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    Numerical Study of Thermally Targeted Liposomal Drug Delivery in Tumor

    Source: Journal of Heat Transfer:;2009:;volume( 131 ):;issue: 004::page 43209
    Author:
    Aili Zhang
    ,
    Lisa X. Xu
    ,
    Xipeng Mi
    ,
    Geer Yang
    DOI: 10.1115/1.3072952
    Publisher: The American Society of Mechanical Engineers (ASME)
    Abstract: The efficacy of cancer chemotherapy can be greatly enhanced by thermally targeted nanoparticle liposome drug delivery system. A new theoretical model coupling heat and mass transfer has been developed to study the spatial and transient drug distributions. In this model, the influence of tumor cell apoptosis and necrosis in drug transport is also considered, in addition to the tumor microvasculature permeability to nanoliposomes. The model predictions agree well with our previous experimental results, and it has been used to simulate the nanoparticle drug distribution in the tumor under hyperthermic conditions. Results show that hyperthermia alone only enhances drug accumulation in the periphery of a tumor with 1 cm in radius, and the tumor cells in the central region are hardly damaged due to poor drug diffusion. Apoptosis or necrosis of the tumor cells could significantly influence the drug penetration and should be accounted for in drug diffusion modeling to accurately predict the therapeutic effect. Simulation study on the combined radio frequency ablation and liposomal doxorubicin delivery shows more effective treatment outcome, especially for larger tumors. The present model can be used to predict the treatment outcome and optimize the clinical protocol.
    keyword(s): Drugs , Tumors , Drug delivery systems AND Biological tissues ,
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      Numerical Study of Thermally Targeted Liposomal Drug Delivery in Tumor

    URI
    http://yetl.yabesh.ir/yetl1/handle/yetl/141095
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    contributor authorAili Zhang
    contributor authorLisa X. Xu
    contributor authorXipeng Mi
    contributor authorGeer Yang
    date accessioned2017-05-09T00:33:53Z
    date available2017-05-09T00:33:53Z
    date copyrightApril, 2009
    date issued2009
    identifier issn0022-1481
    identifier otherJHTRAO-27859#043209_1.pdf
    identifier urihttp://yetl.yabesh.ir/yetl/handle/yetl/141095
    description abstractThe efficacy of cancer chemotherapy can be greatly enhanced by thermally targeted nanoparticle liposome drug delivery system. A new theoretical model coupling heat and mass transfer has been developed to study the spatial and transient drug distributions. In this model, the influence of tumor cell apoptosis and necrosis in drug transport is also considered, in addition to the tumor microvasculature permeability to nanoliposomes. The model predictions agree well with our previous experimental results, and it has been used to simulate the nanoparticle drug distribution in the tumor under hyperthermic conditions. Results show that hyperthermia alone only enhances drug accumulation in the periphery of a tumor with 1 cm in radius, and the tumor cells in the central region are hardly damaged due to poor drug diffusion. Apoptosis or necrosis of the tumor cells could significantly influence the drug penetration and should be accounted for in drug diffusion modeling to accurately predict the therapeutic effect. Simulation study on the combined radio frequency ablation and liposomal doxorubicin delivery shows more effective treatment outcome, especially for larger tumors. The present model can be used to predict the treatment outcome and optimize the clinical protocol.
    publisherThe American Society of Mechanical Engineers (ASME)
    titleNumerical Study of Thermally Targeted Liposomal Drug Delivery in Tumor
    typeJournal Paper
    journal volume131
    journal issue4
    journal titleJournal of Heat Transfer
    identifier doi10.1115/1.3072952
    journal fristpage43209
    identifier eissn1528-8943
    keywordsDrugs
    keywordsTumors
    keywordsDrug delivery systems AND Biological tissues
    treeJournal of Heat Transfer:;2009:;volume( 131 ):;issue: 004
    contenttypeFulltext
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    DSpace software copyright © 2002-2015  DuraSpace
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