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Titre: Oxidative stress as an underling mechanism of anticancer drugs cytotoxicity on human red blood cells' membrane
Auteur(s): MAMERI, Amal
Bournine, Lamine
Mouni, Lotfi
Bensalem, Sihem
Iguer-Ouada, Mokrane
Mots-clés: Anticancer drugs
Red blood cells
Membrane cytotoxicity
Oxidative stress
Methemoglobin
Lipid peroxidation
Date de publication: 2-fév-2021
Editeur: Université de Bouira
Référence bibliographique: Toxicology in Vitro ,Volume 72, pages 105106
Résumé: The aim of this study is to investigate the direct in vitro effects of anticancer drugs on red blood cells (RBCs) and to explore the underlying mechanism, mainly by measuring RBCs oxidative stress (OS) status. After RBCs direct contact with fourteen (14) anticancer drugs, several parameters were assessed including: cellular turbidity, methemoglobin (metHb) generation, released Hb and Hb stability. Moreover, intracellular Hb, considered as new molecular target of anticancer drugs, was quantified inside RBCs. MDA level, the main biomarker of OS, was simultaneously measured. The cellular turbidity reveled severe (docetaxel “TXT”, 0.03 ± 0.002), moderate (methotrexate “MTX”, 0.49 ± 0.009), or none (5-fluorouracil “5-FU”, 0.76 ± 0.029) membrane cytotoxicity (MC). An inverse relationship between cell concentration, released Hb and metHb content was obtained. High metHb generation, revealing intense OS, was also mostly expressed in paclitaxel “TXL” and etoposide “VP16”. Further, epirubicin “EPI” and “TXT” induced important oxidation of membrane lipids with 0.32 ± 0.014 and 0.26 ± 0.004, respectively. Also, MTX (0.17 ± 0.006) and doxorubicin “DOX” (0.32 ± 0.034) affected significantly Hb stability by a direct contact with molecule. These findings demonstrated that anticancer drugs have the ability to induce membrane damages by the exacerbation of OS through membrane lipid peroxidation and Hb oxidation even inside RBCs.
URI/URL: http://dspace.univ-bouira.dz:8080/jspui/handle/123456789/11172
Collection(s) :Articles

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