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A cholecystokinin B receptor antagonist and cocaine interaction, phase I study

机译:胆囊收缩素B受体拮抗剂与可卡因相互作用,I期研究

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Aims RPR 102681, a cholecystokinin‐B antagonist, increased dopamine (DA) release and reduced cocaine self‐administration in animals. This pilot study sought to assess the safety and pharmacokinetics (PK) of co‐administration of RPR 102681 and cocaine, and to confirm the DA release mechanism of RPR 102681. Methods Sixteen cocaine‐dependent participants were randomized to either placebo or RPR102681 at 3 ascending doses; cocaine was co‐administered at steady state of RPR 102681. [sup11/supC]raclopride positron emission tomography scans were conducted at baseline and at each RPR102681 dose. Results RPR 102681 was well tolerated, and safe to co‐administer with cocaine. RPR 102681 did not alter the PK of either cocaine or its metabolite benzoylecgonine and showed no intrinsic abuse liability. There was a trend toward reduction of cocaine craving scores. In contrast to animal studies, RPR 102681 significantly increased the binding potential of [sup11/supC]raclopride in the ventral striatum ( t test, P ?.001) and caudate nucleus ( t test, P ?.0001) in a small subset of patients, suggesting that it may reduce intrasynaptic striatal DA. Conclusion Overall, this pilot study suggests that RPR 102681 would be unlikely candidate, as an agonist medication for the treatment for cocaine addiction but worth investigating further for possible role in reducing craving.
机译:Aims RPR 102681是胆囊收缩素-B拮抗剂,旨在增加动物中的多巴胺(DA)释放并减少可卡因的自我给药。这项初步研究旨在评估RPR 102681和可卡因共同给药的安全性和药代动力学(PK),并确认RPR 102681的DA释放机制。方法将16例可卡因依赖性参与者在3升后随机分为安慰剂或RPR102681剂量可卡因在RPR 102681的稳定状态下共同给药。[ 11 C]雷氯必利正电子发射断层扫描在基线和每个RPR102681剂量下进行。结果RPR 102681具有良好的耐受性,可安全与可卡因共同使用。 RPR 102681并没有改变可卡因或其代谢产物苯甲酰芽子碱的PK,也没有表现出内在的滥用责任。有减少可卡因渴望分数的趋势。与动物研究相反,RPR 102681显着增加了[ 11 C]雷氯必利在腹侧纹状体(t检验,P

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