作者
Marco Sandri, Laura Barberi, AY Bijlsma, Bert Blaauw, KA Dyar, G Milan, Cristina Mammucari, CGM Meskers, G Pallafacchina, Antonio Paoli, D Pion, M Roceri, V Romanello, AL Serrano, Luana Toniolo, Lars Larsson, AB Maier, P Muñoz-Cánoves, Antonio Musarò, M Pende, Carlo Reggiani, Rosario Rizzuto, S Schiaffino
发表日期
2013/6
期刊
Biogerontology
卷号
14
页码范围
303-323
出版商
Springer Netherlands
简介
During ageing skeletal muscles undergo a process of structural and functional remodelling that leads to sarcopenia, a syndrome characterized by loss of muscle mass and force and a major cause of physical frailty. To determine the causes of sarcopenia and identify potential targets for interventions aimed at mitigating ageing-dependent muscle wasting, we focussed on the main signalling pathway known to control protein turnover in skeletal muscle, consisting of the insulin-like growth factor 1 (IGF1), the kinase Akt and its downstream effectors, the mammalian target of rapamycin (mTOR) and the transcription factor FoxO. Expression analyses at the transcript and protein level, carried out on well-characterized cohorts of young, old sedentary and old active individuals and on mice aged 200, 500 and 800 days, revealed only modest age-related differences in this pathway. Our findings suggest that during …
引用总数
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