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Assessment of chemotherapeutic effects on cancer cells using adhesion noise spectroscopy

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  • Additional Information
    • Publication Information:
      Frontiers Media S.A., 2024.
    • Publication Date:
      2024
    • Collection:
      LCC:Biotechnology
    • Abstract:
      With cancer as one of the leading causes of death worldwide, there is a need for the development of accurate, cost-effective, easy-to-use, and fast drug-testing assays. While the NCI 60 cell-line screening as the gold standard is based on a colorimetric assay, monitoring cells electrically constitutes a label-free and non-invasive tool to assess the cytotoxic effects of a chemotherapeutic treatment on cancer cells. For decades, impedance-based cellular assays extensively investigated various cell characteristics affected by drug treatment but lack spatiotemporal resolution. With progress in microelectrode fabrication, high-density Complementary Metal Oxide Semiconductor (CMOS)-based microelectrode arrays (MEAs) with subcellular resolution and time-continuous recording capability emerged as a potent alternative. In this article, we present a new cell adhesion noise (CAN)-based electrical imaging technique to expand CMOS MEA cell-biology applications: CAN spectroscopy enables drug screening quantification with single-cell spatial resolution. The chemotherapeutic agent 5-Fluorouracil exerts a cytotoxic effect on colorectal cancer (CRC) cells hampering cell proliferation and lowering cell viability. For proof-of-concept, we found sufficient accuracy and reproducibility for CAN spectroscopy compared to a commercially available standard colorimetric biological assay. This label-free, non-invasive, and fast electrical imaging technique complements standardized cancer screening methods with significant advances over established impedance-based approaches.
    • File Description:
      electronic resource
    • ISSN:
      2296-4185
    • Relation:
      https://www.frontiersin.org/articles/10.3389/fbioe.2024.1385730/full; https://doaj.org/toc/2296-4185
    • Accession Number:
      10.3389/fbioe.2024.1385730
    • Accession Number:
      edsdoj.b1ab2aa1b247446db1ac3291d5e3d281