A phase 1 trial of pharmacologic interactions between transdermal selegiline and a 4-hour cocaine infusion.

Debra S Harris, Thomas Everhart, Peyton Jacob, Emil Lin, John E Mendelson, Reese T Jones
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引用次数: 7

Abstract

Background: The selective MAO-B inhibitor selegiline has been evaluated in clinical trials as a potential medication for the treatment of cocaine dependence. This study evaluated the safety of and pharmacologic interactions between 7 days of transdermal selegiline dosed with patches (Selegiline Transdermal System, STS) that deliver 6 mg/24 hours and 2.5 mg/kg of cocaine administered over 4 hours.

Methods: Twelve nondependent cocaine-experienced subjects received deuterium-labeled cocaine-d5 intravenously (IV) 0.5 mg/kg over 10 minutes followed by 2 mg/kg over 4 hours before and after one week of transdermal selegiline 6 mg/24 hours. Plasma and urine were collected for analysis of selegiline, cocaine, catecholamine and metabolite concentrations. Pharmacodynamic measures were obtained.

Results: Selegiline did not change cocaine pharmacokinetic parameters. Selegiline administration increased phenylethylamine (PEA) urinary excretion and decreased urinary MHPG-sulfate concentration after cocaine when compared to cocaine alone. No serious adverse effects occurred with the combination of selegiline and cocaine, and cocaine-induced physiological effects were unchanged after selegiline. Only 1 peak subjective cocaine effects rating changed, and only a few subjective ratings decreased across time after selegiline.

Conclusion: No pharmacological interaction occurred between selegiline and a substantial dose of intravenous cocaine, suggesting the combination will be safe in pharmacotherapy trials. Selegiline produced few changes in subjective response to the cocaine challenge perhaps because of some psychoactive neurotransmitters changing in opposite directions.

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经皮塞来吉兰与4小时可卡因输注之间药理学相互作用的一期试验。
这项研究评估了7天的经皮塞来吉兰贴剂(塞来吉兰透皮系统,STS)的安全性和药理学相互作用,贴剂每24小时给药6毫克,可卡因每公斤给药4小时2.5毫克。方法:12名非依赖可卡因的受试者,在经皮给药selegiline 6 mg/24小时之前和之后的一周,分别在10分钟内静脉注射氘标记的可卡因-d5 0.5 mg/kg,然后在4小时内给药2 mg/kg。收集血浆和尿液,分析斯来吉兰、可卡因、儿茶酚胺和代谢物浓度。获得药效学指标。结果:斯来吉兰对可卡因的药动学参数无影响。与单独服用可卡因相比,服用塞来吉兰增加了尿中苯乙胺(PEA)的排泄,降低了尿中mhpg -硫酸盐的浓度。塞来吉兰与可卡因合用未发生严重不良反应,服用塞来吉兰后,可卡因诱导的生理效应未发生变化。服用司来吉兰后,只有1个主观可卡因效应评分高峰发生了变化,只有少数主观评分随时间推移而下降。结论:塞来吉兰与大剂量静脉注射可卡因之间未发生药理相互作用,提示联合用药在药物治疗试验中是安全的。塞来吉兰对可卡因的主观反应几乎没有变化,这可能是因为一些精神活性神经递质在相反的方向上发生了变化。
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