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Simultaneous time-varying viscosity, elasticity, and mass measurements of single adherent cancer cells across cell cycle

机译:在细胞周期上同时的时变粘度,弹性和质量测量单粘附癌细胞

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摘要

Biophysical studies on single cells have linked cell mechanics to physiology, functionality and disease. Evaluation of mass and viscoelasticity versus cell cycle can provide further insights into cell cycle progression and the uncontrolled proliferation of cancer. Using our pedestal microelectromechanical systems resonant sensors, we have developed a non-contact interferometric measurement technique that simultaneously tracks the dynamic changes in the viscoelastic moduli and mass of adherent colon (HT-29) and breast cancer (MCF-7) cells from the interphase through mitosis and then to the cytokinesis stages of their growth cycle. We show that by combining three optomechanical parameters in an optical path length equation and a two-degree-of-freedom model, we can simultaneously extract the viscoelasticity and mass as a function of the nano-scaled membrane fluctuation of each adherent cell. Our measurements are able to discern between soft and stiff cells across the cell cycle and demonstrated sharp viscoelastic changes due to cortical stiffening around mitosis. Cell rounding before division can be detected by measurement of mechanical coupling between the cells and the sensors. Our measurement device and method can provide for new insights into the mechanics of single adherent cells versus time.
机译:对单细胞的生物物理研究对生理学,功能和疾病具有连接的细胞力学。质量和粘弹性的评估与细胞周期相比,可以进一步了解细胞周期进展和癌细胞的不受控制的增殖。使用我们的基座微机电系统共振传感器,我们开发了一种非接触式干涉测量技术,同时跟踪粘附性模育和抗粘附结肠(HT-29)和乳腺癌(MCF-7)细胞的动态变化通过有丝分裂,然后通过细胞因子阶段的生长周期。我们表明,通过在光路长度方程中结合三个光学力学参数和两度自由度模型,我们可以同时提取粘弹性和质量作为每个粘附细胞的纳米缩放膜波动的函数。我们的测量能够在细胞周期横跨细胞周期之间辨别柔软和僵硬的电池,并且由于皮质溶解而展示了尖锐的粘弹性变化。通过测量电池和传感器之间的机械耦合,可以检测分裂前的细胞圆形。我们的测量装置和方法可以为单个粘附细胞的机械师提供新的见解与时间相比。

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