Macromolecule biosynthesis: a key function of sleep

Mackiewicz, Mirosław; Shockley, Keith R.; Romer, Micah; Galante, Raymond J.; Zimmerman, John E.; Naidoo, Nirinjini; Baldwin, Donald; Jensen, Shane T.; Churchill, Gary A.; Pack, Allan I.

doi:10.1152/physiolgenomics.00275.2006

Cited by 329 publications

(376 citation statements)

References 82 publications

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“…Again, the most significantly overexpressed gene after sleep deprivation was Homer1a, followed by those belonging to stress-response and synaptic-plasticity gene groups. The major functional gene groups that reduced their expression after sleep deprivation concern protein synthesis, membrane trafficking, and protein transport (SI Table 5) (12). Real-time quantitative RT-PCR verification for 41 candidate genes (found here and by others) at ZT6 confirmed our microarray findings at this reference time point (SI Table 6).…”

Section: Time-of-day Effects Of Sleep Loss On Brain Transcriptional Csupporting

confidence: 82%

“…According to the Ensemble database (Mus musculus release 46), this region contains 33 known genes, 15 potential unknown coding sequences, and three pseudogenes. Among these, the short splice variant of the Homer1 (Homer1a) gene is the only transcript in the region that was previously reported to be among the up-regulated genes after sleep deprivation (11)(12)(13)(14). However, the specificity of this finding, compared with other gene expression changes after sleep loss, has not yet been established.…”

Section: Resultsmentioning

confidence: 99%

See 1 more Smart Citation

Homer1a is a core brain molecular correlate of sleep loss

Maret¹,

Dorsaz²,

Gurcel³

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

344

380

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Sleep is regulated by a homeostatic process that determines its need and by a circadian process that determines its timing. By using sleep deprivation and transcriptome profiling in inbred mouse strains, we show that genetic background affects susceptibility to sleep loss at the transcriptional level in a tissue-dependent manner. In the brain, Homer1a expression best reflects the response to sleep loss. Timecourse gene expression analysis suggests that 2,032 brain transcripts are under circadian control. However, only 391 remain rhythmic when mice are sleep-deprived at four time points around the clock, suggesting that most diurnal changes in gene transcription are, in fact, sleep-wake-dependent. By generating a transgenic mouse line, we show that in Homer1-expressing cells specifically, apart from Homer1a, three other activity-induced genes (Ptgs2, Jph3, and Nptx2) are overexpressed after sleep loss. All four genes play a role in recovery from glutamate-induced neuronal hyperactivity. The consistent activation of Homer1a suggests a role for sleep in intracellular calcium homeostasis for protecting and recovering from the neuronal activation imposed by wakefulness.homeostasis ͉ microarray ͉ mRNA tagging ͉ sleep deprivation ͉ sleep function T wo main processes regulate sleep. A homeostatic process regulates sleep need and intensity according to the time spent awake or asleep. A circadian process regulates the appropriate timing of sleep and wakefulness across the 24-h day. A highly reliable index of the homeostatic process is provided by the amplitude and prevalence of delta (1-to 4-Hz) oscillations in the electroencephalogram (EEG) of nonrapid eye movement (NREM) sleep (hereafter, ''delta power''). Delta power is high at sleep onset and decreases during sleep, in parallel with sleep depth. Sleep deprivations and naps induce a predictable increase or decrease, respectively, in delta power during subsequent sleep. The interaction between homeostatic and circadian processes is mathematically described in the two-process model of sleep regulation, which provides a framework for prediction and interpretation of a large body of experimental data (1).Among hypotheses concerning the physiological function of waking-induced changes in sleep, the most compelling suggests that sleep plays a key role in synaptic plasticity (2, 3). More specifically, EEG delta power during NREM sleep has been shown to play a critical role in learning-induced plasticity (4-6). In general, the prediction is that local neural activation due to specific behavioral (cognitive) demands imposes a burden on the brain which necessitates sleep and which is reflected by the EEG delta power.On the basis of mathematical modeling and experimental data, we have shown that sleep need, as indexed by the EEG delta power, is under genetic control (7), which is of direct relevance for explaining the interindividual vulnerability to sleep loss in human subjects (8, 9). However, deciphering the molecular bases of sleep need is rendered difficult because the contr...

