基于集成电化学检测系统的微流控芯片监测肿瘤转移的力学响应。

IF 5.4 2区 工程技术 Q1 BIOCHEMICAL RESEARCH METHODS
Lab on a Chip Pub Date : 2025-07-02 DOI:10.1039/D5LC00563A
Shuqi Chen, Hang Qi, Yuanheng Kuang, Quanning Li, Xuejiao Chen and Yanyan Wang
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引用次数: 0

摘要

监测肿瘤细胞在迁移过程中的机械反应是了解肿瘤转移机制的关键。目前对细胞力学反应的研究主要利用微观观察技术,而实时监测细胞反应仍然有限。在这项工作中,我们提出了一种微流控肿瘤迁移芯片,该芯片结合了电化学阻抗谱来研究肿瘤细胞的力学响应。在此平台上,详细评估了空间约束和流体剪切应力对乳腺癌肿瘤细胞形态和迁移能力的影响,并证明了这两种力学因素同时调节肿瘤细胞的形态、迁移速度和迁移方式。具体而言,适度的空间约束和流体剪切应力可促进肿瘤细胞的迁移,并影响其迁移方式的改变。此外,采用电化学阻抗谱法评价肿瘤细胞在不同机械刺激下的阻抗变化。基于该检测系统,不仅可以量化微通道内迁移细胞的数量,还可以表征MDA-MB-231细胞在紧密空间约束下向变形虫迁移模式的转变,以及在流体剪切应力作用下细胞形态的伸长和向间质模式的转变。该平台证明了实时监测细胞响应机械刺激变化的可行性,并为阐明细胞入侵机制提供了有价值的工具。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Monitoring the mechanical responses of tumor metastasis based on a microfluidic chip integrated with an electrochemical detection system†

Monitoring the mechanical responses of tumor metastasis based on a microfluidic chip integrated with an electrochemical detection system†

Monitoring the mechanical responses of tumor cells during migration is crucial for understanding the mechanisms of tumor metastasis. Current studies on cellular mechanical responses primarily utilize microscopic observation techniques, while real-time monitoring cellular responses remains limited. In this work, we present a microfluidic tumor migration chip that incorporates electrochemical impedance spectroscopy to study the mechanical responses of tumor cells. Based on this platform, the impacts of spatial confinement and fluid shear stress on the morphology and migratory capacity of breast cancer tumor cells were evaluated in detail, and it was demonstrated that the morphology, migratory velocity and migratory mode of tumor cells are concurrently modulated by these two mechanical factors. Specifically, moderate spatial confinement and fluid shear stress have been observed to promote the migration of tumor cells and affect the change of their migration mode. Furthermore, electrochemical impedance spectroscopy was employed to evaluate the impedance change of tumor cells under different mechanical stimulation. Based on this detection system, not only the number of migrating cells within the microchannels can be quantified, but the transition of MDA-MB-231 cells to an amoeboid migration mode under tight spatial confinement, as well as the elongation of the cell morphology and transition to a mesenchymal mode due to fluid shear stress, can also be characterized. This platform demonstrates the feasibility of real-time monitoring of cell changes in response to mechanical stimuli, and offers a valuable tool for elucidating the mechanisms underlying cell invasion.

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来源期刊
Lab on a Chip
Lab on a Chip 工程技术-化学综合
CiteScore
11.10
自引率
8.20%
发文量
434
审稿时长
2.6 months
期刊介绍: Lab on a Chip is the premiere journal that publishes cutting-edge research in the field of miniaturization. By their very nature, microfluidic/nanofluidic/miniaturized systems are at the intersection of disciplines, spanning fundamental research to high-end application, which is reflected by the broad readership of the journal. Lab on a Chip publishes two types of papers on original research: full-length research papers and communications. Papers should demonstrate innovations, which can come from technical advancements or applications addressing pressing needs in globally important areas. The journal also publishes Comments, Reviews, and Perspectives.
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