Addiction Clinical Trial
Official title:
Dopamine D2/3- and μ-opioid Receptor Antagonists Reduce Cue-induced Reward Responding and Reward Impulsivity in Healthy Volunteers
The purpose of this study is to determine how the dopamine and opioid system is involved in reward processing, specifically in cue-induced reward responding and reward impulsivity, using dopamine and opioid receptor antagonists in healthy participants. The investigators predict that particularly the dopamine challenge should alter cue-induced reward responding and reward impulsivity. Such effects would be of high interest for the treatment of disorders which involve impairments of reward processing such as addiction.
In this study the investigators use amisulpride and naltrexone to elucidate what function
the dopamine and opioid system have in the processing of reward. Amisulpride [Solian®;
sanofi-aventis] is an atypical antipsychotic and acts as an antagonist at dopamine D2 and D3
(D2/D3) receptors with very high specificity. Amisulpride has been used in numerous past
studies to study the role of dopamine in the brain, for example in studies on reinforcement
learning, memory, and attentional bias in stimulant dependence. Naltrexone [Naltrexin®;
OrPha Swiss GmbH] is an opioid antagonist and is clinically used in the management of
alcohol and opioid dependence. It has been used to investigate the role of opioid in pain
perception, taste detection and recognition, and smoking behavior. The investigators were
interested in particular how amisulpride and naltrexone influence cue-induced reward
responding and reward impulsivity.
Study Aims
A) Investigating the role of the dopamine system in cue-induced reward responding; B)
Investigating the role of the dopamine system in reward impulsivity; C) Investigating the
role of the opioid system in cue-induced reward responding; A) Investigating the role of the
opioid system in reward impulsivity.
Study Design
This is a double-blind, randomized, placebo-controlled, between-subject blocker study. 121
participants received either placebo, the dopamine D2/D3 receptor antagonist amisulpride
(400 mg), or the unselective opioid receptor antagonist naltrexone (50 mg), 3h before the
experimental tasks. Subjective effects on mood were assessed by visual analogue scales
(VAS). Cue-induced reward responding was measured using a standard Pavlovian-to-Instrumental
Transfer (PIT) task, where participants press a button for reward in the presence of a
stimulus predicting that reward. Reward impulsivity was measured using a Delay Discounting
(DD) Task, in which participants choose between smaller, immediate rewards and larger,
delayed rewards.
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Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator)
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