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Calorie restriction modulates the transcription of genes related to stress response and longevity in human muscle: The <scp>CALERIE</scp> study
Jayanta Kumar Das, Nirad Banskota, Julián Candia, Michael Griswold, Melissa C. Orenduff, Rafael de Cabo, David L. Corcoran, Sai Krupa Das, Supriyo De, Kim M. Huffman, Virginia B. Kraus, William E. Kraus, Corby K. Martin, Susan B. Racette, Leanne M. Redman
Aging Cell · 2023 · ▲ 61 citations
Genomic instability
Loss of proteostasis
Mitochondrial dysfunction
Chronic inflammation
Caloric restriction
Human
Abstract
The lifespan extension induced by 40% caloric restriction(definition) (CR) in rodents is accompanied by postponement of disease, preservation of function, and increased stress resistance. Whether CR elicits the same physiological and molecular responses in humans remains mostly unexplored. In the CALERIE study, 12% CR for 2 years in healthy humans induced minor losses of muscle mass (leg lean mass) without changes of muscle strength, but mechanisms for muscle quality preservation remained unclear. We performed high-depth RNA-Seq (387-618 million paired reads) on human vastus lateralis muscle biopsies collected from the CALERIE participants at baseline, 12- and 24-month follow-up from the 90 CALERIE participants randomized to CR and "ad libitum" control. Using linear mixed effect model, we identified protein-coding genes and splicing variants whose expression was significantly changed in the CR group compared to controls, including genes related to proteostasis(definition), circadian rhythm regulation, DNA repair, mitochondrial biogenesis, mRNA processing/splicing, FOXO3 metabolism, apoptosis, and inflammation. Changes in some of these biological pathways mediated part of the positive effect of CR on muscle quality. Differentially expressed splicing variants were associated with change in pathways shown to be affected by CR in model organisms. Two years of sustained CR in humans positively affected skeletal muscle quality, and impacted gene expression and splicing profiles of biological pathways affected by CR in model organisms, suggesting that attainable levels of CR in a lifestyle intervention can benefit muscle health in humans.
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- DOI
- 10.1111/acel.13963
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- 2026-06-15 MST
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APA
Das, J.K., Banskota, N., Candia, J., Griswold, M., Orenduff, M.C., Cabo, R.D., Corcoran, D.L., Das, S.K., De, S., Huffman, K.M., Kraus, V.B., Kraus, W.E., Martin, C.K., Racette, S.B., Redman, L.M., Schilling, B., Belsky, D.W., & Ferrucci, L. (2023). Calorie restriction modulates the transcription of genes related to stress response and longevity in human muscle: The <scp>CALERIE</scp> study. <em>Aging Cell</em>. https://doi.org/10.1111/acel.13963
Vancouver
Das JK, Banskota N, Candia J, Griswold M, Orenduff MC, Cabo RD, et al. Calorie restriction modulates the transcription of genes related to stress response and longevity in human muscle: The <scp>CALERIE</scp> study. Aging Cell. 2023. doi:10.1111/acel.13963.
BibTeX
@article{jayanta2023Calori,
title = {Calorie restriction modulates the transcription of genes related to stress response and longevity in human muscle: The <scp>CALERIE</scp> study},
author = {Jayanta Kumar Das and Nirad Banskota and Julián Candia and Michael Griswold and Melissa C. Orenduff and Rafael de Cabo and David L. Corcoran and Sai Krupa Das and Supriyo De and Kim M. Huffman and Virginia B. Kraus and William E. Kraus and Corby K. Martin and Susan B. Racette and Leanne M. Redman and Birgit Schilling and Daniel W. Belsky and Luigi Ferrucci},
journal = {Aging Cell},
year = {2023},
doi = {10.1111/acel.13963},
}
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