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Alcohol-specific transcriptional dynamics of memory reconsolidation and relapse.

Koral GoltsekerPatricia GarayKatherine M BonefasShigeki IwaseSegev Barak
Published in: Translational psychiatry (2023)
Relapse, a critical issue in alcohol addiction, can be attenuated by disruption of alcohol-associated memories. Memories are thought to temporarily destabilize upon retrieval during the reconsolidation process. Here, we provide evidence for unique transcriptional dynamics underpinning alcohol memory reconsolidation. Using a mouse place-conditioning procedure, we show that alcohol-memory retrieval increases the mRNA expression of immediate-early genes in the dorsal hippocampus and medial prefrontal cortex, and that alcohol seeking is abolished by post-retrieval non-specific inhibition of gene transcription, or by downregulating ARC expression using antisense-oligodeoxynucleotides. However, since retrieval of memories for a natural reward (sucrose) also increased the same immediate-early gene expression, we explored for alcohol-specific transcriptional changes using RNA-sequencing. We revealed a unique transcriptional fingerprint activated by alcohol memories, as the expression of this set of plasticity-related genes was not altered by sucrose-memory retrieval. Our results suggest that alcohol memories may activate two parallel transcription programs: one is involved in memory reconsolidation in general, and another is specifically activated during alcohol-memory processing.
Keyphrases
  • gene expression
  • alcohol consumption
  • working memory
  • transcription factor
  • poor prognosis
  • public health
  • single cell
  • genome wide
  • spinal cord
  • oxidative stress
  • neuropathic pain
  • genome wide identification
  • free survival