| Literature DB >> 36129517 |
Cameron S McAlpine1,2,3, Máté G Kiss1,3, Faris M Zuraikat4,5, David Cheek3, Giulia Schiroli6,7, Hajera Amatullah8, Pacific Huynh1, Mehreen Z Bhatti5, Lai-Ping Wong9, Abi G Yates1, Wolfram C Poller1,3, John E Mindur3, Christopher T Chan1,3, Henrike Janssen1,3, Jeffrey Downey1,3, Sumnima Singh1,3, Ruslan I Sadreyev9,10, Matthias Nahrendorf3, Kate L Jeffrey8, David T Scadden6,7, Kamila Naxerova3, Marie-Pierre St-Onge4,5, Filip K Swirski1,3.
Abstract
A sleepless night may feel awful in its aftermath, but sleep's revitalizing powers are substantial, perpetuating the idea that convalescent sleep is a consequence-free physiological reset. Although recent studies have shown that catch-up sleep insufficiently neutralizes the negative effects of sleep debt, the mechanisms that control prolonged effects of sleep disruption are not understood. Here, we show that sleep interruption restructures the epigenome of hematopoietic stem and progenitor cells (HSPCs) and increases their proliferation, thus reducing hematopoietic clonal diversity through accelerated genetic drift. Sleep fragmentation exerts a lasting influence on the HSPC epigenome, skewing commitment toward a myeloid fate and priming cells for exaggerated inflammatory bursts. Combining hematopoietic clonal tracking with mathematical modeling, we infer that sleep preserves clonal diversity by limiting neutral drift. In humans, sleep restriction alters the HSPC epigenome and activates hematopoiesis. These findings show that sleep slows decay of the hematopoietic system by calibrating the hematopoietic epigenome, constraining inflammatory output, and maintaining clonal diversity.Entities:
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Year: 2022 PMID: 36129517 PMCID: PMC9499822 DOI: 10.1084/jem.20220081
Source DB: PubMed Journal: J Exp Med ISSN: 0022-1007 Impact factor: 17.579