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多模态 CMOS 芯片上平面电极阵列和平滑肌成纤维细胞共培养进行心肌细胞内电位记录。

Intracellular cardiomyocytes potential recording by planar electrode array and fibroblasts co-culturing on multi-modal CMOS chip.

机构信息

School of Electrical and Computer Engineering, Georgia Institute of Technology, Atlanta, GA, USA.

Department of Biomedical Engineering, Emory University, Atlanta, GA, USA.

出版信息

Biosens Bioelectron. 2019 Nov 1;144:111626. doi: 10.1016/j.bios.2019.111626. Epub 2019 Aug 28.

Abstract

Intracellular action potential signals reveal enriched physiological information. Patch clamp techniques have been widely used to measure intracellular potential. Despite their high signal fidelity, they suffer from low throughput. Recently, 3D nanoelectrodes have been developed for intracellular potential recording. However, they are limited by scalability, yield, and cost, directly constraining their use in monitoring large number of cells and high throughput applications. In this paper, we demonstrate intracellular potential monitoring of cardiomyocytes using simple 2D planar electrode array in a standard CMOS process without patch clamps or post fabricated 3D nanoelectrodes. This is enabled by our unique cardiomyocytes/fibroblasts co-culturing technique and electroporation. The co-cultured fibroblasts promote tight sealing of cardiomyocytes on electrodes and enable high-fidelity intracellular potential monitoring based on 2D planar electrode. Compared to existing technologies, our platform has a unique potential to achieve an unprecedented combination of throughput, spatiotemporal resolution, and a tissue-level field-of-view for cellular electrophysiology monitoring.

摘要

细胞内动作电位信号揭示了丰富的生理信息。膜片钳技术已被广泛用于测量细胞内电位。尽管它们具有很高的信号保真度,但它们的通量较低。最近,已经开发出 3D 纳米电极用于细胞内电位记录。然而,它们受到可扩展性、产量和成本的限制,这直接限制了它们在监测大量细胞和高通量应用中的使用。在本文中,我们展示了使用标准 CMOS 工艺中的简单 2D 平面电极阵列在没有膜片钳或后制造的 3D 纳米电极的情况下进行心肌细胞的细胞内电位监测。这是通过我们独特的心肌细胞/成纤维细胞共培养技术和电穿孔实现的。共培养的成纤维细胞促进心肌细胞在电极上紧密密封,并能够基于 2D 平面电极实现高保真度的细胞内电位监测。与现有技术相比,我们的平台具有独特的潜力,可以实现细胞电生理学监测的吞吐量、时空分辨率和组织级视场的前所未有的组合。

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