2023
DOI: 10.1101/2023.01.16.524266
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Ontogenesis of the molecular response to sleep loss

Abstract: Sleep deprivation (SD) results in profound cellular and molecular changes in the adult mammalian brain. Some of these changes may result in, or aggravate, brain disease. However, little is known about how SD impacts gene expression in developing animals. We examined the transcriptional response in the prefrontal cortex (PFC) to SD across postnatal development in male mice. We used RNA sequencing to identify functional gene categories that were specifically impacted by SD. We find that SD has dramatically diffe… Show more

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Cited by 1 publication
(3 citation statements)
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“…Recent mathematical modeling (12) and our current findings strongly indicate that sleep plays a unique role in shaping brain/synapse development in early life, transitioning to homeostatic functions with maturation. Distinct responses to SD between juvenile and adult mice is also supported by recently reported RNAseq analysis (39). The majority of neuronal synapses in the forebrain are formed after birth, during a period of profound synaptogenesis, followed by a period of activity dependent synapse pruning before synapse densities finally stabilize during maturation to adulthood (Fig.…”
Section: Discussionsupporting
confidence: 73%
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“…Recent mathematical modeling (12) and our current findings strongly indicate that sleep plays a unique role in shaping brain/synapse development in early life, transitioning to homeostatic functions with maturation. Distinct responses to SD between juvenile and adult mice is also supported by recently reported RNAseq analysis (39). The majority of neuronal synapses in the forebrain are formed after birth, during a period of profound synaptogenesis, followed by a period of activity dependent synapse pruning before synapse densities finally stabilize during maturation to adulthood (Fig.…”
Section: Discussionsupporting
confidence: 73%
“…Finally, our findings, together with a prior systematic EEG analysis show that juveniles lack well characterized adaptations to SD: increased NREM-SWA 37 , dark phase sleep rebound, induction of Homer1a, and accumulation of synaptic protein phosphorylation, potentially exposing the developing brain to greater vulnerabilities of SD. A recent RNAseq analysis from frontal cortex also shows almost no overlap in SD-induced gene expression changes between juvenile and adult mice 53 . Taken together, our findings suggest sleep plays a distinct and important role supporting brain maturation and highlight the developing synapse as a major node of vulnerability to sleep loss relevant for childhood onset forms of neurodevelopmental disorders.…”
Section: Discussionmentioning
confidence: 97%
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