The antidote effect of quinone oxidoreductase 2 inhibitor against paraquat-induced toxicity in vitro and in vivo |
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| Authors: | Elzbieta Janda Maddalena Parafati Serafina Aprigliano Cristina Carresi Valeria Visalli Iolanda Sacco Domenica Ventrice Tiziana Mega Nuria Vadalá Stefano Rinaldi Vincenzo Musolino Ernesto Palma Santo Gratteri Domenicantonio Rotiroti Vincenzo Mollace |
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| Affiliation: | 1.Department of Health Sciences, University ‘Magna Graecia’, Catanzaro, Italy;2.Center of Excellence for Food Toxicology (CETA), ARPACAL, Catanzaro, Italy;3.Salus Research Institute, Marinella di Bruzzano, Italy;4.Department of Experimental and Clinical Medicine, University ‘Magna Graecia’, Catanzaro, Italy;5.San Raffaele Pisana, IRCCS, Rome, Italy |
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| Abstract: | BACKGROUND AND PURPOSEThe mechanisms of paraquat (PQ)-induced toxicity are poorly understood and PQ poisoning is often fatal due to a lack of effective antidotes. In this study we report the effects of N-[2-(2-methoxy-6H-dipyrido{2,3-a:3,2-e}pyrrolizin-11-yl)ethyl]-2-furamide (NMDPEF), a melatonin-related inhibitor of quinone oxidoreductase2 (QR2) on the toxicity of PQ in vitro & in vivo.EXPERIMENTAL APPROACHPrevention of PQ-induced toxicity was tested in different cells, including primary pneumocytes and astroglial U373 cells. Cell death and reactive oxygen species (ROS) were analysed by flow cytometry and fluorescent probes. QR2 silencing was achieved by lentiviral shRNAs. PQ (30 mg·kg−1) and NMDPEF were administered i.p. to Wistar rats and animals were monitored for 28 days. PQ toxicity in the substantia nigra (SN) was tested by a localized microinfusion and electrocorticography. QR2 activity was measured by fluorimetry of N-benzyldihydronicotinamide oxidation.KEY RESULTSNMDPEF potently antagonized non-apoptotic PQ-induced cell death, ROS generation and inhibited cellular QR2 activity. In contrast, the cytoprotective effect of melatonin and apocynin was limited and transient compared with NMDPEF. Silencing of QR2 attenuated PQ-induced cell death and reduced the efficacy of NMDPEF. Significantly, NMDPEF (4.5 mg·kg−1) potently antagonized PQ-induced systemic toxicity and animal mortality. Microinfusion of NMDPEF into SN prevented severe behavioural and electrocortical effects of PQ which correlated with inhibition of malondialdehyde accumulation in cells and tissues.CONCLUSIONS AND IMPLICATIONSNMDPEF protected against PQ-induced toxicity in vitro and in vivo, suggesting a key role for QR2 in the regulation of oxidative stress.LINKED ARTICLEThis article is commented on by Baltazar et al., pp. 44–45 of this issue. To view this commentary visit http://dx.doi.org/10.1111/j.1476-5381.2012.02017.x |
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| Keywords: | NQO2 oxidative stress ROS paraquat pesticides astrocytes mammary epithelial cells substantia nigra electrocorticogram |
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