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      The Effects of Pharmacological Opioid Blockade on Neural Measures of Drug Cue-Reactivity in Humans

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          Abstract

          Interactions between dopaminergic and opioidergic systems have been implicated in the reinforcing properties of drugs of abuse. The present study investigated the effects of opioid blockade, via naltrexone, on functional magnetic resonance imaging (fMRI) measures during methamphetamine cue-reactivity to elucidate the role of endogenous opioids in the neural systems underlying drug craving. To investigate this question, non-treatment seeking individuals with methamphetamine use disorder ( N=23; 74% male, mean age=34.70 (SD=8.95)) were recruited for a randomized, placebo controlled, within-subject design and underwent a visual methamphetamine cue-reactivity task during two blood-oxygen-level dependent (BOLD) fMRI sessions following 3 days of naltrexone (50 mg) and matched time for placebo. fMRI analyses tested naltrexone-induced differences in BOLD activation and functional connectivity during cue processing. The results showed that naltrexone administration reduced cue-reactivity in sensorimotor regions and related to altered functional connectivity of dorsal striatum, ventral tegmental area, and precuneus with frontal, visual, sensory, and motor-related regions. Naltrexone also weakened the associations between subjective craving and precuneus functional connectivity with sensorimotor regions and strengthened the associations between subjective craving and dorsal striatum and precuneus connectivity with frontal regions. In conclusion, this study provides the first evidence that opioidergic blockade alters neural responses to drug cues in humans with methamphetamine addiction and suggests that naltrexone may be reducing drug cue salience by decreasing the involvement of sensorimotor regions and by engaging greater frontal regulation over salience attribution.

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          Author and article information

          Journal
          Neuropsychopharmacology
          Neuropsychopharmacology
          Neuropsychopharmacology
          Nature Publishing Group
          0893-133X
          1740-634X
          November 2016
          17 June 2016
          13 July 2016
          : 41
          : 12
          : 2872-2881
          Affiliations
          [1 ] Department of Psychology, University of California , Los Angeles, CA, USA
          [2 ] Department of Psychiatry and Biobehavioral Sciences, University of California , Los Angeles, CA, USA
          Author notes
          [* ] Department of Psychology, University of California , 1285 Franz Hall, Box 951563, Los Angeles, CA 90095-1563, USA, Tel: +1 310 794 5383, Fax: +1 310 206 5895, E-mail: lararay@ 123456psych.ucla.edu
          Article
          PMC5061897 PMC5061897 5061897 npp201699
          10.1038/npp.2016.99
          5061897
          27312405
          578240b2-684a-4cff-a5fd-7a8aad99eb9d
          Copyright © 2016 American College of Neuropsychopharmacology
          History
          : 20 December 2015
          : 15 May 2016
          : 08 June 2016
          Categories
          Original Article

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