Microelectrode Arrays Measure Blocking of Voltage‐Gated Calcium Ion Channels on Supported Lipid Bilayers Derived from Primary Neurons

Author:

Lu Zixuan1ORCID,Barberio Chiara1ORCID,Fernandez‐Villegas Ana1,Withers Aimee1,Wheeler Alexandra1,Kallitsis Konstantinos1ORCID,Martinelli Eleonora1,Savva Achilleas1ORCID,Hess Becky M.2,Pappa Anna‐Maria134,Schierle Gabriele S. Kaminski1,Owens Róisín M.1ORCID

Affiliation:

1. Department of Chemical Engineering and Biotechnology University of Cambridge Philippa Fawcett Drive Cambridge CB3 0AS UK

2. Pacific Northwest National Laboratory 902 Battelle Boulevard Richland WA 99 354 USA

3. Department of Biomedical Engineering Khalifa University of Science and Technology Abu Dhabi 127788 UAE

4. Healthcare Engineering Innovation Center (HEIC) Khalifa University of Science and Technology Abu Dhabi 127 788 UAE

Abstract

AbstractDrug studies targeting neuronal ion channels are crucial to understand neuronal function and develop therapies for neurological diseases. The traditional method to study neuronal ion‐channel activities heavily relies on the whole‐cell patch clamp as the industry standard. However, this technique is both technically challenging and labour‐intensive, while involving the complexity of keeping cells alive with low throughput. Therefore, the shortcomings are limiting the efficiency of ion‐channel‐related neuroscience research and drug testing. Here, this work reports a new system of integrating neuron membranes with organic microelectrode arrays (OMEAs) for ion‐channel‐related drug studies. This work demonstrates that the supported lipid bilayers (SLBs) derived from both neuron‐like (neuroblastoma) cells and primary neurons are integrated with OMEAs for the first time. The increased expression of voltage‐gated calcium (CaV) ion channels on differentiated SH‐SY5Y SLBs  compared to non‐differentiated ones is sensed electrically. Also, dose‐response of the CaV ion‐channel blocking effect on primary cortical neuronal SLBs from rats is monitored. The dose range causing ion channel blocking is comparable to literature. This system overcomes the major challenges from traditional methods (e.g., patch clamp) and showcases an easy‐to‐test, rapid, ultra‐sensitive, cell‐free, and high‐throughput platform to monitor dose‐dependent ion‐channel blocking effects on native neuronal membranes.

Funder

HORIZON EUROPE Marie Sklodowska-Curie Actions

Defense Advanced Research Projects Agency

Air Force Office of Scientific Research

European Research Council

Publisher

Wiley

Subject

General Physics and Astronomy,General Engineering,Biochemistry, Genetics and Molecular Biology (miscellaneous),General Materials Science,General Chemical Engineering,Medicine (miscellaneous)

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