Blockade of Cue‐induced Brain Activation of Abstinent Alcoholics by a Single Administration of Amisulpride as Measured With fMRI

阿米必利 渴求 心理学 功能磁共振成像 神经科学 上瘾 精神科 氯氮平 精神分裂症(面向对象编程)
作者
Derik Hermann,Michael N. Smolka,Jana Wrase,Sabine Vollstädt‐Klein,J A. Nikitopoulos,Alexander Georgi,Dieter F. Braus,Herta Flor,Karl Mann,Andreas Heinz
出处
期刊:Alcoholism: Clinical and Experimental Research [Wiley]
卷期号:30 (8): 1349-1354 被引量:95
标识
DOI:10.1111/j.1530-0277.2006.00174.x
摘要

Background: Once alcohol dependence is established, alcohol‐associated cues may induce dopamine release in the reward system, which is accompanied by alcohol craving and may lead to relapse. In cocaine addicts, dopamine release in the thalamus was positively correlated with cocaine craving. We tested the effects of the atypical dopamine D 2/3 blocker amisulpride on cue‐induced brain activation in a functional magnetic resonance imaging (fMRI) paradigm. Methods: Alcohol‐associated and neutral pictures were presented in a block design to 10 male abstinent alcoholics (1–3 weeks after detoxification) and 10 healthy men during fMRI. The fMRI scans were acquired before and 2 hours after the oral application of 400 mg amisulpride. Before and after each scan, alcohol craving was measured with visual analogue scales. Results: Before the application of amisulpride, alcohol versus control cues elicited a higher blood oxygen level–dependent (BOLD) signal in the left frontal and orbitofrontal lobe, left cingulate gyrus, bilateral parietal lobe, and bilateral hippocampus in alcoholics compared with healthy controls. After amisulpride, alcoholics showed a reduced activation in the right thalamus compared with the first scan. Alcoholics no longer showed significant differences in their cue‐elicited BOLD response after amisulpride medication compared with medication‐free controls. Self‐reported craving was not affected by amisulpride medication. Conclusions: Amisulpride medication was associated with reduced cue‐induced activation of the thalamus, a brain region closely connected with frontostriatal circuits that regulate behavior and may influence relapse risk.
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