Epigenetic regulation of the circadian gene Per1 contributes to age-related changes in hippocampal memory

  • Janine L. Kwapis
  • , Yasaman Alaghband
  • , Enikö A. Kramár
  • , Alberto J. López
  • , Annie Vogel Ciernia
  • , André O. White
  • , Guanhua Shu
  • , Diane Rhee
  • , Christina M. Michael
  • , Emilie Montellier
  • , Yu Liu
  • , Christophe N. Magnan
  • , Siwei Chen
  • , Paolo Sassone-Corsi
  • , Pierre Baldi
  • , Dina P. Matheos
  • , Marcelo A. Wood

Research output: Contribution to journalArticlepeer-review

132 Scopus citations

Abstract

Aging is accompanied by impairments in both circadian rhythmicity and long-term memory. Although it is clear that memory performance is affected by circadian cycling, it is unknown whether age-related disruption of the circadian clock causes impaired hippocampal memory. Here, we show that the repressive histone deacetylase HDAC3 restricts long-term memory, synaptic plasticity, and experience-induced expression of the circadian gene Per1 in the aging hippocampus without affecting rhythmic circadian activity patterns. We also demonstrate that hippocampal Per1 is critical for long-term memory formation. Together, our data challenge the traditional idea that alterations in the core circadian clock drive circadian-related changes in memory formation and instead argue for a more autonomous role for circadian clock gene function in hippocampal cells to gate the likelihood of long-term memory formation.

Original languageEnglish
Article number3323
JournalNature Communications
Volume9
Issue number1
DOIs
StatePublished - 1 Dec 2018
Externally publishedYes

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