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    A Molecular Model of Proteoglycan-Associated Electrostatic Forces in Cartilage Mechanics

    Source: Journal of Biomechanical Engineering:;1995:;volume( 117 ):;issue: 002::page 179
    Author:
    M. D. Buschmann
    ,
    A. J. Grodzinsky
    DOI: 10.1115/1.2796000
    Publisher: The American Society of Mechanical Engineers (ASME)
    Abstract: Measured values of the swelling pressure of charged proteoglycans (PG) in solution (Williams RPW, and Comper WD; Biophysical Chemistry 36:223, 1990) and the ionic strength dependence of the equilibrium modulus of PG-rich articular cartilage (Eisenberg SR, and Grodzinsky AJ; J Orthop Res 3: 148, 1985) are compared to the predictions of two models. Each model is a representation of electrostatic forces arising from charge present on spatially fixed macromolecules and spatially mobile micro-ions. The first is a macroscopic continuum model based on Donnan equilibrium that includes no molecular-level structure and assumes that the electrical potential is spatially invariant within the polyelectrolyte medium (i.e. zero electric field). The second model is based on a microstructural, molecular-level solution of the Poisson-Boltzmann (PB) equation within a unit cell containing a charged glycosaminoglycan (GAG) molecule and its surrounding atmosphere of mobile ions. This latter approach accounts for the space-varying electrical potential and electrical field between the GAG constituents of the PG. In computations involving no adjustable parameters, the PB-cell model agrees with the measured pressure of PG solutions to within experimental error (10%), whereas the ideal Donnan model overestimates the pressure by up to 3-fold. In computations involving one adjustable parameter for each model, the PB-cell model predicts the ionic strength dependence of the equilibrium modulus of articular cartilage. Near physiological ionic strength, the Donnan model overpredicts the modulus data by 2-fold, but the two models coincide for low ionic strengths (C0 < 0.025M) where the spatially invariant Donnan potential is a closer approximation to the PB potential distribution. The PB-cell model result indicates that electrostatic forces between adjacent GAGs predominate in determining the swelling pressure of PG in the concentration range found in articular cartilage (20–80 mg/ml). The PB-cell model is also consistent with data (Eisenberg and Grodzinsky, 1985, Lai WM, Hou JS, and Mow VC; J Biomech Eng 113: 245, 1991) showing that these electrostatic forces account for ̃ 1/2 (290kPa) the equilibrium modulus of cartilage at physiological ionic strength while absolute swelling pressures may be as low as ̃ 25 – 100kPa. This important property of electrostatic repulsion between GAGs that are highly charged but spaced a few Debye lengths apart allows cartilage to resist compression (high modulus) without generating excessive intratissue swelling pressures.
    keyword(s): Force , Cartilage , Pressure , Equilibrium (Physics) , Electric fields , Electric potential , Ions , Physiology , Computation , Equations , Errors , Macromolecules , Approximation , Chemistry AND Compression ,
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      A Molecular Model of Proteoglycan-Associated Electrostatic Forces in Cartilage Mechanics

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    http://yetl.yabesh.ir/yetl1/handle/yetl/114995
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    • Journal of Biomechanical Engineering

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    contributor authorM. D. Buschmann
    contributor authorA. J. Grodzinsky
    date accessioned2017-05-08T23:46:39Z
    date available2017-05-08T23:46:39Z
    date copyrightMay, 1995
    date issued1995
    identifier issn0148-0731
    identifier otherJBENDY-25952#179_1.pdf
    identifier urihttp://yetl.yabesh.ir/yetl/handle/yetl/114995
    description abstractMeasured values of the swelling pressure of charged proteoglycans (PG) in solution (Williams RPW, and Comper WD; Biophysical Chemistry 36:223, 1990) and the ionic strength dependence of the equilibrium modulus of PG-rich articular cartilage (Eisenberg SR, and Grodzinsky AJ; J Orthop Res 3: 148, 1985) are compared to the predictions of two models. Each model is a representation of electrostatic forces arising from charge present on spatially fixed macromolecules and spatially mobile micro-ions. The first is a macroscopic continuum model based on Donnan equilibrium that includes no molecular-level structure and assumes that the electrical potential is spatially invariant within the polyelectrolyte medium (i.e. zero electric field). The second model is based on a microstructural, molecular-level solution of the Poisson-Boltzmann (PB) equation within a unit cell containing a charged glycosaminoglycan (GAG) molecule and its surrounding atmosphere of mobile ions. This latter approach accounts for the space-varying electrical potential and electrical field between the GAG constituents of the PG. In computations involving no adjustable parameters, the PB-cell model agrees with the measured pressure of PG solutions to within experimental error (10%), whereas the ideal Donnan model overestimates the pressure by up to 3-fold. In computations involving one adjustable parameter for each model, the PB-cell model predicts the ionic strength dependence of the equilibrium modulus of articular cartilage. Near physiological ionic strength, the Donnan model overpredicts the modulus data by 2-fold, but the two models coincide for low ionic strengths (C0 < 0.025M) where the spatially invariant Donnan potential is a closer approximation to the PB potential distribution. The PB-cell model result indicates that electrostatic forces between adjacent GAGs predominate in determining the swelling pressure of PG in the concentration range found in articular cartilage (20–80 mg/ml). The PB-cell model is also consistent with data (Eisenberg and Grodzinsky, 1985, Lai WM, Hou JS, and Mow VC; J Biomech Eng 113: 245, 1991) showing that these electrostatic forces account for ̃ 1/2 (290kPa) the equilibrium modulus of cartilage at physiological ionic strength while absolute swelling pressures may be as low as ̃ 25 – 100kPa. This important property of electrostatic repulsion between GAGs that are highly charged but spaced a few Debye lengths apart allows cartilage to resist compression (high modulus) without generating excessive intratissue swelling pressures.
    publisherThe American Society of Mechanical Engineers (ASME)
    titleA Molecular Model of Proteoglycan-Associated Electrostatic Forces in Cartilage Mechanics
    typeJournal Paper
    journal volume117
    journal issue2
    journal titleJournal of Biomechanical Engineering
    identifier doi10.1115/1.2796000
    journal fristpage179
    journal lastpage192
    identifier eissn1528-8951
    keywordsForce
    keywordsCartilage
    keywordsPressure
    keywordsEquilibrium (Physics)
    keywordsElectric fields
    keywordsElectric potential
    keywordsIons
    keywordsPhysiology
    keywordsComputation
    keywordsEquations
    keywordsErrors
    keywordsMacromolecules
    keywordsApproximation
    keywordsChemistry AND Compression
    treeJournal of Biomechanical Engineering:;1995:;volume( 117 ):;issue: 002
    contenttypeFulltext
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