Calorie restriction modulates the transcription of genes related to stress response and longevity in human muscle: The CALERIE study

Author:

Das Jayanta Kumar1ORCID,Banskota Nirad2,Candia Julián1ORCID,Griswold Michael E.3,Orenduff Melissa4,de Cabo Rafael5ORCID,Corcoran David L.6,Das Sai Krupa7ORCID,De Supriyo2,Huffman Kim Marie4,Kraus Virginia B.4,Kraus William E.4,Martin Corby K.8,Racette Susan B.9,Redman Leanne M.8,Schilling Birgit10,Belsky Daniel W.11ORCID,Ferrucci Luigi1ORCID

Affiliation:

1. Longitudinal Studies Section, Translation Gerontology Branch National Institute on Aging, National Institutes of Health Baltimore Maryland USA

2. Computational Biology and Genomics Core National Institute on Aging, National Institutes of Health Baltimore Maryland USA

3. MIND Center, UMMC School of Medicine Jackson Mississippi USA

4. Duke Molecular Physiology Institute and Department of Medicine Duke University School of Medicine Durham North Carolina USA

5. Translation Gerontology Branch, National Institute on Aging National Institutes of Health Baltimore Maryland USA

6. Department of Genetics University of North Carolina at Chapel Hill Chapel Hill North Carolina USA

7. Energy Metabolism, Jean Mayer USDA Human Nutrition Research Center on Aging Tufts University Boston Massachusetts USA

8. Pennington Biomedical Research Center Louisiana State University Baton Rouge Louisiana USA

9. College of Health Solutions Arizona State University Phoenix Arizona USA

10. The Buck Institute for Research on Aging Novato California USA

11. Department of Epidemiology & Butler Columbia Aging Center Columbia University Mailman School of Public Health New York City New York USA

Abstract

AbstractThe lifespan extension induced by 40% caloric restriction (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, 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.

Funder

National Institute on Aging

Publisher

Wiley

Subject

Cell Biology,Aging

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1. Emerging epigenetic insights into aging mechanisms and interventions;Trends in Pharmacological Sciences;2024-02

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