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Microfluidic biosensing of viscoelastic properties of normal and cancerous human breast cells

机译:正常和癌性人乳腺细胞粘弹性质的微流控生物传感

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Biomechanical properties have been revealed as potential biomarkers for distinguishing cancer cells from normal cells. In this work, we report a novel technique using a confining microchannel embedded with microelectrodes for biomechanical phenotyping for floating human cells, including one normal breast cell line (MCF-10A) and two breast cancer cell lines (MCF-7 and MDA-MB-231). The floating cells move under a defined pressure profile along the microchannel, in which the cells deform dynamically under compression by the channel sidewalls. We adopt Hertz and Tatara models to convert the deformed cell shapes to cell diameters and transient stress-strain ratios. By further considering the cell viscoelasticity as a Standard Linear Solid (SLS) model, we compute for whole-cell viscosity, and instantaneous and relaxed moduli. Our results show that the selected cell types have significant different viscoelastic properties. Applications of the electrode-embedded confining microchannel can achieve high-throughput, continuous-flow deep phenotyping of rare cells by functionalizing channel side walls with antibodies for both biomechanical and biochemical biomarkers for more comprehensive and promising cell characterization.
机译:已经揭示出生物力学性质作为区分癌细胞与正常细胞的潜在生物标记。在这项工作中,我们报告了一种新技术,该技术使用嵌入微电极的封闭微通道对漂浮的人类细胞进行生物力学表型分析,包括一种正常的乳腺癌细胞系(MCF-10A)和两种乳腺癌细胞系(MCF-7和MDA-MB- 231)。漂浮的细胞在限定的压力分布下沿着微通道移动,其中,细胞在通道侧壁的压缩作用下动态变形。我们采用Hertz和Tatara模型将变形的单元形状转换为单元直径和瞬态应力应变比。通过进一步将细胞粘弹性视为标准线性固体(SLS)模型,我们可以计算全细胞粘度以及瞬时和松弛模量。我们的结果表明,所选的细胞类型具有显着不同的粘弹性质。嵌入电极的封闭微通道的应用可以通过用生物力学和生化生物标记的抗体功能化通道侧壁来实现稀有细胞的高通量,连续流深表型化,从而实现更全面和有希望的细胞表征。

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