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Olanzapine Reduces Craving for Alcohol: A DRD4 VNTR Polymorphism by Pharmacotherapy Interaction

机译:奥氮平减少对酒精的渴望:通过药物疗法相互作用的DRD4 VNTR多态性

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Separate investigations have suggested that olanzapine, a D4 antagonist, decreases craving after a priming dose of alcohol and that the DRD4 variable number of tandem repeats (VNTR) polymorphism influences the expression of craving after a priming dose of alcohol. The present study tested the hypothesis that olanzapine may be differentially effective at reducing cue-elicited craving based on individual differences in DRD4 VNTR in a sample of heavy social drinkers. Participants were randomly assigned to receive olanzapine (5mg) or a control medication (cyproheptadine, 4mg) prior to consuming three alcoholic drinks. Participants completed subjective measures of craving and euphoria after each drink. Participants who were homozygous or heterozygous for the 7 (or longer) repeat allele of the DRD4 VNTR were classified as DRD4 L, while the other participants were classified as DRD4 S. The findings indicated that olanzapine reduces craving for alcohol at baseline for both DRD4 S and DRD4 L individuals, but only reduces craving after exposure to alcohol cues and after a priming dose of alcohol for DRD4 L individuals.
机译:单独的研究表明,D4拮抗剂奥氮平可在启动剂量的酒精后减少对食物的渴望,而DRD4可变数目的串联重复序列(VNTR)多态性会影响启动剂量的酒精后对渴望的表达。本研究检验了以下假设:根据重度社会饮酒者样本中DRD4 VNTR的个体差异,奥氮平在减少提示引起的渴望方面可能有不同的效果。参加者在饮用三种酒精饮料之前被随机分配接受奥氮平(5mg)或对照药物(赛庚啶,4mg)。参与者在每次喝酒后完成了对渴望和欣快的主观测量。对DRD4 VNTR的7个(或更长时间)重复等位基因纯合或杂合的参与者被分类为DRD4 L,而其他参与者被分类为DRD4S。研究结果表明,奥氮平降低了DRD4 S基线时对酒精的渴望。和DRD4 L个人,但只能减少DRD4 L个人暴露于酒精提示后和初次服用酒精后的渴望。

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