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    Atomic Force Microscopy Stiffness Mapping in Human Aortic Smooth Muscle Cells

    Source: Journal of Biomechanical Engineering:;2022:;volume( 144 ):;issue: 008::page 81001-1
    Author:
    Petit, Claudie
    ,
    Karkhaneh Yousefi, Ali-Akbar
    ,
    Guilbot, Marine
    ,
    Barnier, Vincent
    ,
    Avril, Stéphane
    DOI: 10.1115/1.4053657
    Publisher: The American Society of Mechanical Engineers (ASME)
    Abstract: Aortic smooth muscle cells (SMCs) play a vital role in maintaining mechanical homeostasis in the aorta. We recently found that SMCs of aneurysmal aortas apply larger traction forces than SMCs of healthy aortas. This result was explained by the significant increase of hypertrophic SMCs abundance in aneurysms. In this study, we investigate whether the cytoskeleton stiffness of SMCs may also be altered in aneurysmal aortas. For that, we use atomic force microscopy (AFM) nano-indentation with a specific mode that allows subcellular-resolution mapping of the local stiffness across a specified region of interest of the cell. Aortic SMCs from a commercial human lineage (AoSMCs, Lonza) and primary aneurysmal SMCs (AnevSMCs) are cultured in conditions promoting the development of their contractile apparatus, and seeded on hydrogels with stiffness properties of 12 kPa and 25 kPa. Results show that all SMCs exhibit globally a lognormal stiffness distribution, with medians in the range 10–30 kPa. The mean of stiffness distributions is 16 kPa in aneurysmal SMCs and 12 kPa in healthy cells, but the differences are not statistically significant due to the large dispersion of AFM nano-indentation stiffness. We conclude that the possible alterations previously found in aneurysmal SMCs do not affect significantly the AFM nano-indentation stiffness of their cytoskeleton.
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      Atomic Force Microscopy Stiffness Mapping in Human Aortic Smooth Muscle Cells

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    http://yetl.yabesh.ir/yetl1/handle/yetl/4283937
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    contributor authorPetit, Claudie
    contributor authorKarkhaneh Yousefi, Ali-Akbar
    contributor authorGuilbot, Marine
    contributor authorBarnier, Vincent
    contributor authorAvril, Stéphane
    date accessioned2022-05-08T08:26:55Z
    date available2022-05-08T08:26:55Z
    date copyright2/21/2022 12:00:00 AM
    date issued2022
    identifier issn0148-0731
    identifier otherbio_144_08_081001.pdf
    identifier urihttp://yetl.yabesh.ir/yetl1/handle/yetl/4283937
    description abstractAortic smooth muscle cells (SMCs) play a vital role in maintaining mechanical homeostasis in the aorta. We recently found that SMCs of aneurysmal aortas apply larger traction forces than SMCs of healthy aortas. This result was explained by the significant increase of hypertrophic SMCs abundance in aneurysms. In this study, we investigate whether the cytoskeleton stiffness of SMCs may also be altered in aneurysmal aortas. For that, we use atomic force microscopy (AFM) nano-indentation with a specific mode that allows subcellular-resolution mapping of the local stiffness across a specified region of interest of the cell. Aortic SMCs from a commercial human lineage (AoSMCs, Lonza) and primary aneurysmal SMCs (AnevSMCs) are cultured in conditions promoting the development of their contractile apparatus, and seeded on hydrogels with stiffness properties of 12 kPa and 25 kPa. Results show that all SMCs exhibit globally a lognormal stiffness distribution, with medians in the range 10–30 kPa. The mean of stiffness distributions is 16 kPa in aneurysmal SMCs and 12 kPa in healthy cells, but the differences are not statistically significant due to the large dispersion of AFM nano-indentation stiffness. We conclude that the possible alterations previously found in aneurysmal SMCs do not affect significantly the AFM nano-indentation stiffness of their cytoskeleton.
    publisherThe American Society of Mechanical Engineers (ASME)
    titleAtomic Force Microscopy Stiffness Mapping in Human Aortic Smooth Muscle Cells
    typeJournal Paper
    journal volume144
    journal issue8
    journal titleJournal of Biomechanical Engineering
    identifier doi10.1115/1.4053657
    journal fristpage81001-1
    journal lastpage81001-11
    page11
    treeJournal of Biomechanical Engineering:;2022:;volume( 144 ):;issue: 008
    contenttypeFulltext
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    DSpace software copyright © 2002-2015  DuraSpace
    نرم افزار کتابخانه دیجیتال "دی اسپیس" فارسی شده توسط یابش برای کتابخانه های ایرانی | تماس با یابش
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