en 34900143 <p style="text-align:justify"><span style="font-size:11pt"><span style="font-size:9.5pt">Background:</span><span style="font-size:10.0pt"> Ovarian cancer is the leading cause of death caused by genital cancers. One of the most common treatments for this type of cancer is chemotherapy by cisplatin, which induces apoptosis in cancer cells. Apoptosis is a type of physiological cell death. Cisplatin chemotherapy usually has several side effects and cellular resistance to cisplatin is a common incidence. In order to overcome these problems, the use of combination therapies using natural substances has been considered. Fisetin is a flavonoid with anti-cancer activity which induces apoptosis</span><span style="font-size:10.0pt">. In this study, the apoptosis induced by cisplatin along with Fisetin in cisplatin-resistant ovarian cancer cell line (A2780) was investigated.</span></span></p> <p style="text-align:justify"><span style="font-size:11pt"><span style="font-size:9.5pt">Methods:</span><span style="font-size:10.0pt"> In the present experimental study, the effect of combined use of Fisetin and cisplatin on ovarian cancer cell lines (A2780) was investigated by using MTT assay. Cell death was also determined by DAPI, acridine orange/propidium iodide, and Annexin/PI assay. Apoptotic gene expression of <em>Bax</em>, <em>BCL-2</em>, <em>caspase 3</em>, and <em>caspase 9</em> was also assessed by real time PCR.</span></span></p> <p style="text-align:justify"><span style="font-size:11pt"><span style="font-size:9.5pt">Results:</span><span style="font-size:10.0pt"> The results of MTT assay indicated that the combined treatment of Fisetin and cisplatin effectively inhibits proliferation of A2780 cells. The results of DAPI staining showed that fragmentation of chromatin in cells occurred in the combined treatment. Acridine orange-propidium iodide staining and Annexin/PI staining showed an increase in the rate of apoptotic cells in cells under combined treatment. The results of the study regarding changes in gene expression also indicated that <em>Bax</em> pro-apoptotic gene expression and <em>BCL-2</em> anti-apoptotic gene expression increased in cells under treatment; moreover, gene expression of <em>caspases 3</em> and <em>9</em> significantly increased as well.</span></span></p> <p style="text-align:justify"><span style="font-size:11pt"><span style="font-size:9.5pt">Conclusion:</span><span style="font-size:10.0pt"> According to the findings of this study, the combined use of cisplatin and Fisetin increases the induction of apoptosis in cisplatin-resistant ovarian cancer cells (A2780); therefore, the combined use of cisplatin and Fisetin can be considered a promising </span><span style="font-size:10.0pt">strategy</span><span style="font-size:10.0pt"> in the treatment of ovarian cancer.</span></span></p> Apoptosis, Cisplatin, Fisetin, Ovarian neoplasms 176 182 https://www.ajmb.org/En/Article.aspx?id=40474 https://www.ajmb.org/PDF/En/FullText/40474.pdf SamiraJafarzadehDepartment of Biology, Mashhad branch, Islamic Azad University, Mashhad, Iran71803JavadBahararaResearch Center for Animal Development Applied of Biology, Mashhad branch, Islamic Azad University, Mashhad, Iran71804MaryamTehranipourDepartment of Biology, Mashhad branch, Islamic Azad University, Mashhad, Iran71805