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Cited 3 time in webofscience Cited 3 time in scopus
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Integration of reconfigurable microchannels into aligned three-dimensional neural networks for spatially controllable neuromodulationopen access

Authors
Jeong, SohyeonKang, Hyun WookKim, So HyunHong, Gyu-SangNam, Min-HoSeong, JihyeYoon, Eui-SungCho, Il-JooChung, SeokBang, SeokyoungKim, Hong NamChoi, Nakwon
Issue Date
Mar-2023
Publisher
American Association for the Advancement of Science
Keywords
Collagen; Collagen; Calcium Compounds; Microchannels; Potassium Compounds; Sol-gels; Animal Model; Ca 2+; Functional Connectivity; In-vitro; Integration Of Micro-channel; Localised; Neural-networks; Neuromodulation; Reconfigurable; Spatiotemporal Control; Chlorine Compounds; Collagen; Animal; Brain; Physiology; Animals; Brain; Collagen
Citation
Science Advances, v.9, no.10
Indexed
SCIE
SCOPUS
Journal Title
Science Advances
Volume
9
Number
10
URI
https://scholarworks.dongguk.edu/handle/sw.dongguk/20330
DOI
10.1126/sciadv.adf0925
ISSN
2375-2548
2375-2548
Abstract
Anisotropically organized neural networks are indispensable routes for functional connectivity in the brain, which remains largely unknown. While prevailing animal models require additional preparation and stimulation-applying devices and have exhibited limited capabilities regarding localized stimulation, no in vitro platform exists that permits spatiotemporal control of chemo-stimulation in anisotropic three-dimensional (3D) neural networks. We present the integration of microchannels seamlessly into a fibril-aligned 3D scaffold by adapting a single fabrication principle. We investigated the underlying physics of elastic microchannels' ridges and interfacial sol-gel transition of collagen under compression to determine a critical window of geometry and strain. We demonstrated the spatiotemporally resolved neuromodulation in an aligned 3D neural network by local deliveries of KCl and Ca2+ signal inhibitors, such as tetrodotoxin, nifedipine, and mibefradil, and also visualized Ca2+ signal propagation with a speed of similar to 3.7 mu m/s. We anticipate that our technology will pave the way to elucidate functional connectivity and neurological diseases associated with transsynaptic propagation.
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