Development of an integrated microperfusion-EEG electrode for unbiased multimodal sampling of brain interstitial fluid and concurrent neural activity

Objective. To modify off-the-shelf components to build a device for collecting electroencephalography (EEG) from macroelectrodes surrounded by large fluid access ports sampled by an integrated microperfusion system in order to establish a method for sampling brain interstitial fluid (ISF) at the sit...

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Autores principales: Stangler, Luke A, Nicolai, Evan N, Mivalt, Filip, Chang, Su-Youne, Kim, Inyong, Kouzani, Abbas Z, Bennet, Kevin, Berk, Michael, Uthamaraj, Susheil, Burns, Terry C, Worrell, Gregory A, Howe, Charles L
Formato: Online Artículo Texto
Lenguaje:English
Publicado: IOP Publishing 2023
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Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9855636/
https://www.ncbi.nlm.nih.gov/pubmed/36538815
http://dx.doi.org/10.1088/1741-2552/acad29
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author Stangler, Luke A
Nicolai, Evan N
Mivalt, Filip
Chang, Su-Youne
Kim, Inyong
Kouzani, Abbas Z
Bennet, Kevin
Berk, Michael
Uthamaraj, Susheil
Burns, Terry C
Worrell, Gregory A
Howe, Charles L
author_facet Stangler, Luke A
Nicolai, Evan N
Mivalt, Filip
Chang, Su-Youne
Kim, Inyong
Kouzani, Abbas Z
Bennet, Kevin
Berk, Michael
Uthamaraj, Susheil
Burns, Terry C
Worrell, Gregory A
Howe, Charles L
author_sort Stangler, Luke A
collection PubMed
description Objective. To modify off-the-shelf components to build a device for collecting electroencephalography (EEG) from macroelectrodes surrounded by large fluid access ports sampled by an integrated microperfusion system in order to establish a method for sampling brain interstitial fluid (ISF) at the site of stimulation or seizure activity with no bias for molecular size. Approach. Twenty-four 560 µm diameter holes were ablated through the sheath surrounding one platinum–iridium macroelectrode of a standard Spencer depth electrode using a femtosecond UV laser. A syringe pump was converted to push–pull configuration and connected to the fluidics catheter of a commercially available microdialysis system. The fluidics were inserted into the lumen of the modified Spencer electrode with the microdialysis membrane removed, converting the system to open flow microperfusion. Electrical performance and analyte recovery were measured and parameters were systematically altered to improve performance. An optimized device was tested in the pig brain and unbiased quantitative mass spectrometry was used to characterize the perfusate collected from the peri-electrode brain in response to stimulation. Main results. Optimized parameters resulted in >70% recovery of 70 kDa dextran from a tissue analog. The optimized device was implanted in the cortex of a pig and perfusate was collected during four 60 min epochs. Following a baseline epoch, the macroelectrode surrounded by microperfusion ports was stimulated at 2 Hz (0.7 mA, 200 µs pulse width). Following a post-stimulation epoch, the cortex near the electrode was stimulated with benzylpenicillin to induce epileptiform activity. Proteomic analysis of the perfusates revealed a unique inflammatory signature induced by electrical stimulation. This signature was not detected in bulk tissue ISF. Significance. A modified dual-sensing electrode that permits coincident detection of EEG and ISF at the site of epileptiform neural activity may reveal novel pathogenic mechanisms and therapeutic targets that are otherwise undetectable at the bulk tissue level.
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spelling pubmed-98556362023-01-23 Development of an integrated microperfusion-EEG electrode for unbiased multimodal sampling of brain interstitial fluid and concurrent neural activity Stangler, Luke A Nicolai, Evan N Mivalt, Filip Chang, Su-Youne Kim, Inyong Kouzani, Abbas Z Bennet, Kevin Berk, Michael Uthamaraj, Susheil Burns, Terry C Worrell, Gregory A Howe, Charles L J Neural Eng Paper Objective. To modify off-the-shelf components to build a device for collecting electroencephalography (EEG) from macroelectrodes surrounded by large fluid access ports sampled by an integrated microperfusion system in order to establish a method for sampling brain interstitial fluid (ISF) at the site of stimulation or seizure activity with no bias for molecular size. Approach. Twenty-four 560 µm diameter holes were ablated through the sheath surrounding one platinum–iridium macroelectrode of a standard Spencer depth electrode using a femtosecond UV laser. A syringe pump was converted to push–pull configuration and connected to the fluidics catheter of a commercially available microdialysis system. The fluidics were inserted into the lumen of the modified Spencer electrode with the microdialysis membrane removed, converting the system to open flow microperfusion. Electrical performance and analyte recovery were measured and parameters were systematically altered to improve performance. An optimized device was tested in the pig brain and unbiased quantitative mass spectrometry was used to characterize the perfusate collected from the peri-electrode brain in response to stimulation. Main results. Optimized parameters resulted in >70% recovery of 70 kDa dextran from a tissue analog. The optimized device was implanted in the cortex of a pig and perfusate was collected during four 60 min epochs. Following a baseline epoch, the macroelectrode surrounded by microperfusion ports was stimulated at 2 Hz (0.7 mA, 200 µs pulse width). Following a post-stimulation epoch, the cortex near the electrode was stimulated with benzylpenicillin to induce epileptiform activity. Proteomic analysis of the perfusates revealed a unique inflammatory signature induced by electrical stimulation. This signature was not detected in bulk tissue ISF. Significance. A modified dual-sensing electrode that permits coincident detection of EEG and ISF at the site of epileptiform neural activity may reveal novel pathogenic mechanisms and therapeutic targets that are otherwise undetectable at the bulk tissue level. IOP Publishing 2023-02-01 2023-01-18 /pmc/articles/PMC9855636/ /pubmed/36538815 http://dx.doi.org/10.1088/1741-2552/acad29 Text en © 2023 The Author(s). Published by IOP Publishing Ltd https://creativecommons.org/licenses/by/4.0/ Original content from this work may be used under the terms of the Creative Commons Attribution 4.0 license (https://creativecommons.org/licenses/by/4.0/) . Any further distribution of this work must maintain attribution to the author(s) and the title of the work, journal citation and DOI.
spellingShingle Paper
Stangler, Luke A
Nicolai, Evan N
Mivalt, Filip
Chang, Su-Youne
Kim, Inyong
Kouzani, Abbas Z
Bennet, Kevin
Berk, Michael
Uthamaraj, Susheil
Burns, Terry C
Worrell, Gregory A
Howe, Charles L
Development of an integrated microperfusion-EEG electrode for unbiased multimodal sampling of brain interstitial fluid and concurrent neural activity
title Development of an integrated microperfusion-EEG electrode for unbiased multimodal sampling of brain interstitial fluid and concurrent neural activity
title_full Development of an integrated microperfusion-EEG electrode for unbiased multimodal sampling of brain interstitial fluid and concurrent neural activity
title_fullStr Development of an integrated microperfusion-EEG electrode for unbiased multimodal sampling of brain interstitial fluid and concurrent neural activity
title_full_unstemmed Development of an integrated microperfusion-EEG electrode for unbiased multimodal sampling of brain interstitial fluid and concurrent neural activity
title_short Development of an integrated microperfusion-EEG electrode for unbiased multimodal sampling of brain interstitial fluid and concurrent neural activity
title_sort development of an integrated microperfusion-eeg electrode for unbiased multimodal sampling of brain interstitial fluid and concurrent neural activity
topic Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9855636/
https://www.ncbi.nlm.nih.gov/pubmed/36538815
http://dx.doi.org/10.1088/1741-2552/acad29
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