Identificador persistente para citar o vincular este elemento: http://hdl.handle.net/10553/77504
Título: Age associated low mitochondrial biogenesis may be explained by lack of response of PGC-1 alpha to exercise training
Autores/as: Derbre, Frederic
Gómez-Cabrera, Mari Carmen
Nascimento, Ana Lucia
Sanchis-Gomar, Fabian
Essau Martinez-Bello, Vladimir
Tresguerres, Jesus A. F.
Fuentes, Teresa 
Gratas-Delamarche, Arlette
Monsalve, Maria
Viña, Jose
Clasificación UNESCO: 32 Ciencias médicas
320502 Endocrinología
Palabras clave: Mouse Skeletal-Muscle
Calorie Restriction
Physical-Exercise
Fiber-Type
Coactivator, et al.
Fecha de publicación: 2012
Publicación seriada: Age 
Resumen: Low mitochondriogenesis is critical to explain loss of muscle function in aging and in the development of frailty. The aim of this work was to explain the mechanism by which mitochondriogenesis is decreased in aging and to determine to which extent it may be prevented by exercise training. We used aged rats and compared them with peroxisome proliferator-activated receptor-gamma coactivator-1 alpha deleted mice (PGC-1 alpha KO). PGC-1 alpha KO mice showed a significant decrease in the mitochondriogenic pathway in muscle. In aged rats, we found a loss of exercise-induced expression of PGC-1 alpha, nuclear respiratory factor-1 (NRF-1), and of cytochrome C. Thus muscle mitochondriogenesis, which is activated by exercise training in young animals, is not in aged or PGC-1 alpha KO ones. Other stimuli to increase PGC-1 alpha synthesis apart from exercise training, namely cold induction or thyroid hormone treatment, were effective in young rats but not in aged ones. To sum up, the low mitochondrial biogenesis associated with aging may be due to the lack of response of PGC-1 alpha to different stimuli. Aged rats behave as PGC-1 alpha KO mice. Results reported here highlight the role of PGC-1 alpha in the loss of mitochondriogenesis associated with aging and point to this important transcriptional coactivator as a target for pharmacological interventions to prevent age-associated sarcopenia.
URI: http://hdl.handle.net/10553/77504
ISSN: 0161-9152
DOI: 10.1007/s11357-011-9264-y
Fuente: Age [ISSN 0161-9152], v. 34 (3), p. 669-679, (Junio 2012)
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