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- Ayca Arslan-Ergul, Begun Erbaba, Elif Tugce Karoglu, Dilara Ozge Halim, and Michelle M Adams.
- Bilkent University, Interdisciplinary Neuroscience Program, Ankara, Turkey; Bilkent University, Molecular Biology and Genetics Department Zebrafish Facility, Ankara, Turkey; Bilkent University, UNAM-Institute of Materials Science and Nanotechnology, Ankara, Turkey. Electronic address: aycaergul@bilkent.edu.tr.
- Neuroscience. 2016 Oct 15; 334: 64-75.
AbstractBrain aging is marked by a decline in cognitive abilities and associated with neurodegenerative disorders. Recent studies have shown, neurogenesis continues into adulthood but is known to be decreasing during advancing age and these changes may contribute to cognitive alterations. Advances, which aim to promote better aging are of paramount importance. Dietary restriction (DR) is the only non-genetic intervention that reliably extends life- and health-span. Mechanisms of how and why DR and age affect neurogenesis are not well-understood, and have not been utilized much in the zebrafish, which has become a popular model to study brain aging and neurodegenerative disease due to widely available genetic tools. In this study we used young (8-8.5months) and old (26-32.5months) zebrafish as the model to investigate the effects of a short-term DR on actively proliferating cells. We successfully applied a 10-week DR to young and old fish, which resulted in a significant loss of body weight in both groups with no effect on normal age-related changes in body growth. We found that age decreased cell proliferation and increased senescence associated β-galactosidase, as well as shortened telomere lengths. In contrast, DR shortened telomere lengths only in young animals. Neither age nor DR changed the differentiation patterns of glial cells. Our results suggest that the potential effects of DR could be mediated by telomere regulation and whether these are beneficial or negative remains to be determined.Copyright © 2016 IBRO. Published by Elsevier Ltd. All rights reserved.
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