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Telomere attrition: metabolic regulation and signalling function?
Stefania Casagrande, Michaela Hau
Biology Letters · 2019 · ▲ 113 citations
Abstract
Stress exposure can leave long-term footprints within the organism, like in telomeres (TLs), protective chromosome caps that shorten during cell replication and following exposure to stressors. Short TLs are considered to indicate lower fitness prospects, but why TLs shorten under stressful conditions is not understood. Glucocorticoid hormones (GCs) increase upon stress exposure and are thought to promote TL shortening by increasing oxidative damage. However, evidence that GCs are pro-oxidants and oxidative stress is causally linked to TL attrition is mixed . Based on new biochemical findings, we propose the metabolic telomere(definition) attrition hypothesis: during times of substantially increased energy demands, TLs are shortened as part of the transition into an organismal 'emergency state', which prioritizes immediate survival functions over processes with longer-term benefits. TL attrition during energy shortages could serve multiple roles including amplified signalling of cellular energy debt to re-direct critical resources to immediately important processes. This new view of TL shortening as a strategy to resolve major energetic trade-offs can improve our understanding of TL dynamics. We suggest that TLs are master regulators of cell homeostasis and propose future research avenues to understand the interactions between energy homeostasis, metabolic regulators and TL.
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- 10.1098/rsbl.2018.0885
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- 2026-06-12 MST
Cite this
APA
Casagrande, S., & Hau, M. (2019). Telomere attrition: metabolic regulation and signalling function?. <em>Biology Letters</em>. https://doi.org/10.1098/rsbl.2018.0885
Vancouver
Casagrande S, Hau M. Telomere attrition: metabolic regulation and signalling function?. Biology Letters. 2019. doi:10.1098/rsbl.2018.0885.
BibTeX
@article{stefania2019Telome,
title = {Telomere attrition: metabolic regulation and signalling function?},
author = {Stefania Casagrande and Michaela Hau},
journal = {Biology Letters},
year = {2019},
doi = {10.1098/rsbl.2018.0885},
}
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