Mixed copper(ii)-phenanthroline complexes induce cell death of ovarian cancer cells by evoking the unfolded protein response

• Authors: MORÁŇ Lukáš; PIVETTA Tiziana; MASURI Sebastiano; VAŠÍČKOVÁ Kateřina; WALTER Franziska; PREHN Jochen; ELKALAF Moustafa; TRNKA Jan; HAVEL Josef; VAŇHARA Petr
• Year of publication: 2019
• Type: Article in Periodical
• Magazine / Source: Metallomics
• MU Faculty or unit: Faculty of Medicine
• web: http://dx.doi.org/10.1039/c9mt00055k
• Doi: https://doi.org/10.1039/c9mt00055k
• Keywords: ENDOPLASMIC-RETICULUM STRESS; LIGAND COPPER(II) COMPLEXES; DNA CLEAVAGE; TUMOR-CELLS; CISPLATIN; 1_10-PHENANTHROLINE; PHENANTHROLINE; APOPTOSIS; BINDING; CYTOTOXICITY
• Description: There is an ongoing need for the development of new cancer therapeutics that combine high cytotoxic efficiency with low side effects, and also override resistance to the first-line chemotherapeutics. Copper(II)–phenanthroline complexes are promising compounds that were shown previously to induce an immediate cytotoxic response over a panel of tumor cell lines in vitro. The molecular mechanism, however, remained unresolved. In this work we performed a thorough study of the copper(II)–phenanthroline complexes containing different imidazolidine-2-thione ligands in ovarian cancer cells, and revealed that these complexes induce endoplasmic reticulum (ER) stress and subsequently cell death mediated by the unfolded protein response. Alleviation of the ER-stress by tauroursodeoxycholic acid (TUDCA) attenuated the cytotoxic effects. In summary, we have identified a novel, ER-dependent, molecular mechanism mediating cytotoxic effects of copper(II)–phenanthroline complexes.

Related projects

• Centrum analýz a modelování tkání a orgánů
• Zdroje pro tkáňové inženýrství 9