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一种用于在受限条件下表征癌细胞迁移的电动渗透微流控系统。

An electro-osmotic microfluidic system to characterize cancer cell migration under confinement.

机构信息

1 Department of Mechanical Engineering, The University of Hong Kong , Hong Kong SAR , People's Republic of China.

2 Department of Clinical Oncology, Queen Elizabeth Hospital , Hong Kong SAR , People's Republic of China.

出版信息

J R Soc Interface. 2019 Jun 28;16(155):20190062. doi: 10.1098/rsif.2019.0062. Epub 2019 Jun 5.

Abstract

We have developed a novel electro-osmotic microfluidic system to apply precisely controlled osmolarity gradients to cancer cells in micro-channels. We observed that albeit adhesion is not required for cells to migrate in such a confined microenvironment, the migrating velocity of cells is strongly influenced by the interactions between the cells and the channel wall, with a stronger adhesion leading to diminished cell motility. Furthermore, through examining more than 20 different types of cancer cells, we found a linear positive correlation between the protein concentration of the aquaporin-4 (AQP4) and the cell migrating speed. Knockdown of AQP4 in invasive re-populated cancer stem cells reduced their migration capability down to the level that is comparable to their parental cancer cells. Interestingly, these observations can all be quantitatively explained by the osmotic engine model where the cell movement is assumed to be driven by cross-membrane ion/water transport, while adhesion acts as a frictional resistance against the cell motility. By providing versatile and controllable features in regulating and characterizing the migration capability of cells, our system may serve as a useful tool in quantifying how cell motility is influenced by different physical and biochemical factors, as well as elucidating the mechanisms behind, in the future.

摘要

我们开发了一种新颖的电渗透微流控系统,可在微通道中精确控制渗透压梯度以应用于癌细胞。我们观察到,尽管细胞在这种受限的微环境中迁移不需要黏附,但细胞的迁移速度受到细胞与通道壁之间相互作用的强烈影响,更强的黏附导致细胞迁移能力降低。此外,通过检查超过 20 种不同类型的癌细胞,我们发现水通道蛋白-4(AQP4)的蛋白浓度与细胞迁移速度之间存在线性正相关。侵袭性再定植癌症干细胞中 AQP4 的敲低将其迁移能力降低至与其亲本癌细胞相当的水平。有趣的是,这些观察结果都可以通过渗透压引擎模型来定量解释,其中假设细胞运动是由跨膜离子/水转运驱动的,而黏附作用则作为细胞迁移的摩擦阻力。通过提供灵活可控的特性来调节和表征细胞的迁移能力,我们的系统将来可能成为一种有用的工具,用于量化不同物理和生化因素如何影响细胞迁移能力,并阐明其背后的机制。

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