Abstract
The ability to monitor electrogenic cells accurately plays a pivotal role in neuroscience, cardiology and cell biology. Despite pioneering research and long-lasting efforts, the existing methods for intracellular recording of action potentials on the large network scale suffer limitations that prevent their widespread use. Here, we introduce the concept of a meta-electrode, a planar porous electrode that mimics the optical and biological behaviour of three-dimensional plasmonic antennas but also preserves the ability to work as an electrode. Its synergistic combination with plasmonic optoacoustic poration allows commercial complementary metal–oxide semiconductor multi-electrode arrays to record intracellular action potentials in large cellular networks. We apply this approach to measure signals from human-induced pluripotent stem cell-derived cardiac cells, rodent primary cardiomyocytes and immortalized cell types and demonstrate the possibility of non-invasively testing a variety of relevant drugs. Due to its robustness and easiness of use, we expect the method will be rapidly adopted by the scientific community and by pharmaceutical companies.
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Change history
28 August 2018
In the version of this Article originally published, the affiliation for the author Francesca Santoro was incorrectly given; it should have been ‘Center for Advanced Biomaterials for Healthcare, Istituto Italiano di Tecnologia, Napoli, Italy’. This has now been corrected in all versions of the Article.
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Acknowledgements
We thank M. Gandolfo and A. Maccione for discussions and for the impedance spectroscopy data of the CMOS-MEA electrodes. The research that led to these results received funding from the European Research Council under the European Union’s Seventh Framework Programme (FP/2007-2013)/ERC Grant Agreement no. [616213], CoG: Neuro-Plasmonics.
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Contributions
F.D.A. and M.D. conceived and designed the experiments. M.D., G.M. and L.L. performed the electrophysiology experiments. F.S. and V.C. performed the focused ion beam cross-sections and SEM imaging. A.J. and M.D. analysed the data. G.B., A.J. and D.G. characterized the porous meta-electrodes. G.B. and M.D. fabricated the passive MEA devices. M.D. and F.T. designed the experimental set-up. A.A. and A.S. performed the electromagnetic and thermal simulations. F.D.A. supervised the work. All the authors discussed the results and wrote the manuscript.
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Supplementary Information
Supplementary Methods, Supplementary Figures 1–15, Supplementary References
Supplementary Video 1
Whole CMOS-MEA recording during optoacoustic poration on one electrode. The optoacoustic poration occurs at t = 5 s.
Supplementary Video 2
Propagation wave in extracellular mode of human-induced pluripotent stem cells-derived cardiomyocytes on CMOS-MEA. The pixel colours represent the signals’ amplitude.
Supplementary Video 3
Propagation wave in intracellular mode of human-induced pluripotent stem cells-derived cardiomyocytes on CMOS-MEA. The pixel colours represent the signals’ amplitude.
Supplementary Video 4
Propagation wave in extracellular mode of human-induced pluripotent stem cells-derived cardiomyocytes on CMOS-MEA, including example extracellular waveforms from few electrodes. The brown vertical stripes in the graphs represent the time-bins used for calculating the amplitude for the pixel colouring in the map. The time-traces shown in the videos are highlighted by black square contours in the colour maps.
Supplementary Video 5
Propagation wave in intracellular mode of human-induced pluripotent stem cells-derived cardiomyocytes on CMOS-MEA, including example intracellular waveforms from few electrodes. The brown vertical stripes in the graphs represent the time-bins used for calculating the amplitude for the pixel colouring in the map. The time-traces shown in the videos are highlighted by black square contours in the colour maps.
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Dipalo, M., Melle, G., Lovato, L. et al. Plasmonic meta-electrodes allow intracellular recordings at network level on high-density CMOS-multi-electrode arrays. Nature Nanotech 13, 965–971 (2018). https://doi.org/10.1038/s41565-018-0222-z
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DOI: https://doi.org/10.1038/s41565-018-0222-z
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