4.7 Article

Molecular Mechanisms Underlying the Retrieval and Extinction of Morphine Withdrawal-Associated Memories in the Basolateral Amygdala and Dentate Gyrus

Journal

BIOMEDICINES
Volume 10, Issue 3, Pages -

Publisher

MDPI
DOI: 10.3390/biomedicines10030588

Keywords

morphine withdrawal; conditioned place aversion; memory; dentate gyrus; basolateral amygdala; mTOR; Arc; Homer1; NMDA receptors

Funding

  1. ERDF A way of making Europe [MCIN/AEI/10.13039/501100011033]
  2. Fundacion Seneca [AF2017-85679-R, PID2020-113557RB-I00]
  3. Ayuda para la Formacion de Profesorado Universitario program of MICINN [21133/SF/19]
  4. ERDF A way of making Europe [AF2017-85679-R, PID2020-113557RB-I00]
  5. Fundacion Seneca, Region de Murcia, Spain [21133/SF/19]
  6. Ayuda para la Formacion de Profesorado Universitario program of MICINN [FPU19/01722]

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This study investigates the molecular mechanisms involved in the retrieval and extinction of morphine withdrawal memories in the basolateral amygdala (BLA) and the hippocampal dentate gyrus (DG) of rats. The results show differential expression and activity of synaptic molecules in these regions during the extinction of aversive memories of opiate withdrawal, providing evidence for the development of therapeutic strategies to minimize relapses induced by morphine withdrawal-associated aversive memories.
Despite their indisputable efficacy for pain management, opiate prescriptions remain highly controversial partially due to their elevated addictive potential. Relapse in drug use is one of the principal problems for addiction treatment, with drug-associated memories being among its main triggers. Consequently, the extinction of these memories has been proposed as a useful therapeutic tool. Hence, by using the conditioned place aversion (CPA) paradigm in rats, we investigated some of the molecular mechanisms that occurr during the retrieval and extinction of morphine withdrawal memories in the basolateral amygdala (BLA) and the hippocampal dentate gyrus (DG), which control emotional and episodic memories, respectively. The retrieval of aversive memories associated with the abstinence syndrome paralleled with decreased mTOR activity and increased Arc and GluN1 expressions in the DG. Additionally, Arc mRNA levels in this nucleus very strongly correlated with the CPA score exhibited by the opiate-treated rats. On the other hand, despite the unaltered mTOR phosphorylation, Arc levels augmented in the BLA. After the extinction test, Arc and GluN1 expressions were raised in both the DG and BLA of the control and morphine-treated animals. Remarkably, Homer1 expression in both areas correlated almost perfectly with the extinction showed by morphine-dependent animals. Moreover, Arc expression in the DG correlated strongly with the extinction of the CPA manifested by the group treated with the opiate. Finally, our results support the coordinated activity of some of these neuroplastic proteins for the extinction of morphine withdrawal memories in a regional-dependent manner. Present data provide evidence of differential expression and activity of synaptic molecules during the retrieval and extinction of aversive memories of opiate withdrawal in the amygdalar and hippocampal regions that will likely permit the development of therapeutic strategies able to minimize relapses induced by morphine withdrawal-associated aversive memories.

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