4.7 Article

Molecular and Functional Networks Linked to Sarcopenia Prevention by Caloric Restriction in Rhesus Monkeys

期刊

CELL SYSTEMS
卷 10, 期 2, 页码 156-+

出版社

CELL PRESS
DOI: 10.1016/j.cels.2019.12.002

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资金

  1. NIH [AG037000, AG011915, AG047358, AG040178, AG000213]
  2. Department of Medicine, University of Wisconsin-Madison
  3. School of Medicine, University of Wisconsin-Madison
  4. Public Health, University of Wisconsin-Madison
  5. [P51OD011106]
  6. [RR15459-01]
  7. [RR020141-01]

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Caloric restriction (CR) improves survival in nonhuman primates and delays the onset of age-related morbidities including sarcopenia, which is characterized by the age-related loss of muscle mass and function. A shift in metabolism anticipates the onset of muscle-aging phenotypes in nonhuman primates, suggesting a potential role for metabolism in the protective effects of CR. Here, we show that CR induced profound changes in muscle composition and the cellular metabolic environment. Bioinformatic analysis linked these adaptations to proteostasis, RNA processing, and lipid synthetic pathways. At the tissue level, CR maintained contractile content and attenuated age-related metabolic shifts among individual fiber types with higher mitochondrial activity, altered redox metabolism, and smaller lipid droplet size. Biometric and metabolic rate data confirm preserved metabolic efficiency in CR animals that correlated with the attenuation of age-related muscle mass and physical activity. These data suggest that CR-induced reprogramming of metabolism plays a role in delayed aging of skeletal muscle in rhesus monkeys.

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