Jee E. Rim scite author profile

The finite element method is employed to simulate two-dimensional (axisymmetric) drug diffusion from a finite drug reservoir into the skin. The numerical formulation is based on a general mathematical model for multicomponent nonlinear diffusion that takes into account the coupling effects between the different components. The presence of several diffusing components is crucial, as many transdermal drug delivery formulations contain one or more permeation enhancers in addition to the drug. The coupling between the drug and permeation enhancer(s) results in nonlinear diffusion with concentration-dependent diffusivities of the various components. The framework is suitable for modeling both linear and nonlinear, single- and multicomponent diffusions, however, as it reduces to the correct formulation simply by setting the relevant parameters to zero. In addition, we show that partitioning of the penetrants from the reservoir into the skin can be treated in a straightforward manner in this framework using the mixed method. Partitioning at interface boundaries poses some difficulty with the standard finite element method as it creates a discontinuity in the concentration variable at the interface. To our knowledge, nonlinear (concentration-dependent) partitioning in diffusion problems has not been treated numerically before, and we demonstrate that nonlinear partitioning may have an important role in the effect of permeation enhancers. The mixed method that we adopt includes the flux at the interface explicitly in the formulation, allowing the modeling of concentration-dependent partitioning of the permeants between the reservoir and the skin as well as constant (linear) partitioning. The result is a versatile finite element framework suitable for modeling both linear and nonlinear diffusions in heterogeneous media where the diffusivities and partition coefficients may vary in each subregion.

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Multiscale Modeling Framework of Transdermal Drug Delivery

Rim

Pinsky

Osdol

2009

Ann Biomed Eng

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Abstract-This study addresses the modeling of transdermal diffusion of drugs to better understand the permeation of molecules through the skin, especially the stratum corneum, which forms the main permeation barrier to percutaneous permeation. In order to ensure reproducibility and predictability of drug permeation through the skin and into the body, a quantitative understanding of the permeation barrier properties of the stratum corneum (SC) is crucial. We propose a multiscale framework of modeling the multicomponent transdermal diffusion of molecules. The problem is divided into subproblems of increasing length scale: microscopic, mesoscopic, and macroscopic. First, the microscopic diffusion coefficient in the lipid bilayers of the SC is found through molecular dynamics (MD) simulations. Then, a homogenization procedure is performed over a model unit cell of the heterogeneous SC, resulting in effective diffusion parameters. These effective parameters are the macroscopic diffusion coefficients for the homogeneous medium that is ''equivalent'' to the heterogeneous SC, and thus can be used in finite element simulations of the macroscopic diffusion process. The resulting drug flux through the skin shows very reasonable agreement to experimental data.

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Jee E. Rim

Merger of structure and material in nacre and bone – Perspectives on de novo biomimetic materials

Finite Element Modeling of Coupled Diffusion with Partitioning in Transdermal Drug Delivery

Multiscale Modeling Framework of Transdermal Drug Delivery

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