Mathematical models in percutaneous absorption

M. Roberts, Y. Anissimov, Richard A. Gonsalvez
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引用次数: 24

Abstract

A number of mathematical models have been used to describe percutaneous absorption kinetics. In general, most of these models have used either diffusion-based or compartmental equations. The object of any mathematical model is to a) be able to represent the processes associated with absorption accurately, b) be able to describe/summarize experimental data with parametric equations or moments, and c) predict kinetics under varying conditions. However, in describing the processes involved, some developed models often suffer from being of too complex a form to be practically useful. In this chapter, we attempt to approach the issue of mathematical modeling in percutaneous absorption from four perspectives. These are to a) describe simple practical models, b) provide an overview of the more complex models, c) summarize some of the more important/useful models used to date, and d) examine sonic practical applications of the models. The range of processes involved in percutaneous absorption and considered in developing the mathematical models in this chapter is shown in Fig. 1. We initially address in vitro skin diffusion models and consider a) constant donor concentration and receptor conditions, b) the corresponding flux, donor, skin, and receptor amount-time profiles for solutions, and c) amount- and flux-time profiles when the donor phase is removed. More complex issues, such as finite-volume donor phase, finite-volume receptor phase, the presence of an efflux. rate constant at the membrane-receptor interphase, and two-layer diffusion, are then considered. We then look at specific models and issues concerned with a) release from topical products, b) use of compartmental models as alternatives to diffusion models, c) concentration-dependent absorption, d) modeling of skin metabolism, e) role of solute-skin-vehicle interactions, f) effects of vehicle loss, a) shunt transport, and h) in vivo diffusion, compartmental, physiological, and deconvolution models. We conclude by examining topics such as a) deep tissue penetration, b) pharmacodynamics, c) iontophoresis, d) sonophoresis, and e) pitfalls in modeling.
经皮吸收的数学模型
许多数学模型已被用来描述经皮吸收动力学。一般来说,大多数这些模型要么使用基于扩散的方程,要么使用隔室方程。任何数学模型的目标都是a)能够准确地表示与吸收相关的过程,b)能够用参数方程或矩描述/总结实验数据,c)预测不同条件下的动力学。然而,在描述所涉及的过程时,一些开发的模型常常因为形式过于复杂而无法实际使用。在本章中,我们试图从四个角度探讨经皮吸收的数学建模问题。这些是a)描述简单的实用模型,b)提供更复杂模型的概述,c)总结一些迄今为止使用的更重要/有用的模型,d)检查这些模型的声学实际应用。图1显示了经皮吸收过程的范围,并在本章中建立了数学模型。我们首先解决了体外皮肤扩散模型,并考虑了a)恒定的供体浓度和受体条件,b)溶液的相应通量、供体、皮肤和受体的量-时间曲线,以及c)去除供体相时的量-时间曲线。更复杂的问题,如有限体积供体期,有限体积受体期,外排的存在。然后考虑膜-受体间期的速率常数和两层扩散。然后,我们研究了与以下方面相关的具体模型和问题:a)局部产品的释放,b)使用室室模型作为扩散模型的替代品,c)浓度依赖性吸收,d)皮肤代谢模型,e)溶质-皮肤-媒介相互作用的作用,f)媒介损失的影响,a)分流运输,以及h)体内扩散,室室,生理和反卷积模型。我们通过检查主题来总结,如a)深层组织渗透,b)药效学,c)离子导入,d)声导入,e)建模中的陷阱。
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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