N-acetylcysteine prevents HIV gp 120-related damage of human cultured astrocytes: correlation with glutamine synthase dysfunction

<p>Abstract</p> <p>Background</p> <p>HIV envelope gp 120 glycoprotein is released during active HIV infection of brain macrophages thereby generating inflammation and oxidative stress which contribute to the development of the AIDS-Dementia Complex (ADC). Gp120 has also...

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Main Authors: Costa Nicola, Palma Ernesto, Sculco Francesca, Sacco Iolanda, Muscoli Carolina, Visalli Valeria, Colica Carmela, Rotiroti Domenicantonio, Mollace Vincenzo
Format: Article
Language:English
Published: BMC 2007-12-01
Series:BMC Neuroscience
Online Access:http://www.biomedcentral.com/1471-2202/8/106
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spelling doaj-10bd9bebf44e4da3ac000d6fc9c014ed2020-11-24T23:18:02ZengBMCBMC Neuroscience1471-22022007-12-018110610.1186/1471-2202-8-106N-acetylcysteine prevents HIV gp 120-related damage of human cultured astrocytes: correlation with glutamine synthase dysfunctionCosta NicolaPalma ErnestoSculco FrancescaSacco IolandaMuscoli CarolinaVisalli ValeriaColica CarmelaRotiroti DomenicantonioMollace Vincenzo<p>Abstract</p> <p>Background</p> <p>HIV envelope gp 120 glycoprotein is released during active HIV infection of brain macrophages thereby generating inflammation and oxidative stress which contribute to the development of the AIDS-Dementia Complex (ADC). Gp120 has also been found capable to generate excitotoxic effect on brain tissue via enhancement of glutamatergic neurotransmission, leading to neuronal and astroglial damage, though the mechanism is still to be better understood.</p> <p>Here we investigated on the effect of N-acetylcysteine (NAC), on gp120-induced damage in human cultured astroglial cells and the possible contribution of gp120-related reacting oxygen species (ROS) in the imbalanced activity of glutamine synthase (GS), the enzyme that metabolizes glutamate into glutamine within astroglial cells playing a neuroprotective role in brain disorders.</p> <p>Results</p> <p>Incubation of Lipari human cultured astroglial cells with gp 120 (0.1–10 nM) produced a significant reduction of astroglial cell viability and apoptosis as evaluated by TUNEL reaction and flow cytometric analysis (FACS). This effect was accompanied by lipid peroxidation as detected by means of malondialdehyde assay (MDA). In addition, gp 120 reduced both glutamine concentration in astroglial cell supernatants and GS expression as detected by immunocytochemistry and western blotting analysis. Pre-treatment of cells with NAC (0.5–5 mM), dose-dependently antagonised astroglial apoptotic cell death induced by gp 120, an effect accompanied by significant attenuation of MDA accumulation. Furthermore, both effects were closely associated with a significant recovery of glutamine levels in cell supernatants and by GS expression, thus suggesting that overproduction of free radicals might contribute in gp 120-related dysfunction of GS in astroglial cells.</p> <p>Conclusion</p> <p>In conclusion, the present experiments demonstrate that gp 120 is toxic to astroglial cells, an effect accompanied by lipid peroxidation and by altered glutamine release. All the effects of gp120 on astroglial cells were counteracted by NAC thus suggesting a novel and potentially useful approach in the treatment of glutammatergic disorders found in HAD patients.</p> http://www.biomedcentral.com/1471-2202/8/106
collection DOAJ
language English
format Article
sources DOAJ
author Costa Nicola
Palma Ernesto
Sculco Francesca
Sacco Iolanda
Muscoli Carolina
Visalli Valeria
Colica Carmela
Rotiroti Domenicantonio
Mollace Vincenzo
spellingShingle Costa Nicola
Palma Ernesto
Sculco Francesca
Sacco Iolanda
Muscoli Carolina
Visalli Valeria
Colica Carmela
Rotiroti Domenicantonio
Mollace Vincenzo
N-acetylcysteine prevents HIV gp 120-related damage of human cultured astrocytes: correlation with glutamine synthase dysfunction
BMC Neuroscience
author_facet Costa Nicola
Palma Ernesto
Sculco Francesca
Sacco Iolanda
Muscoli Carolina
Visalli Valeria
Colica Carmela
Rotiroti Domenicantonio
Mollace Vincenzo
author_sort Costa Nicola
title N-acetylcysteine prevents HIV gp 120-related damage of human cultured astrocytes: correlation with glutamine synthase dysfunction
title_short N-acetylcysteine prevents HIV gp 120-related damage of human cultured astrocytes: correlation with glutamine synthase dysfunction
title_full N-acetylcysteine prevents HIV gp 120-related damage of human cultured astrocytes: correlation with glutamine synthase dysfunction
title_fullStr N-acetylcysteine prevents HIV gp 120-related damage of human cultured astrocytes: correlation with glutamine synthase dysfunction
title_full_unstemmed N-acetylcysteine prevents HIV gp 120-related damage of human cultured astrocytes: correlation with glutamine synthase dysfunction
title_sort n-acetylcysteine prevents hiv gp 120-related damage of human cultured astrocytes: correlation with glutamine synthase dysfunction
publisher BMC
series BMC Neuroscience
issn 1471-2202
publishDate 2007-12-01
description <p>Abstract</p> <p>Background</p> <p>HIV envelope gp 120 glycoprotein is released during active HIV infection of brain macrophages thereby generating inflammation and oxidative stress which contribute to the development of the AIDS-Dementia Complex (ADC). Gp120 has also been found capable to generate excitotoxic effect on brain tissue via enhancement of glutamatergic neurotransmission, leading to neuronal and astroglial damage, though the mechanism is still to be better understood.</p> <p>Here we investigated on the effect of N-acetylcysteine (NAC), on gp120-induced damage in human cultured astroglial cells and the possible contribution of gp120-related reacting oxygen species (ROS) in the imbalanced activity of glutamine synthase (GS), the enzyme that metabolizes glutamate into glutamine within astroglial cells playing a neuroprotective role in brain disorders.</p> <p>Results</p> <p>Incubation of Lipari human cultured astroglial cells with gp 120 (0.1–10 nM) produced a significant reduction of astroglial cell viability and apoptosis as evaluated by TUNEL reaction and flow cytometric analysis (FACS). This effect was accompanied by lipid peroxidation as detected by means of malondialdehyde assay (MDA). In addition, gp 120 reduced both glutamine concentration in astroglial cell supernatants and GS expression as detected by immunocytochemistry and western blotting analysis. Pre-treatment of cells with NAC (0.5–5 mM), dose-dependently antagonised astroglial apoptotic cell death induced by gp 120, an effect accompanied by significant attenuation of MDA accumulation. Furthermore, both effects were closely associated with a significant recovery of glutamine levels in cell supernatants and by GS expression, thus suggesting that overproduction of free radicals might contribute in gp 120-related dysfunction of GS in astroglial cells.</p> <p>Conclusion</p> <p>In conclusion, the present experiments demonstrate that gp 120 is toxic to astroglial cells, an effect accompanied by lipid peroxidation and by altered glutamine release. All the effects of gp120 on astroglial cells were counteracted by NAC thus suggesting a novel and potentially useful approach in the treatment of glutammatergic disorders found in HAD patients.</p>
url http://www.biomedcentral.com/1471-2202/8/106
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