Drug recirculation model with multiple cycles occurring at unequal time intervals

Y. Plusquellec , G. Houin
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引用次数: 15

Abstract

A pharmacokinetic model for enterohepatic recycling has been developed to take into account multiple recirculations likely to occur at various times after intravenous or subcutaneous injection, after infusion, or after a single oral administration of a drug. The times when the gall bladder empties, the duration of infusion and the number of recirculations may be arbitrarily chosen (for simulations) or computed (for optimization) to express the concentration in the central compartment at any time. Without a new theoretical calculation, the area under the concentration curve may be obtained as a function of the model parameters. As an example, the model is applied to an experimental case of four recirculations after oral administration and to a new drug data fitting.

以不等时间间隔发生多周期的药物再循环模型
肠肝再循环的药代动力学模型已经建立,考虑到静脉或皮下注射后、输注后或单次口服药物后不同时间可能发生的多次再循环。胆囊排空次数、输注时间和循环次数可以任意选择(用于模拟)或计算(用于优化),以表示任何时候中央室的浓度。无需新的理论计算,浓度曲线下的面积可以作为模型参数的函数得到。作为一个例子,该模型应用于一个口服给药后四次再循环的实验案例和一个新药的数据拟合。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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