Glutathione cycle in diquat neurotoxicity: Assessed by intrastriatal pre-treatment with glutathione reductase

Diquat (DQ) neurotoxicity mechanisms are unknown, although, it's systemic toxicity is mediated by free radical reactions. The role of glutathione cycle was assessed by glutathione reductase (GR) applied in the pre-treatment of DQ poisoning. Wistar rats were used and tested compounds were adm...

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Main Authors: Đurđević Dragan, Đukić Mirjana, Ninković Milica, Stevanović Ivana, Jovanović Marina, Vasić Una
Format: Article
Language:English
Published: Sciendo 2013-01-01
Series:Acta Veterinaria
Subjects:
Online Access:http://www.doiserbia.nb.rs/img/doi/0567-8315/2013/0567-83151303159D.pdf
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spelling doaj-69c82ea61c544ee4a1063e958f4a33e72020-11-24T23:39:30ZengSciendoActa Veterinaria0567-83151820-74482013-01-01632-315917510.2298/AVB1303159DGlutathione cycle in diquat neurotoxicity: Assessed by intrastriatal pre-treatment with glutathione reductaseĐurđević DraganĐukić MirjanaNinković MilicaStevanović IvanaJovanović MarinaVasić UnaDiquat (DQ) neurotoxicity mechanisms are unknown, although, it's systemic toxicity is mediated by free radical reactions. The role of glutathione cycle was assessed by glutathione reductase (GR) applied in the pre-treatment of DQ poisoning. Wistar rats were used and tested compounds were administered intrastriatally (i.s.) in one single dose. Total glutathione (tGSH), glutathione disulfide (GSSG) and glutathione peroxidase (GPx) were measured in the vulnerable brain regions (VBRs) (striatum, hippocampus and cortex), at 30 minutes, 24 hours and 7 days post treatment. Results from the intact and the sham operated groups were not statistically different. Rapid spatial spreading of oxidative stress was confirmed in the examined VBRs. Mortality (30-40%, within 24hrs) and signs of lethargy were observed in the DQ group. Activity of GPx activity was elevated and GSSG/GSH was higher in the examined VBRs during the experiment, compared to the controls. The i.s. pre-treatment with GR achieved neuroprotective role against DQ induced neurotoxicity, based on animal survival, absence of lethargy and decreased GPx activity and GSSG/GSH in the examined VBRs during the experiment, compared to the DQ group. Our results confirmed that oxidation of GSH was the reason for the reduced antioxidative defense against DQ neurotoxicity. [Projekat Ministarstva nauke Republike Srbije, br. III41018]http://www.doiserbia.nb.rs/img/doi/0567-8315/2013/0567-83151303159D.pdfdiquatglutathioneglutathione disulfideglutathione peroxidaseglutathione reductaseneurotoxicity
collection DOAJ
language English
format Article
sources DOAJ
author Đurđević Dragan
Đukić Mirjana
Ninković Milica
Stevanović Ivana
Jovanović Marina
Vasić Una
spellingShingle Đurđević Dragan
Đukić Mirjana
Ninković Milica
Stevanović Ivana
Jovanović Marina
Vasić Una
Glutathione cycle in diquat neurotoxicity: Assessed by intrastriatal pre-treatment with glutathione reductase
Acta Veterinaria
diquat
glutathione
glutathione disulfide
glutathione peroxidase
glutathione reductase
neurotoxicity
author_facet Đurđević Dragan
Đukić Mirjana
Ninković Milica
Stevanović Ivana
Jovanović Marina
Vasić Una
author_sort Đurđević Dragan
title Glutathione cycle in diquat neurotoxicity: Assessed by intrastriatal pre-treatment with glutathione reductase
title_short Glutathione cycle in diquat neurotoxicity: Assessed by intrastriatal pre-treatment with glutathione reductase
title_full Glutathione cycle in diquat neurotoxicity: Assessed by intrastriatal pre-treatment with glutathione reductase
title_fullStr Glutathione cycle in diquat neurotoxicity: Assessed by intrastriatal pre-treatment with glutathione reductase
title_full_unstemmed Glutathione cycle in diquat neurotoxicity: Assessed by intrastriatal pre-treatment with glutathione reductase
title_sort glutathione cycle in diquat neurotoxicity: assessed by intrastriatal pre-treatment with glutathione reductase
publisher Sciendo
series Acta Veterinaria
issn 0567-8315
1820-7448
publishDate 2013-01-01
description Diquat (DQ) neurotoxicity mechanisms are unknown, although, it's systemic toxicity is mediated by free radical reactions. The role of glutathione cycle was assessed by glutathione reductase (GR) applied in the pre-treatment of DQ poisoning. Wistar rats were used and tested compounds were administered intrastriatally (i.s.) in one single dose. Total glutathione (tGSH), glutathione disulfide (GSSG) and glutathione peroxidase (GPx) were measured in the vulnerable brain regions (VBRs) (striatum, hippocampus and cortex), at 30 minutes, 24 hours and 7 days post treatment. Results from the intact and the sham operated groups were not statistically different. Rapid spatial spreading of oxidative stress was confirmed in the examined VBRs. Mortality (30-40%, within 24hrs) and signs of lethargy were observed in the DQ group. Activity of GPx activity was elevated and GSSG/GSH was higher in the examined VBRs during the experiment, compared to the controls. The i.s. pre-treatment with GR achieved neuroprotective role against DQ induced neurotoxicity, based on animal survival, absence of lethargy and decreased GPx activity and GSSG/GSH in the examined VBRs during the experiment, compared to the DQ group. Our results confirmed that oxidation of GSH was the reason for the reduced antioxidative defense against DQ neurotoxicity. [Projekat Ministarstva nauke Republike Srbije, br. III41018]
topic diquat
glutathione
glutathione disulfide
glutathione peroxidase
glutathione reductase
neurotoxicity
url http://www.doiserbia.nb.rs/img/doi/0567-8315/2013/0567-83151303159D.pdf
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