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Section: Time-of-day Effects Of Sleep Loss On Brain Transcriptional Csupporting

confidence: 82%

Section: Resultsmentioning

confidence: 99%

Homer1a is a core brain molecular correlate of sleep loss

Maret¹,

Dorsaz²,

Gurcel³

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

344

380

View full text Add to dashboard Cite

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“…Several studies suggest that BiP may also protect the cell against cell death by suppressing the accumulation of reactive oxygen species and by stabilizing mitochondrial function (Liu et al 1998;Lee et al 1999;Yu et al 1999). BiP has been demonstrated to increase following a few hours of sleep loss in the cerebral cortex of mice (Terao et al 2003;Naidoo et al 2005;Mackiewicz et al 2007) rats (Cirelli et al 2004;Terao et al 2006), in the head of fruit flies (Shaw et al 2000;Naidoo et al 2007), as well as in the telencephalon of the white-crowned sparrow (Jones et al 2007). However, its expression is not further increased in the rat cerebral cortex after long-term sleep deprivation relative to short-term sleep loss (Cirelli et al 2006).…”

Section: Discussionmentioning

confidence: 99%

Changes in brain gene expression during migration in the white-crowned sparrow

Jones

Pfister-Genskow

Cirelli

et al. 2008

Brain Research Bulletin

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Long-term recordings of seasonal sleep patterns in captive white-crowned sparrows (Zonotrichia leucophrys gambelii) have shown that these birds markedly reduce sleep time during the migratory period relative to the non-migratory period. It was also found that, despite this sleep reduction, sparrows showed no evidence of neurobehavioral deficits in a standard operant task used to assess the effects of sleep loss. In this study, we performed an extensive microarray analysis of gene expression in the sparrow telencephalon during the migratory season (M), relative to a 78-hour period of enforced sleep restriction during the non-migratory season (SR), and a 6-hour period of normal wakefulness during the non-migratory season (W). Of the estimated 17,100 transcripts that were reliably detected, only 0.17% changed expression as a function of M (relative to both SR and W), and 0.11% as a function of SR (relative to both M and W). Brain transcripts whose expression increased during M include the facilitated glucose transporter GLUT1, the presenilin associated rhomboid-like protein PARL, and several members of the heat shock protein family, such as HSP70, HSP90, GRP78 and BiP. These data suggest that migration is associated with brain cellular stress and enhanced energetic demands.

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“…Nelson and Raizen 2013), so the involvement of sleep in this process lends credence to a hypothesized role for sleep in macromolecular biosynthesis (Mackiewicz et al 2007;Nelson and Raizen 2013). In addition, large-scale synaptic formation and rearrangement in C. elegans occur during development.…”

Section: Worm Sleepmentioning

confidence: 96%

Sleep and Development in Genetically Tractable Model Organisms

Kayser

Biron

2016

Genetics

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Sleep is widely recognized as essential, but without a clear singular function. Inadequate sleep impairs cognition, metabolism, immune function, and many other processes. Work in genetic model systems has greatly expanded our understanding of basic sleep neurobiology as well as introduced new concepts for why we sleep. Among these is an idea with its roots in human work nearly 50 years old: sleep in early life is crucial for normal brain maturation. Nearly all known species that sleep do so more while immature, and this increased sleep coincides with a period of exuberant synaptogenesis and massive neural circuit remodeling. Adequate sleep also appears critical for normal neurodevelopmental progression. This article describes recent findings regarding molecular and circuit mechanisms of sleep, with a focus on development and the insights garnered from models amenable to detailed genetic analyses.

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Macromolecule biosynthesis: a key function of sleep

Cited by 329 publications

References 82 publications

Homer1a is a core brain molecular correlate of sleep loss

Homer1a is a core brain molecular correlate of sleep loss

Changes in brain gene expression during migration in the white-crowned sparrow

Sleep and Development in Genetically Tractable Model Organisms

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