用非指数组织俘获解释胺碘酮的异常药代动力学。

M Weiss
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引用次数: 50

摘要

传统的药代动力学(PK)概念无法描述极阳离子两亲性药物胺碘酮的长期药代动力学。提出了一种基于组织结合位点捕获现象的非经典模型,该模型具有很长的释放时间,这意味着不能定义分布的体积和稳态水平。与文献中可用的临床PK数据一致,该模型不仅可以很好地描述单剂量处置曲线,还可以描述长期治疗(长达5年)期间持续增加的血药浓度-时间曲线以及停止治疗后的洗脱曲线。新颖的方面是将长尾组织停留时间分布纳入循环模型,使初始分布过程和间隙概念保持不变。在物理科学中被称为“奇怪或异常”动力学的基本理论方法和模型的分形标度特性可能会增强我们对极疏水性异种生物的PK的理解。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The anomalous pharmacokinetics of amiodarone explained by nonexponential tissue trapping.

Conventional pharmacokinetic (PK) concepts fail to describe the long-term pharmacokinetics of the extremely cationic amphiphilic drug amiodarone. A nonclassical model based on the phenomenon of trapping at tissue binding sites with very long release times is presented, which implies that a volume of distribution and a steady-state level cannot be defined. In agreement with clinical PK data available in the literature, the model well describes not only single-dose disposition curves but also the persistently increasing plasma concentration-time curve during long-term treatment (up to 5 years) and the washout curve following cessation of therapy. The novel aspect is a long-tailed tissue residence time distribution which is incorporated into a recirculatory model leaving the initial distribution process and the clearance concept unchanged. The underlying theoretical approach, which is known as "strange or anomalous" kinetics in physical sciences, and the fractal scaling property of the model may enhance our understanding of the PK of extremely hydrophobic xenobiotics.

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