首页> 外文期刊>Journal of Analytical Toxicology >Cocaine and metabolite concentrations in plasma during repeated oral administration: development of a human laboratory model of chronic cocaine use.
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Cocaine and metabolite concentrations in plasma during repeated oral administration: development of a human laboratory model of chronic cocaine use.

机译:重复口服期间血浆中可卡因和代谢物的浓度:长期使用可卡因的人类实验室模型的建立。

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Long-term use of cocaine may produce neurophysiological and metabolic alterations that differ from acute drug use. A laboratory model that was capable of evaluating the effects of chronic cocaine administration in human subjects was needed. Chronic oral administration of cocaine was considered a feasible route because of the ease of administration, control of dosing patterns, and possible reduction in medical risks compared with the intravenous and smoked routes. This clinical study was conducted to evaluate chronically administered oral cocaine as a means of studying cocaine addiction and withdrawal in humans. Cocaine-abusing volunteers were given multiple doses of oral cocaine each day in up to 16 daily sessions (including three placebo sessions). In each daily session, volunteers received five equal doses separated by hourly intervals. Across sessions, the dose was increased from an initial dose of 100 mg (500 mg/day) to 400 mg (2000 mg/day) in the last session. The dose for each consecutive cocaine session was increased by 25 mg/dose/session (125-mg total increase per session). Twelve subjects were enrolled in the study; however, three subjects dropped out prior to completion of at least three sessions. Two subjects completed all 13 cocaine sessions. The remaining seven subjects completed from 3 to 11 sessions; their participation was terminated early for safety and behavioral reasons. Plasma was collected during all sessions and analyzed for cocaine and metabolites by solid-phase extraction followed by gas chromatography-mass spectrometry. Oral cocaine administration resulted in peak plasma concentrations of cocaine approximately 1 h after administration. Accumulation of cocaine was evident between hourly doses and there was evidence of dose-proportional increases in area under the curve (AUC) measures across sessions. A variety of cocaine metabolites was measured in plasma including benzoylecgonine, ecgonine methyl ester, norcocaine, benzoylnorecgonine, and p and m-hydroxy metabolites of cocaine and benzoylecgonine. During chronic oral dosing, there appeared to be a trend for AUC ratios (AUCmetabolite/AUCcocaine) of benzoylecgonine and ecgonine methyl ester to decrease and norcocaine to increase, indicating the possibility of dose-, time-, or route-dependent changes in the absorption and/or metabolism of cocaine. Overall, this study demonstrated that chronic oral dosing of cocaine produced dose-related increases in plasma cocaine concentration, and this model could be useful for studying the effects of chronic cocaine use in human subjects.
机译:长期使用可卡因可能会产生与急性药物使用不同的神经生理和代谢改变。需要一种能够评估慢性可卡因对人类受试者的影响的实验室模型。与静脉内和烟熏途径相比,长期口服可卡因被认为是一种可行的途径,因为它易于管理,控制给药方式并可能降低医疗风险。进行该临床研究以评估长期施用的口服可卡因,作为研究人类可卡因成瘾和戒断的一种手段。每天在多达16个疗程中(包括3个安慰剂疗程)每天向滥用可卡因的志愿者服用多剂口服可卡因。在每一天的会议中,志愿者接受五次相等的剂量,每小时间隔一次。在整个疗程中,剂量从最初的100 mg(500 mg /天)增加到最后疗程的400 mg(2000 mg /天)。每个连续的可卡因疗程剂量增加25毫克/剂量/疗程(每次疗程总共增加125毫克)。该研究招募了12名受试者;但是,三个主题在至少完成三个会话之前就退出了。两名受试者完成了全部13次可卡因疗程。其余七个科目从3到11节完成;由于安全和行为原因,他们的参与被提前终止。在所有疗程中均收集血浆,并通过固相萃取然后气相色谱-质谱法分析可卡因和代谢产物。口服可卡因后约1小时可卡因血浆浓度达到峰值。每小时剂量之间可卡因的积累很明显,并且有证据表明整个疗程中曲线下面积(AUC)的剂量成比例增加。在血浆中测量了多种可卡因代谢物,包括苯甲酰基芽子碱,芽子碱甲酯,去甲可卡因,苯甲酰基正芽子碱以及可卡因和苯甲酰基芽子碱的对羟基和间羟基代谢产物。在长期口服给药过程中,苯甲酰芽子碱和芽子碱甲酯的AUC比率(AUCmetabolite / AUC可卡因)似乎有下降的趋势,而诺卡卡因有上升的趋势,这表明吸收的剂量,时间或途径依赖性变化的可能性和/或可卡因的新陈代谢。总的来说,这项研究表明,长期口服可卡因可导致血浆可卡因浓度的剂量相关增加,该模型可用于研究慢性可卡因对人类受试者的影响。

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