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    Freezing-Assisted Intracellular Drug Delivery to Multidrug Resistant Cancer Cells

    Source: Journal of Biomechanical Engineering:;2009:;volume( 131 ):;issue: 007::page 74513
    Author:
    Ka Yaw Teo
    ,
    Bumsoo Han
    DOI: 10.1115/1.3153325
    Publisher: The American Society of Mechanical Engineers (ASME)
    Abstract: The efficacy of chemotherapy is significantly impaired by the multidrug resistance (MDR) of cancer cells. The mechanism of MDR is associated with the overexpression of certain adenosine triphosphate-binding cassette protein transporters in plasma membranes, which actively pump out cytotoxic drugs from the intracellular space. In this study, we tested a hypothesis that freezing and thawing (F/T) may enhance intracellular drug delivery to MDR cancer cells via F/T-induced denaturation of MDR-associated proteins and/or membrane permeabilization. After a human MDR cancer cell line (NCI/ADR-RES) was exposed to several F/T conditions, its cellular drug uptake was quantified by a fluorescent calcein assay using calcein as a model drug. After F/T to −20°C, the intracellular uptake of calcein increased by 70.1% (n=5, P=0.0004). It further increased to 118% as NCI/ADR-RES cells were frozen/thawed to −40°C (n=3, P=0.009). These results support the hypothesis, and possible mechanisms of F/T-enhanced intracellular drug delivery were proposed and discussed.
    keyword(s): Freezing , Drug delivery systems , Cancer , Drugs , Membranes , Mechanisms AND Proteins ,
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      Freezing-Assisted Intracellular Drug Delivery to Multidrug Resistant Cancer Cells

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    http://yetl.yabesh.ir/yetl1/handle/yetl/139908
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    contributor authorKa Yaw Teo
    contributor authorBumsoo Han
    date accessioned2017-05-09T00:31:38Z
    date available2017-05-09T00:31:38Z
    date copyrightJuly, 2009
    date issued2009
    identifier issn0148-0731
    identifier otherJBENDY-26987#074513_1.pdf
    identifier urihttp://yetl.yabesh.ir/yetl/handle/yetl/139908
    description abstractThe efficacy of chemotherapy is significantly impaired by the multidrug resistance (MDR) of cancer cells. The mechanism of MDR is associated with the overexpression of certain adenosine triphosphate-binding cassette protein transporters in plasma membranes, which actively pump out cytotoxic drugs from the intracellular space. In this study, we tested a hypothesis that freezing and thawing (F/T) may enhance intracellular drug delivery to MDR cancer cells via F/T-induced denaturation of MDR-associated proteins and/or membrane permeabilization. After a human MDR cancer cell line (NCI/ADR-RES) was exposed to several F/T conditions, its cellular drug uptake was quantified by a fluorescent calcein assay using calcein as a model drug. After F/T to −20°C, the intracellular uptake of calcein increased by 70.1% (n=5, P=0.0004). It further increased to 118% as NCI/ADR-RES cells were frozen/thawed to −40°C (n=3, P=0.009). These results support the hypothesis, and possible mechanisms of F/T-enhanced intracellular drug delivery were proposed and discussed.
    publisherThe American Society of Mechanical Engineers (ASME)
    titleFreezing-Assisted Intracellular Drug Delivery to Multidrug Resistant Cancer Cells
    typeJournal Paper
    journal volume131
    journal issue7
    journal titleJournal of Biomechanical Engineering
    identifier doi10.1115/1.3153325
    journal fristpage74513
    identifier eissn1528-8951
    keywordsFreezing
    keywordsDrug delivery systems
    keywordsCancer
    keywordsDrugs
    keywordsMembranes
    keywordsMechanisms AND Proteins
    treeJournal of Biomechanical Engineering:;2009:;volume( 131 ):;issue: 007
    contenttypeFulltext
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