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D-环丝氨酸增强线索诱发的酒精渴望消退:一种转化医学方法。

D-cycloserine to enhance extinction of cue-elicited craving for alcohol: a translational approach.

作者信息

MacKillop J, Few L R, Stojek M K, Murphy C M, Malutinok S F, Johnson F T, Hofmann S G, McGeary J E, Swift R M, Monti P M

机构信息

1] Peter Boris Centre for Addictions Research, Department of Psychiatry and Behavioural Neurosciences, McMaster University/St. Joseph's Healthcare Hamilton, Hamilton, ON, Canada [2] Homewood Research Institute, Homewood Health Centre, Guelph, ON, Canada [3] Center for Alcohol and Addiction Studies, Brown University, Providence, RI, USA.

Department of Psychiatry, Washington University, St. Louis, MO, USA.

出版信息

Transl Psychiatry. 2015 Apr 7;5(4):e544. doi: 10.1038/tp.2015.41.

Abstract

Cue-elicited craving for alcohol is well established but extinction-based treatment to extinguish this response has generated only modest positive outcomes in clinical trials. Basic and clinical research suggests that D-cycloserine (DCS) enhances extinction to fear cues under certain conditions. However, it remains unclear whether DCS would also accelerate extinction of cue-elicited craving for alcohol. The goal of the current study was to examine whether, compared with placebo (PBO), DCS enhanced extinction of cue-elicited craving among treatment-seeking individuals with alcohol use disorders (AUDs). Participants were administered DCS (50 mg) or PBO 1 h before an alcohol extinction paradigm in a simulated bar environment on two occasions. The extinction procedures occurred 1 week apart and were fully integrated into outpatient treatment. Subjective craving for alcohol was the primary variable of interest. Follow-up cue reactivity sessions were conducted 1 week and 3 weeks later to ascertain persisting DCS effects. Drinking outcomes and tolerability were also examined. DCS was associated with augmented reductions in alcohol craving to alcohol cues during the first extinction session and these effects persisted through all subsequent sessions, suggesting facilitation of extinction. Participants in the DCS condition reported significant short-term reductions in drinking, although these did not persist to follow-up, and found the medication highly tolerable. These findings provide evidence that DCS enhances extinction of cue-elicited craving for alcohol in individuals with AUDs in the context of outpatient treatment. The potential clinical utility of DCS is discussed, including methodological considerations and context-dependent learning.

摘要

线索诱发的酒精渴望已得到充分证实,但基于消退的治疗方法来消除这种反应在临床试验中仅产生了适度的积极效果。基础和临床研究表明,D-环丝氨酸(DCS)在某些条件下可增强对恐惧线索的消退。然而,尚不清楚DCS是否也会加速线索诱发的酒精渴望的消退。本研究的目的是检验与安慰剂(PBO)相比,DCS是否能增强酒精使用障碍(AUDs)寻求治疗个体中线索诱发渴望的消退。参与者在模拟酒吧环境中的酒精消退范式前1小时接受DCS(50毫克)或PBO,共进行两次。消退程序相隔1周进行,并完全纳入门诊治疗。对酒精的主观渴望是主要的研究变量。在1周和3周后进行随访线索反应性 sessions,以确定DCS的持续效果。还检查了饮酒结果和耐受性。DCS与第一次消退 session 期间对酒精线索的酒精渴望的更大程度降低相关,并且这些效果在所有后续 session 中持续存在,表明促进了消退。DCS组的参与者报告饮酒量有显著短期减少,尽管这些减少在随访时没有持续,并且发现该药物耐受性良好。这些发现提供了证据,表明在门诊治疗背景下,DCS可增强AUDs个体中线索诱发的酒精渴望的消退。讨论了DCS的潜在临床效用,包括方法学考虑和情境依赖性学习。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9f83/4462604/95830a8eeb5d/tp201541f1.jpg

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