Effects of caloric restriction on mitochondrial function and gene transcripts in rat muscle
Endocrinology Division, Mayo Clinic, Rochester, Minnesota 55905 Rodent skeletal muscle mitochondrial DNA has been shown to be a potential site of oxidative damage during aging. Caloric restriction (CR) is reported to reduce oxidative stress and prolong life expectancy in rodents. Gene expression pro...
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Veröffentlicht in: | American journal of physiology: endocrinology and metabolism 2002-07, Vol.283 (1), p.E38-E43 |
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Zusammenfassung: | Endocrinology Division, Mayo Clinic, Rochester, Minnesota
55905
Rodent skeletal muscle mitochondrial DNA
has been shown to be a potential site of oxidative damage during aging.
Caloric restriction (CR) is reported to reduce oxidative stress and
prolong life expectancy in rodents. Gene expression profiling and
measurement of mitochondrial ATP production capacity were performed in
skeletal muscle of male rats after feeding them either a control diet
or calorie-restricted diet (60% of control diet) for 36 wk to
determine the potential mechanism of the beneficial effects of CR. CR
enhanced the transcripts of genes involved in reactive oxygen free
radical scavenging function, tissue development, and energy metabolism
while decreasing expression of those genes involved in signal
transduction, stress response, and structural and contractile proteins.
Real-time PCR measurments confirmed the changes in transcript levels of
cytochrome- c oxidase III, superoxide dismutase (SOD)1, and
SOD2 that were noted by the microarray approach. Mitochondrial ATP
production and citrate synthase were unaltered by the dietary changes.
We conclude that CR alters transcript levels of several genes in
skeletal muscle and that mitochondrial function in skeletal muscle
remains unaltered by the dietary intervention. Alterations in
transcripts of many genes involved in reactive oxygen scavenging
function may contribute to the increase in longevity reported with CR.
rat muscle; microarrays and mitochondrial adenosine 5'-triphosphate
production |
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ISSN: | 0193-1849 1522-1555 |
DOI: | 10.1152/ajpendo.00387.2001 |