Opposing mechanisms mediate morphine- and cocaine-induced generation of silent synapses

  • Nicholas M. Graziane
  • , Shichao Sun
  • , William J. Wright
  • , Daniel Jang
  • , Zheng Liu
  • , Yanhua H. Huang
  • , Eric J. Nestler
  • , Yu Tian Wang
  • , Oliver M. Schlüter
  • , Yan Dong

Research output: Contribution to journalArticlepeer-review

144 Scopus citations

Abstract

Exposures to cocaine and morphine produce similar adaptations in nucleus accumbens (NAc)-based behaviors, yet produce very different adaptations at NAc excitatory synapses. In an effort to explain this paradox, we found that both drugs induced NMDA receptor-containing, AMPA receptor-silent excitatory synapses, albeit in distinct cell types through opposing cellular mechanisms. Cocaine selectively induced silent synapses in D1-type neurons, likely via a synaptogenesis process, whereas morphine induced silent synapses in D2-type neurons via internalization of AMPA receptors from pre-existing synapses. After drug withdrawal, cocaine-generated silent synapses became 'unsilenced' by recruiting AMPA receptors to strengthen excitatory inputs to D1-type neurons, whereas morphine-generated silent synapses were likely eliminated to weaken excitatory inputs to D2-type neurons. Thus, these cell type-specific, opposing mechanisms produced the same net shift of the balance between excitatory inputs to D1- and D2-type NAc neurons, which may underlie certain common alterations in NAc-based behaviors induced by both classes of drugs.

Original languageEnglish (US)
Pages (from-to)915-925
Number of pages11
JournalNature Neuroscience
Volume19
Issue number7
DOIs
StatePublished - Jul 1 2016

All Science Journal Classification (ASJC) codes

  • General Neuroscience

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