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首页> 外文期刊>British journal of clinical pharmacology >Pharmacokinetic–pharmacodynamic relationships of central nervous system effects of scopolamine in healthy subjects
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Pharmacokinetic–pharmacodynamic relationships of central nervous system effects of scopolamine in healthy subjects

机译:东pol碱对健康受试者中枢神经系统作用的药代动力学与药效关系

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WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT? The cholinergic system is important for different central nervous system functions, including memory, learning and attention. Scopolamine, a centrally active muscarinic antagonist, has been used to model dementia and to demonstrate the pharmacological effects of cholinergic drugs, but for most effects the concentration–effect relationships are unknown.WHAT THIS STUDY ADDS? We determined the pharmacokinetic–pharmacodynamic relationships of scopolamine using a multidimensional central nervous system test battery in a large group of healthy volunteers. The results suggested there are various functional cholinergic systems with different pharmacological characteristics, which can be used to study the effects of drugs that directly or indirectly modify cholinergic systems. The design of such studies should take the different concentration–effect relationships into account.AIM(S) Although scopolamine is a frequently used memory impairment model, the relationships between exposure and corresponding central nervous system (CNS) effects are mostly unknown. The aim of our study was to characterize these using pharmacokinetic–pharmacodynamic (PK–PD) modelling.METHODS In two double-blind, placebo-controlled, four-way crossover studies, 0.5-mg scopolamine was administered i.v. to 90 healthy male subjects. PK and PD/safety measures were monitored pre-dose and up to 8.5 h after administration. PK–PD relationships were modelled using non-linear mixed-effect modelling.RESULTS Most PD responses following scopolamine administration in 85 subjects differed significantly from placebo. As PD measures lagged behind the plasma PK profile, PK–PD relationships were modelled using an effect compartment and arbitrarily categorized according to their equilibration half-lives (t1/2keo; hysteresis measure). t1/2keo for heart rate was 17 min, saccadic eye movements and adaptive tracking 1–1.5 h, body sway, smooth pursuit, visual analogue scales alertness and psychedelic 2.5–3.5 h, pupil size, finger tapping and visual analogue scales feeling high more than 8 h.CONCLUSIONS Scopolamine affected different CNS functions in a concentration-dependent manner, which based on their distinct PK–PD characteristics seemed to reflect multiple distinct functional pathways of the cholinergic system. All PD effects showed considerable albeit variable delays compared with plasma concentrations. The t1/2keo of the central effects was longer than of the peripheral effects on heart rate, which at least partly reflects the long CNS retention of scopolamine, but possibly also the triggering of independent secondary mechanisms. PK–PD analysis can optimize scopolamine administration regimens for future research and give insight into the physiology and pharmacology of human cholinergic systems.
机译:此主题已经知道什么?胆碱能系统对于不同的中枢神经系统功能(包括记忆,学习和注意力)很重要。 Scopolamine是一种中枢活性毒蕈碱拮抗剂,已被用于模拟痴呆症并证明胆碱能药物的药理作用,但对于大多数作用,浓度-作用关系尚不清楚。我们使用多维中枢神经系统测试电池在一大批健康志愿者中确定了东pol碱的药代动力学与药效关系。结果表明存在各种具有不同药理特性的功能性胆碱能系统,可用于研究直接或间接修饰胆碱能系统的药物的作用。这类研究的设计应考虑不同的浓度-效应关系。AIM(S)尽管东pol碱是一种经常使用的记忆障碍模型,但暴露与相应的中枢神经系统(CNS)效应之间的关系尚不清楚。我们的研究目的是使用药代动力学-药效学(PK-PD)模型对这些特征进行表征。方法在两项双盲,安慰剂对照,四向交叉研究中,静脉内给予0.5 mg东碱。 90名健康男性受试者。给药前和给药后长达8.5 h监测PK和PD /安全性措施。使用非线性混合效应模型对PK-PD关系进行建模。结果东85碱给药后85名受试者的大多数PD反应与安慰剂有显着差异。由于PD测量值落后于血浆PK曲线,因此使用效应区对PK-PD关系进行建模,并根据其平衡半衰期(t 1/2 k eo ;磁滞量)。 t 1/2 k eo 的心律为17分钟,眼跳运动和适应性跟踪为1–1.5小时,身体摇摆,平稳追逐,视觉模拟量表警觉性和迷幻感2.5-3.5小时,瞳孔大小,手指敲击和视觉模拟量表感觉超过8小时。结论东co碱以浓度依赖的方式影响不同的中枢神经系统功能,这基于其独特的PK-PD特性似乎反映了多种不同的功能途径胆碱能系统。与血浆浓度相比,所有的PD效应均显示出可观的变化,尽管延迟有所变化。 t 1/2 k eo 对心率的中枢效应比周围效应长,这至少部分反映了东pol碱对CNS的长期保留,但可能也触发了独立的辅助机制。 PK-PD分析可以优化东pol碱的给药方案,以备将来研究之用,并有助于深入了解人类胆碱能系统的生理学和药理学。

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