochondrial genome per se can promote systemic metabolic disturbances relevant to the pathogenesis of common diseases.
Erratum in: Genome Res. 2008 Oct;18(10):1680.
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