The adipokine leptin mediates muscle- and liver-derived IGF-1 in aged mice

The adipokine leptin mediates muscle- and liver-derived IGF-1 in aged mice

Muscle- and liver-derived IGF-1 play important roles in muscle anabolism throughout growth and aging. Yet, prolonged food restriction is thought to increase longevity in part by lowering levels of IGF-1, which in turn reduces the risk for developing various cancers. The dietary factors that modulate...

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Veröffentlicht in:Experimental gerontology 2015-10, Vol.70, p.92-96
Hauptverfasser: Hamrick, M.W., Dukes, A., Arounleut, P., Davis, C., Periyasamy-Thandavan, S., Mork, S., Herberg, S., Johnson, M.H., Isales, C.M., Hill, W.D., Otvos, L., Belin de Chantemèle, E.J.
Format: Artikel
Sprache:eng
Schlagworte:
Aging
Aging - metabolism
Animals
Body Weight - drug effects
Body Weight - physiology
Caloric Restriction
Calorie restriction
Eating
Food intake
Growth Hormone - blood
Insulin-Like Growth Factor I - drug effects
Insulin-Like Growth Factor I - metabolism
Leptin - pharmacology
Leptin - physiology
Liver - metabolism
Longevity
Longevity - physiology
Mice
Muscle, Skeletal - metabolism
Peptides - pharmacology
Receptors, Leptin - antagonists & inhibitors
Recombinant Proteins - pharmacology
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Zusammenfassung:Muscle- and liver-derived IGF-1 play important roles in muscle anabolism throughout growth and aging. Yet, prolonged food restriction is thought to increase longevity in part by lowering levels of IGF-1, which in turn reduces the risk for developing various cancers. The dietary factors that modulate IGF-1 levels are, however, poorly understood. We tested the hypothesis that the adipokine leptin, which is elevated with food intake and suppressed during fasting, is a key mediator of IGF-1 levels with aging and food restriction. First, leptin levels in peripheral tissues were measured in young mice fed ad libitum, aged mice fed ad libitum, and aged calorie-restricted (CR) mice. A group of aged CR mice were also treated with recombinant leptin for 10days. Later, aged mice fed ad libitum were treated with saline (VEH) or with a novel leptin receptor antagonist peptide (Allo-aca) and tissue-specific levels of IGF-1 were determined. On one hand, recombinant leptin induced a three-fold increase in liver-derived IGF-1 and a two-fold increase in muscle-derived IGF-1 in aged, CR mice. Leptin also significantly increased serum growth hormone levels in the aged, CR mice. On the other, the leptin receptor antagonist Allo-aca did not alter body weight or muscle mass in treated mice compared to VEH mice. Allo-aca did, however, produce a significant (20%) decline in liver-derived IGF-1 as well as an even more pronounced (>50%) decrease in muscle-derived IGF-1 compared to VEH-treated mice. The reduced IGF-1 levels in Allo-aca treated mice were not accompanied by any significant change in growth hormone levels compared to VEH mice. These findings suggest that leptin receptor antagonists may represent novel therapeutic agents for attenuating IGF-1 signaling associated with aging, and could potentially mimic some of the positive effects of calorie restriction on longevity. •Calorie restriction is thought to increase longevity by lowering levels of IGF-1•A leptin receptor antagonist reduced liver- and muscle-derived IGF-1 in aged mice•Leptin receptor antagonists may mimic some of the effects of calorie restriction
ISSN:0531-5565
1873-6815
DOI:10.1016/j.exger.2015.07.014