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Publication : Fasting induces a highly resilient deep quiescent state in muscle stem cells via ketone body signaling.

First Author  Benjamin DI Year  2022
Journal  Cell Metab Volume  34
Issue  6 Pages  902-918.e6
PubMed ID  35584694 Mgi Jnum  J:336973
Mgi Id  MGI:7286137 Doi  10.1016/j.cmet.2022.04.012
Citation  Benjamin DI, et al. (2022) Fasting induces a highly resilient deep quiescent state in muscle stem cells via ketone body signaling. Cell Metab 34(6):902-918.e6
abstractText  Short-term fasting is beneficial for the regeneration of multiple tissue types. However, the effects of fasting on muscle regeneration are largely unknown. Here, we report that fasting slows muscle repair both immediately after the conclusion of fasting as well as after multiple days of refeeding. We show that ketosis, either endogenously produced during fasting or a ketogenic diet or exogenously administered, promotes a deep quiescent state in muscle stem cells (MuSCs). Although deep quiescent MuSCs are less poised to activate, slowing muscle regeneration, they have markedly improved survival when facing sources of cellular stress. Furthermore, we show that ketone bodies, specifically beta-hydroxybutyrate, directly promote MuSC deep quiescence via a nonmetabolic mechanism. We show that beta-hydroxybutyrate functions as an HDAC inhibitor within MuSCs, leading to acetylation and activation of an HDAC1 target protein p53. Finally, we demonstrate that p53 activation contributes to the deep quiescence and enhanced resilience observed during fasting.
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