Effect of long‐term caloric restriction on telomere length in healthy adults: CALERIE™ 2 trial analysis

Author:

Hastings Waylon J.1ORCID,Ye Qiaofeng2,Wolf Sarah E.23,Ryan Calen P.4,Das Sai Krupa5ORCID,Huffman Kim M.6,Kobor Michael S.7,Kraus William E.6,MacIsaac Julia L.7,Martin Corby K.8,Racette Susan B.9ORCID,Redman Leanne M.8,Belsky Daniel W.410ORCID,Shalev Idan2ORCID

Affiliation:

1. Department of Psychiatry and Behavioral Sciences Tulane University School of Medicine New Orleans Louisiana USA

2. Department of Biobehavioral Health Pennsylvania State University, University Park State College Pennsylvania USA

3. Institute for Ecology and Evolution, School of Biological Sciences University of Edinburgh Edinburgh UK

4. Butler Columbia Aging Center Columbia University Mailman School of Public Health New York New York USA

5. Jean Mayer USDA Human Nutrition Research Center on Aging at Tufts University Boston Massachusetts USA

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

7. Edwin S.H. Leong Centre for Healthy Aging, Department of Medical Genetics University of British Columbia Vancouver British Columbia Canada

8. Pennington Biomedical Research Center Baton Rouge Louisiana USA

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

10. Department of Epidemiology Columbia University Mailman School of Public Health New York New York USA

Abstract

AbstractCaloric restriction (CR) modifies lifespan and aging biology in animal models. The Comprehensive Assessment of Long‐Term Effects of Reducing Intake of Energy (CALERIE™) 2 trial tested translation of these findings to humans. CALERIE™ randomized healthy, nonobese men and premenopausal women (age 21–50y; BMI 22.0–27.9 kg/m2), to 25% CR or ad‐libitum (AL) control (2:1) for 2 years. Prior analyses of CALERIE™ participants' blood chemistries, immunology, and epigenetic data suggest the 2‐year CR intervention slowed biological aging. Here, we extend these analyses to test effects of CR on telomere length (TL) attrition. TL was quantified in blood samples collected at baseline, 12‐, and 24‐months by quantitative PCR (absolute TL; aTL) and a published DNA‐methylation algorithm (DNAmTL). Intent‐to‐treat analysis found no significant differences in TL attrition across the first year, although there were trends toward increased attrition in the CR group for both aTL and DNAmTL measurements. When accounting for adherence heterogeneity with an Effect‐of‐Treatment‐on‐the‐Treated analysis, greater CR dose was associated with increased DNAmTL attrition during the baseline to 12‐month weight‐loss period. By contrast, both CR group status and increased CR were associated with reduced aTL attrition over the month 12 to month 24 weight maintenance period. No differences were observed when considering TL change across the study duration from baseline to 24‐months, leaving it unclear whether CR‐related effects reflect long‐term detriments to telomere fidelity, a hormesis‐like adaptation to decreased energy availability, or measurement error and insufficient statistical power. Unraveling these trends will be a focus of future CALERIE™ analyses and trials.

Publisher

Wiley

Cited by 1 articles. 订阅此论文施引文献 订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献

1. Can geroscience be translated into healthcare?;Zeitschrift für Gerontologie und Geriatrie;2024-07-09

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