AI Article Synopsis

  • Dietary protein plays a key role in healthy aging, with low-protein diets extending lifespan and improving healthspan in mice.
  • A significant reduction in amino acids, either overall or specifically isoleucine, led to decreased body fat and better glucose tolerance without cutting calorie intake.
  • Both dietary regimens also showed improvements in frailty and molecular markers of aging, suggesting potential benefits for healthy aging in older individuals.

Article Abstract

In defiance of the paradigm that calories from all sources are equivalent, we and others have shown that dietary protein is a dominant regulator of healthy aging. The restriction of protein or the branched-chain amino acid isoleucine promotes healthspan and extends lifespan when initiated in young or adult mice. However, many interventions are less efficacious or even deleterious when initiated in aged animals. Here, we investigate the physiological, metabolic, and molecular consequences of consuming a diet with a 67% reduction of all amino acids (Low AA), or of isoleucine alone (Low Ile), in male and female C57BL/6J.Nia mice starting at 20 months of age. We find that both diet regimens effectively reduce adiposity and improve glucose tolerance, which were benefits that were not mediated by reduced calorie intake. Both diets improve specific aspects of frailty, slow multiple molecular indicators of aging rate, and rejuvenate the aging heart and liver at the molecular level. These results demonstrate that Low AA and Low Ile diets can drive youthful physiological and molecular signatures, and support the possibility that these dietary interventions could help to promote healthy aging in older adults.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9934591PMC
http://dx.doi.org/10.1101/2023.02.06.527311DOI Listing

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