Engineered biological neural networks on high density CMOS microelectrode arrays

Author:

Duru JensORCID,Küchler Joël,Ihle Stephan J.,Forró Csaba,Bernardi Aeneas,Girardin Sophie,Hengsteler Julian,Wheeler Stephen,Vörös JánosORCID,Ruff TobiasORCID

Abstract

ABSTRACTIn bottom-up neuroscience, questions on neural information processing are addressed by engineering small but reproducible biological neural networks of defined network topology in vitro. The network topology can be controlled by culturing neurons within polydimethylsiloxane (PDMS) microstructures that are combined with microelectrode arrays (MEAs) for electric access to the network. However, currently used glass MEAs are limited to 256 electrodes and pose a limitation to the spatial resolution as well as the design of more complex microstructures. The use of high density complementary metal-oxide-semiconductor (CMOS) MEAs greatly increases the spatiotemporal resolution, enabling sub-cellular readout and stimulation of neurons in defined neural networks. Unfortunately, the non-planar surface of CMOS MEAs complicates the attachment of PDMS microstructures. To overcome the problem of axons escaping the microstructures through the ridges of the CMOS MEA, we stamp-transferred a thin film of hexane-diluted PDMS onto the array such that the PDMS filled the ridges at the contact surface of the microstructures without clogging the axon guidance channels. Moreover, we provide an impedance-based method to visualize the exact location of the microstructures on the MEA and show that our method can confine axonal growth within the PDMS microstructures. Finally, the high spatiotemporal resolution of the CMOS MEA enabled us to show that we can guide action potentials using the unidirectional topology of our circular multi-node microstructure.

Publisher

Cold Spring Harbor Laboratory

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1. Stability Analysis of Mutually Synchronized Spatially Distributed 24 GHz Oscillators;2022 IEEE International Instrumentation and Measurement Technology Conference (I2MTC);2022-05-16

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