Transcriptional dynamics of sleep deprivation and subsequent recovery sleep in the male mouse cortex.

IF 2.5 4区生物学 Q3 CELL BIOLOGY

Physiological genomics Pub Date : 2025-07-01 Epub Date: 2025-05-02 DOI:10.1152/physiolgenomics.00128.2024

Alexander Popescu, Caitlin Ottaway, Kaitlyn Ford, Elizabeth Medina, Taylor Wintler Patterson, Ashley Ingiosi, Stephanie C Hicks, Kristan Singletary, Lucia Peixoto

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引用次数: 0

Abstract

Sleep is an essential, tightly regulated biological function. Sleep is also a homeostatic process, with the need to sleep increasing as a function of being awake. Acute sleep deprivation (SD) increases sleep need, and subsequent recovery sleep (RS) discharges it. SD is known to alter brain gene expression in rodents, but it remains unclear which changes are linked to sleep homeostasis. To investigate this question, we analyzed RNA-seq data from adult male mice subjected to 3 and 5-6 h of SD and 2 and 6 h of subsequent RS. We hypothesized that molecular changes associated with sleep homeostasis would mirror sleep pressure dynamics as defined by brain electrical activity, peaking at 5-6 h of SD and no longer differentially expressed after 2 h of RS. We report that 5-6 h of SD produces the largest effect on gene expression, and the majority of differentially expressed genes normalize after 2 h of RS. These genes are involved in cellular redox homeostasis, DNA damage/repair, and chromatin regulation and may underlie the molecular basis of sleep homeostasis. Genes associated with cellular stress do not normalize within 6 h of RS and may underlie non-sleep-specific effects of SD. In addition, RS affects gene expression related to energy metabolism and Wnt-signaling, potentially contributing to its restorative effects. Finally, our study also points to the regulation of expression of a subset of circadian transcription factors as a function of sleep need. Overall, our results offer novel insights into the molecular mechanisms underlying sleep homeostasis and the broader effects of SD.NEW & NOTEWORTHY This study investigates different time points of sleep deprivation and recovery sleep to better understand the molecular processes influenced by sleep and lack of sleep. This study highlights redox metabolism, chromatin regulation, and DNA damage/repair as molecular mechanisms linked to sleep homeostasis while showing the effects of stress are probably non-sleep-specific based on transcriptional dynamics.

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睡眠剥夺和随后恢复睡眠在雄性小鼠皮层的转录动力学。

睡眠是一种重要的、受到严格调节的生物功能。睡眠也是一个自我平衡的过程，随着清醒，对睡眠的需求也在增加。急性睡眠剥夺（SD）会增加睡眠需求，随后的恢复性睡眠（RS）会消除这种需求。SD可以改变啮齿动物的大脑基因表达，但目前尚不清楚哪些变化与睡眠稳态有关。为了研究这个问题，我们分析了接受3小时和5-6小时SD以及随后2小时和6小时RS的成年雄性小鼠的RNA-seq数据。我们假设与睡眠稳态相关的分子变化反映了由脑电活动定义的睡眠压力动态。我们报告说，5-6小时的睡眠对基因表达的影响最大，大多数deg在2小时后恢复正常，这些基因参与细胞氧化还原稳态、DNA损伤/修复和染色质调节，可能是睡眠稳态的分子基础。与细胞应激相关的基因在睡眠后6小时内不会恢复正常，这可能是睡眠障碍非睡眠特异性效应的基础。此外，RS影响与能量代谢和wnt信号相关的基因表达，可能有助于其恢复作用。最后，我们的研究还指出了昼夜节律转录因子子集的表达调节作为睡眠需求的功能。总的来说，我们的研究结果为睡眠稳态的分子机制和SD的更广泛影响提供了新的见解。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Physiological genomics 生物-生理学

CiteScore

6.10

自引率

0.00%

发文量

审稿时长

4-8 weeks

期刊介绍： The Physiological Genomics publishes original papers, reviews and rapid reports in a wide area of research focused on uncovering the links between genes and physiology at all levels of biological organization. Articles on topics ranging from single genes to the whole genome and their links to the physiology of humans, any model organism, organ, tissue or cell are welcome. Areas of interest include complex polygenic traits preferably of importance to human health and gene-function relationships of disease processes. Specifically, the Journal has dedicated Sections focused on genome-wide association studies (GWAS) to function, cardiovascular, renal, metabolic and neurological systems, exercise physiology, pharmacogenomics, clinical, translational and genomics for precision medicine, comparative and statistical genomics and databases. For further details on research themes covered within these Sections, please refer to the descriptions given under each Section.