Affiliation:
1. Princess Máxima Center for Pediatric Oncology Utrecht Netherlands
2. Oncode Institute Utrecht Netherlands
3. School of Biological Sciences University of Reading Reading UK
4. College of Medicine Wasit University Kut Iraq
5. III. Department of Medicine University Medical Center Hamburg‐Eppendorf Hamburg Germany
6. Hamburg Center for Kidney Health (HCKH) Hamburg Germany
7. Department of Neuroscience Erasmus University Medical Center Rotterdam Rotterdam Netherlands
8. Department of Molecular Genetics, Erasmus MC Cancer Institute Erasmus University Medical Center Rotterdam Rotterdam Netherlands
9. School of Pharmacy University of Reading Reading UK
10. Department of Physiology University of Helsinki Helsinki Finland
Abstract
AbstractBackgroundAgeing is a complex multifactorial process, impacting all organs and tissues, with DNA damage accumulation serving as a common underlying cause. To decelerate ageing, various strategies have been applied to model organisms and evaluated for health and lifespan benefits. Dietary restriction (DR, also known as caloric restriction) is a well‐established long‐term intervention recognized for its universal anti‐ageing effects. DR temporarily suppresses growth, and when applied to progeroid DNA repair‐deficient mice doubles lifespan with systemic health benefits. Counterintuitively, attenuation of myostatin/activin signalling by soluble activin receptor (sActRIIB), boosts the growth of muscle and, in these animals, prevents muscle wasting, improves kidney functioning, and compresses morbidity.MethodsHere, we investigated a combined approach, applying an anabolic regime (sActRIIB) at the same time as DR to Ercc1Δ/− progeroid mice. Following both single treatments and combined, we monitored global effects on body weight, lifespan and behaviour, and local effects on muscle and tissue weight, muscle morphology and function, and ultrastructural and transcriptomic changes in muscle and kidney.ResultsLifespan was mostly influenced by DR (extended from approximately 20 to 40 weeks; P < 0.001), with sActRIIB clearly increasing muscle mass (35–65%) and tetanic force (P < 0.001). The combined regime yielded a stable uniform body weight, but increased compared with DR alone, synergistically improved motor coordination and further delayed the onset and development of balance problems. sActRIIB significantly increased muscle fibre size (P < 0.05) in mice subjected to DR and lowered all signs of muscle damage. Ercc1Δ/− mice showed abnormal neuromuscular junctions. Single interventions by sActRIIB treatment or DR only partially rescued this phenotype, while in the double intervention group, the regularly shaped junctional foldings were maintained. In kidney of Ercc1Δ/− mice, we observed a mild but significant foot process effacement, which was restored by either intervention. Transcriptome analysis also pointed towards reduced levels of DNA damage in muscle and kidney by DR, but not sActRIIB, while these levels retained lower in the double intervention.ConclusionsIn muscle, we found synergistic effects of combining sActRIIB with DR, but not in kidney, with an overall better health in the double intervention group. Crucially, the benefits of each single intervention are not lost when administered in combination, but rather strengthened, even when sActRIIB was applied late in life, opening opportunities for translation to human.
Funder
Deutsche Forschungsgemeinschaft
Bundesministerium für Bildung und Frauen
Nederlandse Organisatie voor Wetenschappelijk Onderzoek
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