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A fluid-walled microfluidic platform for human neuron microcircuits and directed axotomy

Output Details

Preprint November 17, 2023

Published June 5, 2024

In our brains, different neurons make appropriate connections; however, there remain few in vitro models of such circuits. We use an open microfluidic approach to build and study neuronal circuits in vitro in ways that fit easily into existing bio-medical workflows. Dumbbell-shaped circuits are built in minutes in standard Petri dishes; the aqueous phase is confined by fluid walls – interfaces between cell-growth medium and an immiscible fluorocarbon, FC40. Conditions are established that ensure post-mitotic neurons derived from human induced pluripotent stem cells (iPSCs) plated in one chamber of a dumbbell remain where deposited. After seeding cortical neurons on one side, axons grow through the connecting conduit to ramify amongst striatal neurons on the other – an arrangement mimicking unidirectional cortico-striatal connectivity. We also develop a moderate-throughput non-contact axotomy assay. Cortical axons in conduits are severed by a media jet; then, brain-derived neurotrophic factor and striatal neurons in distal chambers promote axon regeneration. As additional conduits and chambers are easily added, this opens up the possibility of mimicking complex neuronal networks, and screening drugs for their effects on connectivity.
Identifier (DOI)
10.1039/d4lc00107a
Tags
  • Cortical
  • Dopaminergic neurons
  • hiPSCs (Human induced pluripotent stem cells)
  • Microfluidic devices
  • Original Research

Meet the Authors

  • User avatar fallback logo

    Federico Nebuloni

    External Collaborator

  • User avatar fallback logo

    Quyen Do

    Key Personnel: Team Cragg

    University of Oxford

  • User avatar fallback logo

    Peter Cook

    External Collaborator

  • User avatar fallback logo

    Edmond Walsh

    External Collaborator

  • Richard Wade-Martins, PhD

    Co-PI (Core Leadership): Team Cragg

    University of Oxford

Aligning Science Across Parkinson's
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