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    Numerical Model of Fluid Flow and Oxygen Transport in a Radial-Flow Microchannel Containing Hepatocytes

    Source: Journal of Biomechanical Engineering:;1999:;volume( 121 ):;issue: 001::page 58
    Author:
    G. A. Ledezma
    ,
    A. Folch
    ,
    S. N. Bhatia
    ,
    U. J. Balis
    ,
    M. L. Yarmush
    ,
    M. Toner
    DOI: 10.1115/1.2798043
    Publisher: The American Society of Mechanical Engineers (ASME)
    Abstract: The incorporation of monolayers of cultured hepatocytes into an extracorporeal perfusion system has become a promising approach for the development of a temporary bioartificial liver (BAL) support system. In this paper we present a numerical investigation of the oxygen tension, shear stress, and pressure drop in a bioreactor for a BAL composed of plasma-perfused chambers containing monolayers of porcine hepatocytes. The chambers consist of microfabricated parallel disks with center-to-edge radial flow. The oxygen uptake rate (OUR), measured in vitro for porcine hepatocytes, was curve-fitted using Michaelis–Menten kinetics for simulation of the oxygen concentration profile. The effect of different parameters that may influence the oxygen transport inside the chambers, such as the plasma flow rate, the chamber height, the initial oxygen tension in the perfused plasma, the OUR, and Km was investigated. We found that both the plasma flow rate and the initial oxygen tension may have an important effect upon oxygen transport. Increasing the flow rate and/or the inlet oxygen tension resulted in improved oxygen transport to cells in the radial-flow microchannels, and allowed significantly greater diameter reactor without oxygen limitation to the hepatocytes. In the range investigated in this paper (10 μm < H < 100 μm), and for a constant plasma flow rate, the chamber height, H, had a negligible effect on the oxygen transport to hepatocytes. On the contrary, it strongly affected the mechanical stress on the cells that is also crucial for the successful design of the BAL reactors. A twofold decrease in chamber height from 50 to 25 μm produced approximately a fivefold increase in maximal shear stress at the inlet of the reactor from 2 to 10 dyn/cm2 . Further decrease in chamber height resulted in shear stress values that are physiologically unrealistic. Therefore, the channel height needs to be carefully chosen in a BAL design to avoid deleterious hydrodynamic effects on hepatocytes.
    keyword(s): Fluid dynamics , Computer simulation , Oxygen , Radial flow , Microchannels , Plasmas (Ionized gases) , Flow (Dynamics) , Stress , Tension , Shear (Mechanics) , Design , Disks , Bioreactors , Liver , Channels (Hydraulic engineering) , Simulation AND Pressure drop ,
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      Numerical Model of Fluid Flow and Oxygen Transport in a Radial-Flow Microchannel Containing Hepatocytes

    URI
    http://yetl.yabesh.ir/yetl1/handle/yetl/121838
    Collections
    • Journal of Biomechanical Engineering

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    contributor authorG. A. Ledezma
    contributor authorA. Folch
    contributor authorS. N. Bhatia
    contributor authorU. J. Balis
    contributor authorM. L. Yarmush
    contributor authorM. Toner
    date accessioned2017-05-08T23:59:04Z
    date available2017-05-08T23:59:04Z
    date copyrightFebruary, 1999
    date issued1999
    identifier issn0148-0731
    identifier otherJBENDY-26012#58_1.pdf
    identifier urihttp://yetl.yabesh.ir/yetl/handle/yetl/121838
    description abstractThe incorporation of monolayers of cultured hepatocytes into an extracorporeal perfusion system has become a promising approach for the development of a temporary bioartificial liver (BAL) support system. In this paper we present a numerical investigation of the oxygen tension, shear stress, and pressure drop in a bioreactor for a BAL composed of plasma-perfused chambers containing monolayers of porcine hepatocytes. The chambers consist of microfabricated parallel disks with center-to-edge radial flow. The oxygen uptake rate (OUR), measured in vitro for porcine hepatocytes, was curve-fitted using Michaelis–Menten kinetics for simulation of the oxygen concentration profile. The effect of different parameters that may influence the oxygen transport inside the chambers, such as the plasma flow rate, the chamber height, the initial oxygen tension in the perfused plasma, the OUR, and Km was investigated. We found that both the plasma flow rate and the initial oxygen tension may have an important effect upon oxygen transport. Increasing the flow rate and/or the inlet oxygen tension resulted in improved oxygen transport to cells in the radial-flow microchannels, and allowed significantly greater diameter reactor without oxygen limitation to the hepatocytes. In the range investigated in this paper (10 μm < H < 100 μm), and for a constant plasma flow rate, the chamber height, H, had a negligible effect on the oxygen transport to hepatocytes. On the contrary, it strongly affected the mechanical stress on the cells that is also crucial for the successful design of the BAL reactors. A twofold decrease in chamber height from 50 to 25 μm produced approximately a fivefold increase in maximal shear stress at the inlet of the reactor from 2 to 10 dyn/cm2 . Further decrease in chamber height resulted in shear stress values that are physiologically unrealistic. Therefore, the channel height needs to be carefully chosen in a BAL design to avoid deleterious hydrodynamic effects on hepatocytes.
    publisherThe American Society of Mechanical Engineers (ASME)
    titleNumerical Model of Fluid Flow and Oxygen Transport in a Radial-Flow Microchannel Containing Hepatocytes
    typeJournal Paper
    journal volume121
    journal issue1
    journal titleJournal of Biomechanical Engineering
    identifier doi10.1115/1.2798043
    journal fristpage58
    journal lastpage64
    identifier eissn1528-8951
    keywordsFluid dynamics
    keywordsComputer simulation
    keywordsOxygen
    keywordsRadial flow
    keywordsMicrochannels
    keywordsPlasmas (Ionized gases)
    keywordsFlow (Dynamics)
    keywordsStress
    keywordsTension
    keywordsShear (Mechanics)
    keywordsDesign
    keywordsDisks
    keywordsBioreactors
    keywordsLiver
    keywordsChannels (Hydraulic engineering)
    keywordsSimulation AND Pressure drop
    treeJournal of Biomechanical Engineering:;1999:;volume( 121 ):;issue: 001
    contenttypeFulltext
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