Random point mutations with major effects on protein-coding genes are the driving force behind premature aging in mtDNA mutator mice. - Wikidata - wikimedia - TriplyDB

Random point mutations with major effects on protein-coding genes are the driving force behind premature aging in mtDNA mutator mice.

Random point mutations with major effects on protein-coding genes are the driving force behind premature aging in mtDNA mutator mice.

http://www.wikidata.org/entity/Q53379421

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Mitochondrial DNA replication and disease: insights from DNA polymerase γ mutations Changes in Regenerative Capacity through Lifespan Modelling age-related metabolic disorders in the mouse Endogenous Parkin Preserves Dopaminergic Substantia Nigral Neurons following Mitochondrial DNA Mutagenic Stress Mitochondria in the Aging Muscles of Flies and Mice: New Perspectives for Old Characters The hallmarks of aging Cancer and age related colonic crypt deficiencies in cytochrome c oxidase I Mitochondria and oxidative stress in heart aging Mitochondrial DNA mutations induce mitochondrial dysfunction, apoptosis and sarcopenia in skeletal muscle of mitochondrial DNA mutator mice Endurance exercise rescues progeroid aging and induces systemic mitochondrial rejuvenation in mtDNA mutator mice Addressing RNA integrity to determine the impact of mitochondrial DNA mutations on brain mitochondrial function with age.The mtDNA mutator mouse: Dissecting mitochondrial involvement in aging.Increased mtDNA mutations with aging promotes amyloid accumulation and brain atrophy in the APP/Ld transgenic mouse model of Alzheimer's disease.Inactivation of Pif1 helicase causes a mitochondrial myopathy in mice Chronic ethanol consumption increases myocardial mitochondrial DNA mutations: a potential contribution by mitochondrial topoisomerases Mitochondrial genome maintenance in health and disease.mip1 containing mutations associated with mitochondrial disease causes mutagenesis and depletion of mtDNA in Saccharomyces cerevisiae Ultra-deep sequencing of mouse mitochondrial DNA: mutational patterns and their origins.Mitochondrial DNA repair and association with aging--an update Mitochondrial DNA alterations and reduced mitochondrial function in aging Role of somatic mutations in vascular disease formation.Re-engineering the mitochondrial genomes in mammalian cells Therapeutic prospects for mitochondrial disease.High brain lactate is a hallmark of aging and caused by a shift in the lactate dehydrogenase A/B ratio DNA damage and base excision repair in mitochondria and their role in aging.Mitochondrial DNA mutations in mutator mice confer respiration defects and B-cell lymphoma development.Heterozygous Polg mutation causes motor dysfunction due to mtDNA deletions.Sensitivity to low-dose/low-LET ionizing radiation in mammalian cells harboring mutations in succinate dehydrogenase subunit C is governed by mitochondria-derived reactive oxygen species Dysregulation of mitochondrial quality control processes contribute to sarcopenia in a mouse model of premature aging.Metabolism, genomics, and DNA repair in the mouse aging liver.Ultra-sensitive sequencing reveals an age-related increase in somatic mitochondrial mutations that are inconsistent with oxidative damage Mitochondria DNA mutations cause sex-dependent development of hypertension and alterations in cardiovascular function Mitochondrial DNA mutations in disease and aging Post-translational decrease in respiratory chain proteins in the Polg mutator mouse brain.The mtDNA mutation spectrum of the progeroid Polg mutator mouse includes abundant control region multimers The pleiotropic effect of physical exercise on mitochondrial dynamics in aging skeletal muscle.Mitochondrial Diseases Part II: Mouse models of OXPHOS deficiencies caused by defects in regulatory factors and other components required for mitochondrial function.Mitochondrial oxidative stress in aortic stiffening with age: the role of smooth muscle cell function.TP53 codon 72 polymorphism affects accumulation of mtDNA damage in human cells.Visualization of mitochondrial respiratory function using cytochrome c oxidase/succinate dehydrogenase (COX/SDH) double-labeling histochemistry.

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Random point mutations with major effects on protein-coding genes are the driving force behind premature aging in mtDNA mutator mice.

http://www.wikidata.org/entity/Q53379421

description

2009 nî lūn-bûn

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2009年の論文

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2009年学术文章

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2009年学术文章

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2009年学术文章

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2009年学术文章

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2009年学术文章

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2009年學術文章

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2009年學術文章

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2009年學術文章

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name

Random point mutations with ma ...... e aging in mtDNA mutator mice.

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Random point mutations with ma ...... e aging in mtDNA mutator mice.

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type

label

Random point mutations with ma ...... e aging in mtDNA mutator mice.

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Random point mutations with ma ...... e aging in mtDNA mutator mice.

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Random point mutations with ma ...... e aging in mtDNA mutator mice.

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Random point mutations with ma ...... e aging in mtDNA mutator mice.

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J.CMET.2009.06.010

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Cell Metabolism

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Random point mutations with ma ...... e aging in mtDNA mutator mice.

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Aleksandra Trifunovic

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Barbara Cannon

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Daniel Edgar

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Leo Nijtmans

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Maria Antonietta Calvaruso

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Yolanda Camara

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131-138

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scholarly article

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10.1016/J.CMET.2009.06.010

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2

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10

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Irina G. Shabalina

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2009-08-01T00:00:00Z

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26718671

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19656491

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