There is increasing evidence that oxidative stress is involved in the etiology and pathogenesis of neurodegenerative disorders. Overproduction of reactive oxygen species (ROS) is due in part to the reactivity of catecholamines, such as dopamine, adrenaline, and noradrenaline. These molecules are rapidly converted, chemically or enzymatically, into catechol-quinone and then into highly deleterious semiquinone radicals after 1-electron reduction in cells. Notably, the overexpression of dihydronicotinamide riboside: quinone oxidoreductase (QR2) in Chinese hamster ovary (CHO) cells increases the production of ROS, mainly superoxide radicals, when it is exposed to exogenous catechol-quinones (e.g. dopachrome, aminochrome, and adrenochrome). Here we used electron paramagnetic resonance analysis to demonstrate that the phenomenon observed in CHO cells is also seen in human leukemic cells (K562 cells) that naturally express QR2. Moreover, by manipulating the level of QR2 in neuronal cells, including immortalized neuroblast cells and ex vivo neurons isolated from QR2 knockout animals, we showed that there is a direct relationship between QR2-mediated quinone reduction and ROS overproduction. Supporting this result, the withdraw of the QR2 co-factor (BNAH) or the addition of the specific QR2 inhibitor S29434 suppressed oxidative stress. Taken together, these data suggest that the overexpression of QR2 in brain cells in the presence of catechol quinones might lead to ROS-induced cell death via the rapid conversion of superoxide radicals into hydrogen peroxide and then into highly reactive hydroxyl radicals. Thus, QR2 may be implicated in the early stages of neurodegenerative disorders.
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Univ Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
IRD, UMR 152, F-31062 Toulouse 9, FranceUniv Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
Cassagnes, Laure-Estelle
Perio, Pierre
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Univ Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
IRD, UMR 152, F-31062 Toulouse 9, FranceUniv Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
Perio, Pierre
Ferry, Gilles
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Inst Rech Servier, Biotechnol Pharmacol Mol & Cellulaire, F-78290 Croissy Sur Seine, FranceUniv Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
Ferry, Gilles
Moulharat, Natacha
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Inst Rech Servier, Biotechnol Pharmacol Mol & Cellulaire, F-78290 Croissy Sur Seine, FranceUniv Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
Moulharat, Natacha
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Antoine, Mathias
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Gayon, Regis
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Boutin, Jean A.
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Nepveu, Francoise
Reybier, Karine
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Univ Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
IRD, UMR 152, F-31062 Toulouse 9, FranceUniv Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
机构:
Univ Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
IRD, UMR 152, F-31062 Toulouse 9, FranceUniv Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
Cassagnes, Laure-Estelle
Perio, Pierre
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h-index: 0
机构:
Univ Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
IRD, UMR 152, F-31062 Toulouse 9, FranceUniv Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
Perio, Pierre
Ferry, Gilles
论文数: 0引用数: 0
h-index: 0
机构:
Inst Rech Servier, Biotechnol Pharmacol Mol & Cellulaire, F-78290 Croissy Sur Seine, FranceUniv Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
Ferry, Gilles
Moulharat, Natacha
论文数: 0引用数: 0
h-index: 0
机构:
Inst Rech Servier, Biotechnol Pharmacol Mol & Cellulaire, F-78290 Croissy Sur Seine, FranceUniv Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
Moulharat, Natacha
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Antoine, Mathias
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机构:
Gayon, Regis
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机构:
Boutin, Jean A.
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h-index:
机构:
Nepveu, Francoise
Reybier, Karine
论文数: 0引用数: 0
h-index: 0
机构:
Univ Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France
IRD, UMR 152, F-31062 Toulouse 9, FranceUniv Toulouse, UPS, UMR PHARMA DEV 152, F-31062 Toulouse 9, France