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Cell cycle-dependent force transmission in cancer cells

机译:癌细胞中细胞周期依赖性力传递

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摘要

The generation of traction forces and their transmission to the extracellular environment supports the disseminative migration of cells from a primary tumor. In cancer cells, the periodic variation of nuclear stiffness during the cell cycle provides a functional link between efficient translocation and proliferation. However, the mechanical framework completing this picture remains unexplored. Here, the Fucci2 reporter was expressed in various human epithelial cancer cells to resolve their cell cycle phase transition. The corresponding tractions were captured by a recently developed reference-free confocal traction-force microscopy platform. The combined approach was conducive to the analysis of phase-dependent force variation at the level of individual integrin contacts. Detected forces were invariably higher in the G1 and early S phases than in the ensuing late S/G2, and locally colocalized with high levels of paxillin phosphorylation. Perturbation of paxillin phosphorylation at focal adhesions, obtained through the biochemical inhibition of focal adhesion kinase (FAK) or the transfection of nonphosphorylatable or phosphomimetic paxillin mutants, significantly diminished the force transmitted to the substrate. These data demonstrate a reproducible modulation of force transmission during the cell cycle progression of cancer cells, instrumental to their invasion of dense environments. In addition, they delineate a model in which paxillin phosphorylation supports the mechanical maturation of adhesions relaying forces to the substrate.
机译:牵引力的产生及其对细胞外环境的透射支持来自初级肿瘤的细胞的易动迁移。在癌细胞中,细胞周期期间核刚度的周期性变化提供了有效的易位和增殖之间的功能性联系。但是,完成此图片的机械框架仍未开发。这里,FUCCI2报告者在各种人上皮癌细胞中表达以解决其细胞周期阶段转变。通过最近开发的基准共聚焦牵引力显微镜平台捕获相应的诉讼。合并的方法有利于分析个体整合蛋白触点的相位依赖性力变化。在G1和早期S阶段中检测到的力总是更高的,而不是随后的S / G2,并且具有高水平的帕雪林磷酸化局部覆盖。通过局灶性粘附激酶(FAK)的生物化学抑制或非磷属可磷酸化或磷脂素突变体的转染而获得的卵毛蛋白磷酸化的扰动,显着减少了传递到基材的力。这些数据表明了在癌细胞的细胞周期进展过程中的可重复调节癌细胞的进展,有助于它们对致密环境的侵袭。此外,它们描绘了一种模型,其中帕西林磷酸化支撑粘连的机械成熟转换到基板。

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  • 来源
    《Molecular biology of the cell》 |2018年第21期|共12页
  • 作者单位

    Swiss Fed Inst Technol Lab Thermodynam Emerging Technol Dept Mech &

    Proc Engn CH-8092 Zurich Switzerland;

    Swiss Fed Inst Technol Lab Thermodynam Emerging Technol Dept Mech &

    Proc Engn CH-8092 Zurich Switzerland;

    Swiss Fed Inst Technol Lab Thermodynam Emerging Technol Dept Mech &

    Proc Engn CH-8092 Zurich Switzerland;

    Swiss Fed Inst Technol Lab Thermodynam Emerging Technol Dept Mech &

    Proc Engn CH-8092 Zurich Switzerland;

    Swiss Fed Inst Technol Lab Thermodynam Emerging Technol Dept Mech &

    Proc Engn CH-8092 Zurich Switzerland;

    Swiss Fed Inst Technol Lab Thermodynam Emerging Technol Dept Mech &

    Proc Engn CH-8092 Zurich Switzerland;

    Swiss Fed Inst Technol Lab Thermodynam Emerging Technol Dept Mech &

    Proc Engn CH-8092 Zurich Switzerland;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
  • 关键词

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