Superoxide dismutase reduces monosodium glutamate-induced injury in an organotypic whole hemisphere brain slice model of excitotoxicity
Abstract Background Knowledge of glutamate excitotoxicity has increased substantially over the past few decades, with multiple proposed pathways involved in inflicting damage. We sought to develop a monosodium glutamate (MSG) exposed ex vivo organotypic whole hemisphere (OWH) brain slice model of ex...
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doaj-91257632227a4c2e9f5626b6c83997412021-02-07T12:26:26ZengBMCJournal of Biological Engineering1754-16112020-02-0114111210.1186/s13036-020-0226-8Superoxide dismutase reduces monosodium glutamate-induced injury in an organotypic whole hemisphere brain slice model of excitotoxicityRick Liao0Thomas R. Wood1Elizabeth Nance2Department of Chemical Engineering, University of WashingtonDepartment of Pediatrics, University of WashingtonDepartment of Chemical Engineering, University of WashingtonAbstract Background Knowledge of glutamate excitotoxicity has increased substantially over the past few decades, with multiple proposed pathways involved in inflicting damage. We sought to develop a monosodium glutamate (MSG) exposed ex vivo organotypic whole hemisphere (OWH) brain slice model of excitotoxicity to study excitotoxic processes and screen the efficacy of superoxide dismutase (SOD). Results The OWH model is a reproducible platform with high cell viability and retained cellular morphology. OWH slices exposed to MSG induced significant cytotoxicity and downregulation of neuronal excitation-related gene expression. The OWH brain slice model has enabled us to isolate and study components of excitotoxicity, distinguishing the effects of glutamate excitation, hyperosmolar stress, and inflammation. We find that extracellularly administered SOD is significantly protective in inhibiting cell death and restoring healthy mitochondrial morphology. SOD efficacy suggests that superoxide scavenging is a promising therapeutic strategy in excitotoxic injury. Conclusions Using OWH brain slice models, we can obtain a better understanding of the pathological mechanisms of excitotoxic injury, and more rapidly screen potential therapeutics.https://doi.org/10.1186/s13036-020-0226-8Oxidative stressPeroxynitriteMitochondriaNeuroinflammationHyperosmolar stress8-hydroxy-2-deoxyguanosine |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Rick Liao Thomas R. Wood Elizabeth Nance |
spellingShingle |
Rick Liao Thomas R. Wood Elizabeth Nance Superoxide dismutase reduces monosodium glutamate-induced injury in an organotypic whole hemisphere brain slice model of excitotoxicity Journal of Biological Engineering Oxidative stress Peroxynitrite Mitochondria Neuroinflammation Hyperosmolar stress 8-hydroxy-2-deoxyguanosine |
author_facet |
Rick Liao Thomas R. Wood Elizabeth Nance |
author_sort |
Rick Liao |
title |
Superoxide dismutase reduces monosodium glutamate-induced injury in an organotypic whole hemisphere brain slice model of excitotoxicity |
title_short |
Superoxide dismutase reduces monosodium glutamate-induced injury in an organotypic whole hemisphere brain slice model of excitotoxicity |
title_full |
Superoxide dismutase reduces monosodium glutamate-induced injury in an organotypic whole hemisphere brain slice model of excitotoxicity |
title_fullStr |
Superoxide dismutase reduces monosodium glutamate-induced injury in an organotypic whole hemisphere brain slice model of excitotoxicity |
title_full_unstemmed |
Superoxide dismutase reduces monosodium glutamate-induced injury in an organotypic whole hemisphere brain slice model of excitotoxicity |
title_sort |
superoxide dismutase reduces monosodium glutamate-induced injury in an organotypic whole hemisphere brain slice model of excitotoxicity |
publisher |
BMC |
series |
Journal of Biological Engineering |
issn |
1754-1611 |
publishDate |
2020-02-01 |
description |
Abstract Background Knowledge of glutamate excitotoxicity has increased substantially over the past few decades, with multiple proposed pathways involved in inflicting damage. We sought to develop a monosodium glutamate (MSG) exposed ex vivo organotypic whole hemisphere (OWH) brain slice model of excitotoxicity to study excitotoxic processes and screen the efficacy of superoxide dismutase (SOD). Results The OWH model is a reproducible platform with high cell viability and retained cellular morphology. OWH slices exposed to MSG induced significant cytotoxicity and downregulation of neuronal excitation-related gene expression. The OWH brain slice model has enabled us to isolate and study components of excitotoxicity, distinguishing the effects of glutamate excitation, hyperosmolar stress, and inflammation. We find that extracellularly administered SOD is significantly protective in inhibiting cell death and restoring healthy mitochondrial morphology. SOD efficacy suggests that superoxide scavenging is a promising therapeutic strategy in excitotoxic injury. Conclusions Using OWH brain slice models, we can obtain a better understanding of the pathological mechanisms of excitotoxic injury, and more rapidly screen potential therapeutics. |
topic |
Oxidative stress Peroxynitrite Mitochondria Neuroinflammation Hyperosmolar stress 8-hydroxy-2-deoxyguanosine |
url |
https://doi.org/10.1186/s13036-020-0226-8 |
work_keys_str_mv |
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