TY - JOUR T1 - Redox-related Molecular Mechanism of Sensitizing Colon Cancer Cells to Camptothecin Analog SN38 JF - Anticancer Research JO - Anticancer Res SP - 5159 LP - 5170 DO - 10.21873/anticanres.14519 VL - 40 IS - 9 AU - BILIANA NIKOLOVA AU - SEVERINA SEMKOVA AU - IANA TSONEVA AU - ELENA STOYANOVA AU - PAVEL LEFTEROV AU - DESSISLAVA LAZAROVA AU - ZHIVKO ZHELEV AU - ICHIO AOKI AU - TATSUYA HIGASHI AU - RUMIANA BAKALOVA Y1 - 2020/09/01 UR - http://ar.iiarjournals.org/content/40/9/5159.abstract N2 - Background/Aim: The aim of this study was to elucidate the possibility of sensitizing colon cancer cells to the chemotherapeutic drug SN38 and investigate its mechanism of action after combined treatment with electroporation (EP). Materials and Methods: Cells were treated with SN38, EP and their combination for 24/48 h. The cell viability, actin cytoskeleton integrity, mitochondrial superoxide, hydroperoxides, total glutathione, phosphatidyl serine expression, DNA damages and expression of membrane ABC transporters were analyzed using conventional analytical tests. Results: The combination of EP and SN38 affected cell viability and cytoskeleton integrity. This effect was accompanied by: (i) high production of intracellular superoxide and hydroperoxides and depletion of glutathione; (ii) increased DNA damage and apoptotic/ferroptotic cell death; (iii) changes in the expression of membrane ABC transporters – up-regulation of SLCO1B1 and retention of SN38 in the cells. Conclusion: The anticancer effect of the combined treatment of SN38 and EP is related to changes in the redox-homeostasis of cancer cells, leading to cell death via apoptosis and/or ferroptosis. Thus, electroporation has a potential to increase the sensitivity of cancer cells to conventional anticancer therapy with SN38. ER -