Sarcopenia Clinical Trial
Official title:
Role of Hypoxia Inducible Factor-1α (HIF-1α) in Skeletal Muscle Aging
Deficits in skeletal muscle function exist during aging and muscular dystrophy, and suboptimal function has been related to factors such as atrophy, excessive inflammation and fibrosis. Sarcopenia is the age-related loss of skeletal muscle mass and function. It is now recognised as a major clinical problem for older people and research in the area is expanding exponentially. This interest stems from the fact that sarcopenia is both common and associated with serious health consequences in terms of frailty, disability, morbidity and mortality. The age-related loss of human skeletal muscle mass is due to a decrease in myofibre size and number with the loss of both fast and slow type myofibres, although the loss of fast myofibres tends to start earlier, at ∼70 years. Many factors influence the decrease in muscle mass. A significant contributor is an anabolic resistance of older skeletal muscle to protein nutrition as seen during immobilisation which can be ameliorated at least in part by resistance exercise and dietary supplementation. Other intensive areas of research are related to the loss of innervation and oxidative damage. Moreover, ineffective muscle regeneration underlies each condition and has been attributed to a deficit in myogenic potential of resident stem cells or satellite cells. It is now widely accepted that satellite cells, and generally adult stem cells, are normally quiescent and tend to reside in hypoxic areas of the tissue to preserve their undifferentiated state. To govern these processes, cells have developed a very complex machinery that is mainly regulated by a group of transcription factors known as hypoxia-inducible factors (HIFs). In particular, several observations support the idea that oxygen deprivation and HIF-1a may play a key role during ischemia to activate the regeneration process, which, after an initial hypoxic insult, needs to proceed under normoxia. On these bases, in this study we will investigate the role of HIF-1a in skeletal atrophy during aging.
Deficits in skeletal muscle function exist during aging and muscular dystrophy, and
suboptimal function has been related to factors such as atrophy, excessive inflammation and
fibrosis. Sarcopenia is the age-related loss of skeletal muscle mass and function. It is now
recognised as a major clinical problem for older people and research in the area is expanding
exponentially. This interest stems from the fact that sarcopenia is both common and
associated with serious health consequences in terms of frailty, disability, morbidity and
mortality. The age-related loss of human skeletal muscle mass is due to a decrease in
myofibre size and number with the loss of both fast and slow type myofibres, although the
loss of fast myofibres tends to start earlier, at ∼70 years. Many factors influence the
decrease in muscle mass. A significant contributor is an anabolic resistance of older
skeletal muscle to protein nutrition as seen during immobilisation which can be ameliorated
at least in part by resistance exercise and dietary supplementation. Other intensive areas of
research are related to the loss of innervation and oxidative damage. Moreover, ineffective
muscle regeneration underlies each condition and has been attributed to a deficit in myogenic
potential of resident stem cells or satellite cells. It is now widely accepted that satellite
cells, and generally adult stem cells, are normally quiescent and tend to reside in hypoxic
areas of the tissue to preserve their undifferentiated state. To govern these processes,
cells have developed a very complex machinery that is mainly regulated by a group of
transcription factors known as hypoxia-inducible factors (HIFs). In particular, several
observations support the idea that oxygen deprivation and HIF-1a may play a key role during
ischemia to activate the regeneration process, which, after an initial hypoxic insult, needs
to proceed under normoxia. On these bases, in this study we will investigate the role of
HIF-1a in skeletal atrophy during aging.
In particular, we will isolate satellite cells from muscular biopsies harvested from old
sarcopenic patients and from young patients. The, we will measure HIF-1a levels and we will
compare them.
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