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Pharmacotherapeutic strategies for treating cocaine use disorder-what do we have to offer?治疗可卡因使用障碍的药物治疗策略——我们有什么可以提供的?
Addiction. 2021 Apr;116(4):694-710. doi: 10.1111/add.15242. Epub 2020 Sep 28.
2
Extended release mixed amphetamine salts and topiramate for cocaine dependence: A randomized clinical replication trial with frequent users.延胡索酸依他普仑和托吡酯联合治疗可卡因依赖:一项针对高频使用者的随机临床试验。
Drug Alcohol Depend. 2020 Jan 1;206:107700. doi: 10.1016/j.drugalcdep.2019.107700. Epub 2019 Nov 1.
3
The Neuroscience of Drug Reward and Addiction.药物奖赏和成瘾的神经科学。
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BMJ Open. 2019 Jun 21;9(6):e026604. doi: 10.1136/bmjopen-2018-026604.
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Study characteristics influence the efficacy of substance abuse treatments: A meta-analysis of medications for alcohol use disorder.研究特征会影响物质滥用治疗的效果:酒精使用障碍药物治疗的荟萃分析。
Drug Alcohol Depend. 2018 Sep 1;190:229-234. doi: 10.1016/j.drugalcdep.2018.06.015. Epub 2018 Jul 24.
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Distinct cognitive performance and patterns of drug use among early and late onset cocaine users.早发和晚发可卡因使用者在认知表现和用药模式上存在差异。
Addict Behav. 2017 Oct;73:41-47. doi: 10.1016/j.addbeh.2017.04.013. Epub 2017 Apr 29.
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Sustained-release dexamfetamine in the treatment of chronic cocaine-dependent patients on heroin-assisted treatment: a randomised, double-blind, placebo-controlled trial.在接受海洛因辅助治疗的慢性可卡因依赖患者中,持续释放型右旋苯丙胺治疗:一项随机、双盲、安慰剂对照试验。
Lancet. 2016 May 28;387(10034):2226-34. doi: 10.1016/S0140-6736(16)00205-1. Epub 2016 Mar 22.
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Antipsychotic medications for cocaine dependence.用于可卡因依赖的抗精神病药物。
Cochrane Database Syst Rev. 2016 Mar 19;3(3):CD006306. doi: 10.1002/14651858.CD006306.pub3.
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Susceptibility loci for heroin and cocaine addiction in the serotonergic and adrenergic pathways in populations of different ancestry.不同血统人群中血清素能和肾上腺素能途径中阿片类药物和可卡因成瘾的易感基因座。
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一项关于昂丹司琼治疗可卡因使用障碍的随机、双盲、安慰剂对照试验,事后进行了基于药理学的遗传分析。

A randomized, double-blind, placebo-controlled trial of ondansetron for the treatment of cocaine use disorder with post hoc pharmacogenetic analysis.

机构信息

Department of Psychiatry, Columbia University Irving Medical Center/New York State Psychiatric Institute, New York, NY, United States.

Department of Psychiatry, University of Maryland School of Medicine, Baltimore, MD 21201, United States.

出版信息

Drug Alcohol Depend. 2021 Nov 1;228:109074. doi: 10.1016/j.drugalcdep.2021.109074. Epub 2021 Sep 24.

DOI:10.1016/j.drugalcdep.2021.109074
PMID:34600264
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8595865/
Abstract

BACKGROUND

Cocaine use disorder (CUD) has significant consequences and there remain no FDA-approved pharmacotherapies. Ondansetron is an indirect dopaminergic modulator that has shown efficacy in alcohol use disorder, particularly in phenotypic and genotypic subgroups, and was found to be efficacious in a pilot dose-finding trial for CUD.

METHODS

One-hundred eight (108) adults with CUD were randomized to ondansetron 4 mg twice daily or placebo for 9 weeks and assessed up to thrice weekly to evaluate self-reported cocaine use and urine benzoylecgonine. Participants received cognitive-behavioral therapy and brief behavioral compliance enhancement therapy. Consenting participants (N = 79) provided blood samples for exploratory pharmacogenetic analyses.

RESULTS

Participants in both arms reduced cocaine use over time, but there was no statistically significant difference on percentage of cocaine-free days (PCFD; p = 0.972) or percentage of cocaine-free urine samples (PCFU; p = 0.909). Participants with early-onset CUD had greater improvement regardless of study arm (p = 0.002). Post hoc pharmacogenetic analyses demonstrated an interaction effect between treatment and rs1176713 SNP on PCFU in the total sample (p = 0.040) and African ancestry subset (p = 0.03). Constipation, fatigue, and somnolence were more common among ondansetron-treated participants (Fisher exact p < 0.05). Those who developed constipation were mostly rs1176713:GG carriers (Fisher exact p = 0.029).

CONCLUSIONS

Ondansetron did not demonstrate efficacy in the treatment of CUD. However, these preliminary results suggest a genotype-based variance in response to ondansetron in African ancestry individuals with CUD. Further studies are needed to validate findings for developing a personalized genomic approach for CUD treatment in racially and ethnically diverse populations.

摘要

背景

可卡因使用障碍(CUD)后果严重,目前仍没有获得 FDA 批准的药物治疗方法。昂丹司琼是一种间接的多巴胺调节剂,已被证明对酒精使用障碍有效,特别是在表型和基因型亚组中,并且在一项针对 CUD 的试点剂量发现试验中被证明是有效的。

方法

108 名患有 CUD 的成年人被随机分配到昂丹司琼 4mg 每日两次或安慰剂治疗 9 周,并每周评估 3 次,以评估自我报告的可卡因使用情况和尿液苯甲酰基古柯碱。参与者接受认知行为疗法和简短的行为依从性增强治疗。同意参加的参与者(N=79)提供血液样本进行探索性药物遗传学分析。

结果

两组参与者的可卡因使用量都随时间减少,但可卡因无使用天数百分比(PCFD;p=0.972)或可卡因无使用尿液样本百分比(PCFU;p=0.909)无统计学显著差异。无论研究臂如何,早期发病的 CUD 患者的改善程度更大(p=0.002)。事后药物遗传学分析表明,总样本(p=0.040)和非洲裔亚组(p=0.03)中 rs1176713 SNP 与治疗之间存在交互作用效应。昂丹司琼治疗组更常见便秘、疲劳和嗜睡(Fisher 精确检验 p<0.05)。出现便秘的患者大多是 rs1176713:GG 携带者(Fisher 精确检验 p=0.029)。

结论

昂丹司琼治疗 CUD 无效。然而,这些初步结果表明,在患有 CUD 的非洲裔个体中,基于基因型的对昂丹司琼反应存在差异。需要进一步的研究来验证这些发现,以便为治疗不同种族和民族的 CUD 患者制定个性化的基因组方法。