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Articles, Cellular/Molecular

Effects of Sleep and Wake on Oligodendrocytes and Their Precursors

Michele Bellesi, Martha Pfister-Genskow, Stephanie Maret, Sunduz Keles, Giulio Tononi and Chiara Cirelli
Journal of Neuroscience 4 September 2013, 33 (36) 14288-14300; DOI: https://doi.org/10.1523/JNEUROSCI.5102-12.2013
Michele Bellesi
1Departments of Psychiatry and
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Martha Pfister-Genskow
1Departments of Psychiatry and
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Stephanie Maret
1Departments of Psychiatry and
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Sunduz Keles
2Biostatistics and Medical Informatics, University of Wisconsin-Madison, Madison, Wisconsin 53719
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Giulio Tononi
1Departments of Psychiatry and
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Chiara Cirelli
1Departments of Psychiatry and
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Abstract

Previous studies of differential gene expression in sleep and wake pooled transcripts from all brain cells and showed that several genes expressed at higher levels during sleep are involved in the synthesis/maintenance of membranes in general and of myelin in particular, a surprising finding given the reported slow turnover of many myelin components. Other studies showed that oligodendrocyte precursor cells (OPCs) are responsible for the formation of new myelin in both the injured and the normal adult brain, and that glutamate released from neurons, via neuron–OPC synapses, can inhibit OPC proliferation and affect their differentiation into myelin-forming oligodendrocytes. Because glutamatergic transmission is higher in wake than in sleep, we asked whether sleep and wake can affect oligodendrocytes and OPCs. Using the translating ribosome affinity purification technology combined with microarray analysis in mice, we obtained a genome-wide profiling of oligodendrocytes after sleep, spontaneous wake, and forced wake (acute sleep deprivation). We found that hundreds of transcripts being translated in oligodendrocytes are differentially expressed in sleep and wake: genes involved in phospholipid synthesis and myelination or promoting OPC proliferation are transcribed preferentially during sleep, while genes implicated in apoptosis, cellular stress response, and OPC differentiation are enriched in wake. We then confirmed through BrdU and other experiments that OPC proliferation doubles during sleep and positively correlates with time spent in REM sleep, whereas OPC differentiation is higher during wake. Thus, OPC proliferation and differentiation are not perfectly matched at any given circadian time but preferentially occur during sleep and wake, respectively.

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The Journal of Neuroscience: 33 (36)
Journal of Neuroscience
Vol. 33, Issue 36
4 Sep 2013
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Effects of Sleep and Wake on Oligodendrocytes and Their Precursors
Michele Bellesi, Martha Pfister-Genskow, Stephanie Maret, Sunduz Keles, Giulio Tononi, Chiara Cirelli
Journal of Neuroscience 4 September 2013, 33 (36) 14288-14300; DOI: 10.1523/JNEUROSCI.5102-12.2013

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Effects of Sleep and Wake on Oligodendrocytes and Their Precursors
Michele Bellesi, Martha Pfister-Genskow, Stephanie Maret, Sunduz Keles, Giulio Tononi, Chiara Cirelli
Journal of Neuroscience 4 September 2013, 33 (36) 14288-14300; DOI: 10.1523/JNEUROSCI.5102-12.2013
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  • INSIGHTS ON THE LINK AMONG MYELIN SHEATH PROLIFERATION AND SLEEP
    Isabella Panfoli
    Published on: 08 September 2013
  • Published on: (8 September 2013)
    Page navigation anchor for INSIGHTS ON THE LINK AMONG MYELIN SHEATH PROLIFERATION AND SLEEP
    INSIGHTS ON THE LINK AMONG MYELIN SHEATH PROLIFERATION AND SLEEP
    • Isabella Panfoli, Associate Professor
    • Other Contributors:
      • Alessandro M. Morelli

    In this study Authors report that oligodendrocyte precursor cell (OPCs) proliferation and differentiation preferentially occur during sleep and wake, respectively. In particular, genes involved in myelination are transcribed preferentially during sleep, so that OPC proliferation doubles during sleep. This is a very well constructed and significant study. We would like to comment on the fact that that these results are con...

    Show More

    In this study Authors report that oligodendrocyte precursor cell (OPCs) proliferation and differentiation preferentially occur during sleep and wake, respectively. In particular, genes involved in myelination are transcribed preferentially during sleep, so that OPC proliferation doubles during sleep. This is a very well constructed and significant study. We would like to comment on the fact that that these results are consistent with our previous reports. These showed that myelin sheath plays an energetic role (Morelli et al., 2011a), which may coincide with its trophic role in long-term axonal survival. We had also proposed that Myelin Basic Protein, whose role is not completely understood, may act as a proton (H+) sink during sleep to allowing myelin to handle H+ for oxidative phosphorylation during wake (Morelli et al., 2011b). Pointing at a role of OPCs and myelin in sleep, the paper from Bellesi et al., represents a step further towards our understanding of the phenomenon of sleep, one of the mysteries of biology. This is true especially considering that the traditionally accepted idea that synapses and spines are formed during sleep was surprisingly challenged by the same authors (Maret et al., 2011).

    CONFLICT OF INTEREST: Authors decare no Conflict of Interest

    REFERENCES

    Maret S, Faraguna U, Nelson AB, Cirelli C, Tononi G (2011) Sleep and waking modulate spine turnover in the adolescent mouse cortex. Nat Neurosci 14:1418-1420. Morelli A, Ravera S, Panfoli I (2011a) Hypothesis of an Energetic Function for Myelin. Cell Biochem Biophys. Morelli A, Ravera S, Panfoli I (2011b) Myelin sheath: a new possible role in sleep mechanism. Sleep Med 12:199.

    Conflict of Interest:

    None declared

    Show Less
    Competing Interests: None declared.

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