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Imaging voltage in complete neuronal networks within patterned microislands reveals preferential wiring of excitatory hippocampal neurons

Alison S. Walker, Benjamin K. Raliski, Dat Vinh Nguyen, Patrick Zhang, Kate Sanders, Kaveh Karbasi, Evan W. Miller
doi: https://doi.org/10.1101/2020.10.09.332304
Alison S. Walker
‡Departments of Chemistry, University of California, Berkeley, 94720, United States of America
§Departments of Molecular & Cell Biology, University of California, Berkeley, 94720, United States of America
†Departments of Helen Wills Neuroscience Institute. University of California, Berkeley, 94720, United States of America
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Benjamin K. Raliski
‡Departments of Chemistry, University of California, Berkeley, 94720, United States of America
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Dat Vinh Nguyen
‡Departments of Chemistry, University of California, Berkeley, 94720, United States of America
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Patrick Zhang
‡Departments of Chemistry, University of California, Berkeley, 94720, United States of America
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Kate Sanders
‡Departments of Chemistry, University of California, Berkeley, 94720, United States of America
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Kaveh Karbasi
‡Departments of Chemistry, University of California, Berkeley, 94720, United States of America
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Evan W. Miller
‡Departments of Chemistry, University of California, Berkeley, 94720, United States of America
§Departments of Molecular & Cell Biology, University of California, Berkeley, 94720, United States of America
†Departments of Helen Wills Neuroscience Institute. University of California, Berkeley, 94720, United States of America
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  • For correspondence: evanwmiller@berkeley.edu
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Abstract

Voltage imaging with fluorescent dyes affords the opportunity to map neuronal activity in both time and space. One limitation to imaging is the inability to image complete neuronal networks: some fraction of cells remains outside of the observation window. Here, we combine voltage imaging, post hoc immunocytochemistry, and patterned microisland hippocampal culture to provide imaging of complete neuronal networks. The patterned microislands completely fill the field of view of our high-speed (500 Hz) camera, enabling reconstruction of the spiking patterns of every single neuron in the network. Cultures raised on microislands develop similarly to neurons grown on coverslips and display similar composition of inhibitory and excitatory cell types. The principal excitatory cell types (CA1, CA3, and dentate granule cells, or DGC) are also present in similar proportions in both preparations. We calculate the likelihood that action potential firing in one neuron to trigger action potential firing in a downstream neuron in a spontaneously active network to construct a functional connection map of these neuronal ensembles. Importantly, this functional map indicates preferential connectivity between DGC and CA3 neurons and between CA3 and CA1 neurons, mimicking the neuronal circuitry of the intact hippocampus. We envision that patterned microislands, in combination with voltage imaging and methods to classify cell types, will be a powerful method for exploring neuronal function in both healthy and disease states. Additionally, because the entire neuronal network is sampled simultaneously, this strategy has the power to go further, revealing all functional connections between all cell types.

Significance Statement In vitro model systems provide unsurpassed control and access for exploring the molecular and cellular details of neurobiology. We developed a patterned microisland system for culturing rat hippocampal neurons that recapitulates the features of bulk hippocampal cultures, but with the added benefit of allowing access to high-speed imaging of entire neuronal ensembles using voltage imaging. By using far-red voltage-sensitive fluorophores, we map the functional connections across all cells in the neuronal ensemble, revealing that several important functional synapses present in the intact hippocampus are recapitulated in this microisland system. We envision the methods described here will be a powerful complement to ongoing research into basic neurobiological mechanisms and the search for therapies to treat diseases arising from their dysfunction.

Competing Interest Statement

EWM and ASW are listed as inventors on a patent application filed by the Regents of the University of California describing "long wavelength voltage sensitive dyes."

Footnotes

  • Conflict of Interest: EWM and ASW are listed as inventors on a patent application filed by the Regents of the University of California describing “long wavelength voltage sensitive dyes.”

Copyright 
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY-NC 4.0 International license.
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Posted October 10, 2020.
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Imaging voltage in complete neuronal networks within patterned microislands reveals preferential wiring of excitatory hippocampal neurons
Alison S. Walker, Benjamin K. Raliski, Dat Vinh Nguyen, Patrick Zhang, Kate Sanders, Kaveh Karbasi, Evan W. Miller
bioRxiv 2020.10.09.332304; doi: https://doi.org/10.1101/2020.10.09.332304
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Imaging voltage in complete neuronal networks within patterned microislands reveals preferential wiring of excitatory hippocampal neurons
Alison S. Walker, Benjamin K. Raliski, Dat Vinh Nguyen, Patrick Zhang, Kate Sanders, Kaveh Karbasi, Evan W. Miller
bioRxiv 2020.10.09.332304; doi: https://doi.org/10.1101/2020.10.09.332304

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