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Safety and efficacy of varenicline to reduce positive subjective effects produced by methamphetamine in methamphetamine-dependent volunteers

机译:伐尼克兰减少依赖甲基苯丙胺的志愿者体内甲基苯丙胺产生的积极主观作用的安全性和有效性

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Methamphetamine use is increasing in the US. Although there are no Food and Drug Administration (FDA)-approved medications for methamphetamine dependence, preclinical and clinical studies suggest that methamphetamine users may benefit from treatments that enhance cholinergic neurotransmission. Consequently, we determined the safety and the efficacy of varenicline treatment, a partial agonist at α4β2 and a full agonist at α7 nicotinic acetylcholine receptors, to reduce positive subjective effects produced by smoked methamphetamine. Additionally, the effects of treatment with varenicline on the cardiovascular and reinforcing effects of methamphetamine were determined. We conducted a double-blind, placebo-controlled, within-subjects trial of varenicline vs. placebo in methamphetamine-dependent volunteers who were not seeking treatment. Participants were randomly assigned to receive one dose of varenicline (0, 1, or 2 mg) po BID, titrated up to the target dose over days 1–7, during each of three separate inpatient phases. Safety measures included the frequency, duration, severity, and relatedness of adverse events reported. Positive subjective effects included ‘Any drug effect', ‘High', ‘Good effects', ‘Stimulated', and ‘Drug liking', which were rated by participants before and for 1 h after smoking methamphetamine (0, 10, and 30 mg). There were no serious adverse events and no differences in adverse events reported during the three phases. Varenicline (2 mg) significantly reduced ratings of ‘Any drug effect' and ‘Stimulated', as well as attenuated ratings of ‘High', ‘Drug liking', and ‘Good effects', produced by methamphetamine (30 mg). The ability of varenicline to attenuate the positive subjective effects of methamphetamine in the laboratory suggests that varenicline should continue to be explored as a treatment for methamphetamine dependence.
机译:在美国,甲基苯丙胺的使用正在增加。尽管没有获得美国食品药品监督管理局(FDA)批准的用于甲基苯丙胺依赖的药物,但临床前和临床研究表明,甲基苯丙胺使用者可能会从增强胆碱能神经传递的治疗中受益。因此,我们确定了伐尼克兰治疗(减少α4β2的部分激动剂和抑制α7烟碱乙酰胆碱受体的完全激动剂)的安全性和功效,以减少烟酸甲基苯丙胺产生的积极主观效果。另外,确定了伐尼克兰治疗对甲基苯丙胺的心血管和增强作用的作用。我们在不寻求治疗的甲基苯丙胺依赖性志愿者中进行了缬草胺与安慰剂的双盲,安慰剂对照,受试者内试验。在三个单独的住院阶段中的每一个阶段,参与者被随机分配接受一剂缬草酸(0、1或2 mg)口服BID,并在1至7天内逐步升高至目标剂量。安全措施包括报告的不良事件的发生频率,持续时间,严重性和相关性。积极的主观效果包括“任何药物效果”,“高”,“良好效果”,“刺激性”和“吸毒”,参与者在吸食甲基苯丙胺(0、10和30 mg)之前和之后1小时对其进行了评分)。在这三个阶段中,没有发生严重的不良事件,也没有不良事件的报道。缬氨酸(2 mg)大大降低了甲基苯丙胺(30 mg)产生的“任何药物作用”和“刺激”的评分,并减弱了“高”,“药物喜欢”和“良好效果”的评分。法伦尼克林在实验室中减轻甲基苯丙胺的积极主观作用的能力表明,应继续探索法尼克兰作为对甲基苯丙胺依赖性治疗的方法。

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