ARNT2 Tunes Activity-Dependent Gene Expression through NCoR2-Mediated Repression and NPAS4-Mediated Activation

Nikhil Sharma, Elizabeth A. Pollina, M. Aurel Nagy, Ee Lynn Yap, Florence A. DiBiase, Sinisa Hrvatin, Linda Hu, Cindy Lin, Michael E. Greenberg

Research output: Contribution to journalArticlepeer-review

30 Scopus citations

Abstract

Neuronal activity-dependent transcription is tuned to ensure precise gene induction during periods of heightened synaptic activity, allowing for appropriate responses of activated neurons within neural circuits. The consequences of aberrant induction of activity-dependent genes on neuronal physiology are not yet clear. Here, we demonstrate that, in the absence of synaptic excitation, the basic-helix-loop-helix (bHLH)-PAS family transcription factor ARNT2 recruits the NCoR2 co-repressor complex to suppress neuronal activity-dependent regulatory elements and maintain low basal levels of inducible genes. This restricts inhibition of excitatory neurons, maintaining them in a state that is receptive to future sensory stimuli. By contrast, in response to heightened neuronal activity, ARNT2 recruits the neuronal-specific bHLH-PAS factor NPAS4 to activity-dependent regulatory elements to induce transcription and thereby increase somatic inhibitory input. Thus, the interplay of bHLH-PAS complexes at activity-dependent regulatory elements maintains temporal control of activity-dependent gene expression and scales somatic inhibition with circuit activity.

Original languageEnglish
Pages (from-to)390-406.e9
JournalNeuron
Volume102
Issue number2
DOIs
StatePublished - Apr 17 2019

Keywords

  • ARNT2
  • NCoR2
  • NPAS4
  • activity-dependent transcription
  • enhancer
  • genomics
  • inhibitory circuit
  • repression
  • transcriptional regulation

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