Literature DB >> 21809945

Triphasic mixture model of cell-mediated enzymatic degradation of hydrogels.

Franck J Vernerey1, Eric C Greenwald, Stephanie J Bryant.   

Abstract

One critical component of engineering living tissue equivalents is the design scaffolds (often made of hydrogels) whose degradation kinetics can match that of matrix production by cells. However, cell-mediated enzymatic degradation of a hydrogel is a highly complex and nonlinear process that is challenging to comprehend based solely on experimental observations. To address this issue, this study presents a triphasic mixture model of the enzyme-hydrogel system, which consists of a solid polymer network, water and enzyme. On the basis mixture theory, the rubber elasticity theory and the Michaelis-Menton kinetics for degradation, the model naturally incorporates a strong coupling between gel mechanical properties, the kinetics of degradation and the transport of enzyme through the gel. The model is then used to investigate the particular problem of a single spherical enzyme-producing cell, embedded in a spherical hydrogel domain, for which the governing equations can be cast within the cento-symmetric assumptions. The governing equations are subsequently solved using an implicit nonlinear finite element procedure to obtain the evolution of enzyme concentration and gel degradation through time and space. The model shows that two regimes of degradation behaviour exist, whereby degradation is dominated either by diffusion or dominated by reaction kinetics. Depending on the enzyme properties and the initial hydrogel design, the temporal and spatial changes in gel cross-linking are dramatically impacted, a feature that is likely to strongly affect new tissue development.

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Year:  2011        PMID: 21809945      PMCID: PMC3501263          DOI: 10.1080/10255842.2011.585973

Source DB:  PubMed          Journal:  Comput Methods Biomech Biomed Engin        ISSN: 1025-5842            Impact factor:   1.763


  24 in total

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  13 in total

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Review 3.  A mixture approach to investigate interstitial growth in engineering scaffolds.

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4.  Determination of the Polymer-Solvent Interaction Parameter for PEG Hydrogels in Water: Application of a Self Learning Algorithm.

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5.  * Understanding the Spatiotemporal Degradation Behavior of Aggrecanase-Sensitive Poly(ethylene glycol) Hydrogels for Use in Cartilage Tissue Engineering.

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6.  Dynamics of Stress Fibers Turnover in Contractile Cells.

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7.  On the role of hydrogel structure and degradation in controlling the transport of cell-secreted matrix molecules for engineered cartilage.

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8.  Tuning Reaction and Diffusion Mediated Degradation of Enzyme-Sensitive Hydrogels.

Authors:  Stacey C Skaalure; Umut Akalp; Franck J Vernerey; Stephanie J Bryant
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9.  An enzyme-sensitive PEG hydrogel based on aggrecan catabolism for cartilage tissue engineering.

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10.  Spatiotemporal neocartilage growth in matrix-metalloproteinase-sensitive poly(ethylene glycol) hydrogels under dynamic compressive loading: an experimental and computational approach.

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