Combined Experimental Approach and Finite Element Modeling of Small Molecule Transport Through Joint Synovium to Measure Effective DiffusivitySource: Journal of Biomechanical Engineering:;2020:;volume( 142 ):;issue: 004::page 041010-1Author:Guang, Young
,
McGrath, Tom M.
,
Klug, Natalie R.
,
Nims, Robert J.
,
Shih, Chien-Cheng
,
Bayguinov, Peter O.
,
Guilak, Farshid
,
Pham, Christine T. N.
,
Fitzpatrick, James A. J.
,
Setton, Lori A.
DOI: 10.1115/1.4044892Publisher: The American Society of Mechanical Engineers (ASME)
Abstract: Trans-synovial solute transport plays a critical role in the clearance of intra-articularly (IA) delivered drugs. In this study, we present a computational finite element model (FEM) of solute transport through the synovium validated by experiments on synovial explants. Unsteady diffusion of urea, a small uncharged molecule, was measured through devitalized porcine and human synovium using custom-built diffusion chambers. A multiphasic computational model was constructed and optimized with the experimental data to extract effective diffusivity for urea within the synovium. A monotonic decrease in urea concentration was observed in the donor bath over time, with an effective diffusivity found to be an order of magnitude lower in synovium versus that measured in free solution. Parametric studies incorporating an intimal cell layer with varying thickness and varying effective diffusivities were performed, revealing a dependence of drug clearance kinetics on both parameters. The findings of this study indicate that the synovial matrix impedes urea solute transport out of the joint with little retention of the solute in the matrix.
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contributor author | Guang, Young | |
contributor author | McGrath, Tom M. | |
contributor author | Klug, Natalie R. | |
contributor author | Nims, Robert J. | |
contributor author | Shih, Chien-Cheng | |
contributor author | Bayguinov, Peter O. | |
contributor author | Guilak, Farshid | |
contributor author | Pham, Christine T. N. | |
contributor author | Fitzpatrick, James A. J. | |
contributor author | Setton, Lori A. | |
date accessioned | 2022-02-04T23:03:50Z | |
date available | 2022-02-04T23:03:50Z | |
date copyright | 4/1/2020 12:00:00 AM | |
date issued | 2020 | |
identifier issn | 0148-0731 | |
identifier other | bio_142_04_041010.pdf | |
identifier uri | http://yetl.yabesh.ir/yetl1/handle/yetl/4276021 | |
description abstract | Trans-synovial solute transport plays a critical role in the clearance of intra-articularly (IA) delivered drugs. In this study, we present a computational finite element model (FEM) of solute transport through the synovium validated by experiments on synovial explants. Unsteady diffusion of urea, a small uncharged molecule, was measured through devitalized porcine and human synovium using custom-built diffusion chambers. A multiphasic computational model was constructed and optimized with the experimental data to extract effective diffusivity for urea within the synovium. A monotonic decrease in urea concentration was observed in the donor bath over time, with an effective diffusivity found to be an order of magnitude lower in synovium versus that measured in free solution. Parametric studies incorporating an intimal cell layer with varying thickness and varying effective diffusivities were performed, revealing a dependence of drug clearance kinetics on both parameters. The findings of this study indicate that the synovial matrix impedes urea solute transport out of the joint with little retention of the solute in the matrix. | |
publisher | The American Society of Mechanical Engineers (ASME) | |
title | Combined Experimental Approach and Finite Element Modeling of Small Molecule Transport Through Joint Synovium to Measure Effective Diffusivity | |
type | Journal Paper | |
journal volume | 142 | |
journal issue | 4 | |
journal title | Journal of Biomechanical Engineering | |
identifier doi | 10.1115/1.4044892 | |
journal fristpage | 041010-1 | |
journal lastpage | 041010-8 | |
page | 8 | |
tree | Journal of Biomechanical Engineering:;2020:;volume( 142 ):;issue: 004 | |
contenttype | Fulltext |