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Snord116-dependent diurnal rhythm of DNA methylation in mouse cortex

Author

Listed:
  • Rochelle L. Coulson

    (University of California)

  • Dag H. Yasui

    (University of California)

  • Keith W. Dunaway

    (University of California)

  • Benjamin I. Laufer

    (University of California)

  • Annie Vogel Ciernia

    (University of California)

  • Yihui Zhu

    (University of California)

  • Charles E. Mordaunt

    (University of California)

  • Theresa S. Totah

    (University of California)

  • Janine M. LaSalle

    (University of California)

Abstract

Rhythmic oscillations of physiological processes depend on integrating the circadian clock and diurnal environment. DNA methylation is epigenetically responsive to daily rhythms, as a subset of CpG dinucleotides in brain exhibit diurnal rhythmic methylation. Here, we show a major genetic effect on rhythmic methylation in a mouse Snord116 deletion model of the imprinted disorder Prader–Willi syndrome (PWS). More than 23,000 diurnally rhythmic CpGs are identified in wild-type cortex, with nearly all lost or phase-shifted in PWS. Circadian dysregulation of a second imprinted Snord cluster at the Temple/Kagami-Ogata syndrome locus is observed at the level of methylation, transcription, and chromatin, providing mechanistic evidence of cross-talk. Genes identified by diurnal epigenetic changes in PWS mice overlapped rhythmic and PWS-specific genes in human brain and are enriched for PWS-relevant phenotypes and pathways. These results support the proposed evolutionary relationship between imprinting and sleep, and suggest possible chronotherapy in the treatment of PWS and related disorders.

Suggested Citation

  • Rochelle L. Coulson & Dag H. Yasui & Keith W. Dunaway & Benjamin I. Laufer & Annie Vogel Ciernia & Yihui Zhu & Charles E. Mordaunt & Theresa S. Totah & Janine M. LaSalle, 2018. "Snord116-dependent diurnal rhythm of DNA methylation in mouse cortex," Nature Communications, Nature, vol. 9(1), pages 1-11, December.
  • Handle: RePEc:nat:natcom:v:9:y:2018:i:1:d:10.1038_s41467-018-03676-0
    DOI: 10.1038/s41467-018-03676-0
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