Diverse effects of natural antioxidants on cyclosporin cytotoxicity in rat renal tubular cells

doi:10.1093/ndt/gfh846

NDT Advance Access originally published online on April 26, 2005
Nephrology Dialysis Transplantation 2005 20(8):1551-1558; doi:10.1093/ndt/gfh846

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Original Article

Diverse effects of natural antioxidants on cyclosporin cytotoxicity in rat renal tubular cells

Patrizia Galletti¹, Chiara Iolanda Di Gennaro¹, Valentina Migliardi¹, Stefania Indaco¹, Fulvio Della Ragione¹, Caterina Manna¹, Paolo Chiodini², Giovanni Capasso³ and Vincenzo Zappia¹

¹ Department of Biochemistry and Biophysics ‘F. Cedrangolo’, ² Department of Medicine and Public Health and ³ Chair of Nephrology, Medical School, Second University of Naples, Naples, Italy

Correspondence and offprint requests to: Prof Patrizia Galletti, Department of Biochemistry and Biophysics "F. Cedrangolo", Via Costantinopoli, 16, 80138, Napoli, Italia. Tel. +39 0815665868, Fax: 39 0815667608, Email: patrizia.galletti{at}unina2.it

Background. As is well known, the use of the immunosuppressivedrug cyclosporin A (CsA) is partially restricted by its nephrotoxiceffects, which include early changes in haemodynamics followedby irreversible injuries to the renal tubules. Although themechanisms responsible for these side effects are poorly understood,an involvement of reactive oxygen species (ROS) has been suggested.In this study, we selected three natural antioxidants, resveratrol,hydroxytyrosol and vitamin E, on the basis of their scavengingcapabilities, and tested their protective effects against CsAtoxicity.

Methods. Immortalized rat tubular cells (RPTc) were used asthe model system. Cell viability was checked with trypan blueassay, and free radical formation was measured using the fluorescentprobe 2,7-dichlorofluorescein (DCF). We evaluated several oxidativestress parameters, including phospholipid peroxidation products,glutathione levels and oxygenase expression.

Results. Incubation of RPTc with 25 µM CsA induced a significantdecrease in cell viability paralleled by intracellular ROS formationand alterations in lipid peroxidation. There was also an imbalanceof glutathione redox state as well as upregulation of heme oxygenase-1(HO-1). The three antioxidants, at micromolar concentration,quantitatively prevented the ROS-activated DCF fluorescent signaland membrane lipid peroxidation. Both hydroxytyrosol and resveratrolstrengthened the CsA induction of HO-1 expression. Moreover,vitamin E and resveratrol counteracted CsA-induced changes inthe glutathione redox state via different mechanisms, whereashydroxytyrosol was completely ineffective. Similarly, CsA-dependentnephrotoxicity was prevented by vitamin E, while resveratrolonly exerted partial protection, and hydroxytyrosol showed noprotective effects.

Conclusion. Our results indicate that the diverse cytoprotectiveeffects of the antioxidants tested in these studies were notdirectly related to their scavenging capabilities. These findingsconfirm a key role for glutathione in protecting cells fromCsA-induced adverse effects and do not support a direct linkbetween CsA-mediated ROS generation and adverse renal effects.

Keywords: cyclosporin A; hydroxytyrosol; oxidative stress; proximal tubular cells; resveratrol; ROS; vitamin E

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