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Application of the Convection–Dispersion Equation to Modelling Oral Drug Absorption

机译:对流扩散方程在口服药物吸收模型中的应用

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摘要

Models of systemic drug absorption after oral administration are frequently based on a direct or a delayed first-order rate process. In practice, the use of the first-order approach to predict drug concentrations in blood plasma frequently yields a considerable mismatch between predicted and measured concentration profiles. This is particularly true for the upswing of the plasma concentration after oral administration. The current investigation explores an alternative model to describe the absorption rate based on the convection–dispersion equation describing the transport of chemicals through the GI tract. This equation is governed by two parameters, transport velocity and dispersion coefficient. One solution of this equation for a specific set of initial and boundary conditions was used to model absorption of paracetamol in a 22-year-old man after oral administration. The GI-tract passage rate in this subject was influenced by co-administration of drugs that stimulate or delay gastric emptying. The transport-limited absorption function is more accurate in describing the plasma concentration versus time curve after oral administration than the first-order model. Additionally, it provides a mechanistic explanation for the observed curve through the differences in GI-tract passage rate.
机译:口服后全身药物吸收的模型通常基于直接或延迟的一级速率过程。在实践中,使用一阶方法预测血浆中的药物浓度经常会在预测浓度曲线和测量浓度曲线之间产生相当大的失配。对于口服给药后血浆浓度的上升尤其如此。当前的研究探索了一种替代模型,该模型基于对流扩散方程来描述吸收速率,该对流扩散方程描述了化学物质通过胃肠道的传输。该方程由两个参数控制,即传输速度和分散系数。对于一组特定的初始和边界条件,该方程的一个解用于模拟口服后22岁男性对乙酰氨基酚的吸收。该受试者的胃肠道通过率受刺激或延迟胃排空药物的共同给药影响。在描述口服给药后血浆浓度与时间的关系曲线时,与一阶模型相比,转运受限的吸收函数更准确。此外,它通过胃肠道通过率的差异为观察到的曲线提供了机械解释。

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