Selective Inhibition of Amygdala Neuronal Ensembles Encoding Nicotine-Associated Memories Inhibits Nicotine Preference and Relapse.

Yan-Xue Xue Ya-Yun Chen Li-Bo Zhang Li-Qun Zhang Geng-Di Huang Shi-Chao Sun Jia-Hui Deng Yi-Xiao Luo Yan-Ping Bao Ping Wu Ying Han Bruce T Hope Yavin Shaham Jie Shi Lin Lu

Biol Psychiatry

Peking University Sixth Hospital and Institute of Mental Health, Peking University, Beijing, China; National Institute on Drug Dependence and Beijing Key Laboratory of Drug Dependence, Peking University, Beijing, China; National Clinical Research Center for Mental Disorders and Key Laboratory of Mental Health, Ministry of Health, Peking University, Beijing, China; Peking-Tsinghua Center for Life Sciences and PKU-IDG/McGovern Institute for Brain Research, Peking University, Beijing, China. Electronic address:

Published: December 2017

Researchers found that reactivating nicotine reward memories can trigger cravings and relapse, but using a specific memory interference technique reduced these cravings in rats and smokers.* -
The study involved injecting a protein synthesis inhibitor into rats after they experienced nicotine, which prevented them from relapsing or seeking nicotine again after a break.* -
The brain region studied, the basolateral amygdala, showed that different groups of neurons were responsible for storing different types of nicotine reward memories, and selectively targeting these neurons reduced cravings and relapse.*

Background: Nicotine craving and relapse often occurs after reactivation of nicotine reward memories. We recently developed a memory retrieval-reconsolidation interference procedure in which reactivating nicotine reward memories by acute exposure to nicotine (the unconditioned stimulus [UCS]) and then pharmacologically interfering with memory reconsolidation decreased relapse to nicotine seeking in rats and nicotine craving in smokers. Here, we investigated underlying mechanisms.

Methods: In the first series of experiments, we trained rats for nicotine-induced conditioned place preference (CPP) or nicotine self-administration and ventricularly microinjected them with the protein synthesis inhibitor anisomycin immediately after UCS-induced memory retrieval. In the second series of experiments, we used tyramide-amplified immunohistochemistry-fluorescence in situ hybridization to examine neural ensembles in the basolateral amygdala (BLA) reactivated by nicotine conditioned stimulus- or UCS-induced memory retrieval. We then used the Daun02 chemogenetic inactivation procedure to selectively inhibit the nicotine UCS-reactivated BLA neuronal ensembles.

Results: Ventricular injections of the anisomycin immediately after nicotine UCS memory retrieval inhibited subsequent nicotine CPP and relapse to operant nicotine seeking after short or prolonged abstinence. More important, within BLA, distinct neuronal ensembles encoded pavlovian CPP and operant self-administration reward memories and nicotine (the UCS) injections in the home cage reactivated both neuronal ensembles. Daun02 chemogenetic inactivation of the nicotine-reactivated ensembles inhibited both nicotine CPP and relapse to nicotine seeking.

Conclusions: Results demonstrate that the nicotine UCS-induced memory retrieval manipulation reactivates multiple nicotine reward memories that are encoded by distinct BLA neuronal ensembles that play a role in nicotine preference and relapse.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6192421	PMC
http://dx.doi.org/10.1016/j.biopsych.2017.04.017	DOI Listing

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