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    Role of Cytoskeletal Components in Stress-Relaxation Behavior of Adherent Vascular Smooth Muscle Cells

    Source: Journal of Biomechanical Engineering:;2009:;volume( 131 ):;issue: 004::page 41001
    Author:
    Jason D. Hemmer
    ,
    Jiro Nagatomi
    ,
    Scott T. Wood
    ,
    Alexey A. Vertegel
    ,
    Delphine Dean
    ,
    Martine LaBerge
    DOI: 10.1115/1.3049860
    Publisher: The American Society of Mechanical Engineers (ASME)
    Abstract: A number of recent studies have demonstrated the effectiveness of atomic force microscopy (AFM) for characterization of cellular stress-relaxation behavior. However, this technique’s recent development creates considerable need for exploration of appropriate mechanical models for analysis of the resultant data and of the roles of various cytoskeletal components responsible for governing stress-relaxation behavior. The viscoelastic properties of vascular smooth muscle cells (VSMCs) are of particular interest due to their role in the development of vascular diseases, including atherosclerosis and restenosis. Various cytoskeletal agents, including cytochalasin D, jasplakinolide, paclitaxel, and nocodazole, were used to alter the cytoskeletal architecture of the VSMCs. Stress-relaxation experiments were performed on the VSMCs using AFM. The quasilinear viscoelastic (QLV) reduced-relaxation function, as well as a simple power-law model, and the standard linear solid (SLS) model, were fitted to the resultant stress-relaxation data. Actin depolymerization via cytochalasin D resulted in significant increases in both rate of relaxation and percentage of relaxation; actin stabilization via jasplakinolide did not affect stress-relaxation behavior. Microtubule depolymerization via nocodazole resulted in nonsignificant increases in rate and percentage of relaxation, while microtubule stabilization via paclitaxel caused significant decreases in both rate and percentage of relaxation. Both the QLV reduced-relaxation function and the power-law model provided excellent fits to the data (R2=0.98), while the SLS model was less adequate (R2=0.91). Data from the current study indicate the important role of not only actin, but also microtubules, in governing VSMC viscoelastic behavior. Excellent fits to the data show potential for future use of both the QLV reduced-relaxation function and power-law models in conjunction with AFM stress-relaxation experiments.
    keyword(s): Relaxation (Physics) , Stress , Muscle AND Atomic force microscopy ,
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      Role of Cytoskeletal Components in Stress-Relaxation Behavior of Adherent Vascular Smooth Muscle Cells

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    http://yetl.yabesh.ir/yetl1/handle/yetl/139968
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    • Journal of Biomechanical Engineering

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    contributor authorJason D. Hemmer
    contributor authorJiro Nagatomi
    contributor authorScott T. Wood
    contributor authorAlexey A. Vertegel
    contributor authorDelphine Dean
    contributor authorMartine LaBerge
    date accessioned2017-05-09T00:31:45Z
    date available2017-05-09T00:31:45Z
    date copyrightApril, 2009
    date issued2009
    identifier issn0148-0731
    identifier otherJBENDY-26924#041001_1.pdf
    identifier urihttp://yetl.yabesh.ir/yetl/handle/yetl/139968
    description abstractA number of recent studies have demonstrated the effectiveness of atomic force microscopy (AFM) for characterization of cellular stress-relaxation behavior. However, this technique’s recent development creates considerable need for exploration of appropriate mechanical models for analysis of the resultant data and of the roles of various cytoskeletal components responsible for governing stress-relaxation behavior. The viscoelastic properties of vascular smooth muscle cells (VSMCs) are of particular interest due to their role in the development of vascular diseases, including atherosclerosis and restenosis. Various cytoskeletal agents, including cytochalasin D, jasplakinolide, paclitaxel, and nocodazole, were used to alter the cytoskeletal architecture of the VSMCs. Stress-relaxation experiments were performed on the VSMCs using AFM. The quasilinear viscoelastic (QLV) reduced-relaxation function, as well as a simple power-law model, and the standard linear solid (SLS) model, were fitted to the resultant stress-relaxation data. Actin depolymerization via cytochalasin D resulted in significant increases in both rate of relaxation and percentage of relaxation; actin stabilization via jasplakinolide did not affect stress-relaxation behavior. Microtubule depolymerization via nocodazole resulted in nonsignificant increases in rate and percentage of relaxation, while microtubule stabilization via paclitaxel caused significant decreases in both rate and percentage of relaxation. Both the QLV reduced-relaxation function and the power-law model provided excellent fits to the data (R2=0.98), while the SLS model was less adequate (R2=0.91). Data from the current study indicate the important role of not only actin, but also microtubules, in governing VSMC viscoelastic behavior. Excellent fits to the data show potential for future use of both the QLV reduced-relaxation function and power-law models in conjunction with AFM stress-relaxation experiments.
    publisherThe American Society of Mechanical Engineers (ASME)
    titleRole of Cytoskeletal Components in Stress-Relaxation Behavior of Adherent Vascular Smooth Muscle Cells
    typeJournal Paper
    journal volume131
    journal issue4
    journal titleJournal of Biomechanical Engineering
    identifier doi10.1115/1.3049860
    journal fristpage41001
    identifier eissn1528-8951
    keywordsRelaxation (Physics)
    keywordsStress
    keywordsMuscle AND Atomic force microscopy
    treeJournal of Biomechanical Engineering:;2009:;volume( 131 ):;issue: 004
    contenttypeFulltext
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