1. Açık Erişim@BUU
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Please use this identifier to cite or link to this item: http://hdl.handle.net/11452/29316
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dc.contributor.authorAçılan, Ceyda-
dc.contributor.authorAdıguzel, Zelal-
dc.contributor.authorRibeiro, Nádia-
dc.contributor.authorCorreia, Isabel-
dc.contributor.authorPessoa, João Costa-
dc.date.accessioned2022-11-02T06:41:47Z-
dc.date.available2022-11-02T06:41:47Z-
dc.date.issued2017-02-
dc.identifier.citationAçılan, C. vd. (2017). ''Synthesis, biological characterization and evaluation of molecular mechanisms of novel copper complexes as anticancer agents''. Biochimica et Biophysica Acta General Subjects, 1861(2), 218-134.en_US
dc.identifier.issn0304-4165-
dc.identifier.issn1872-8006-
dc.identifier.urihttps://doi.org/10.1016/j.bbagen.2016.10.014-
dc.identifier.urihttps://www.sciencedirect.com/science/article/pii/S0304416516303890-
dc.identifier.urihttp://hdl.handle.net/11452/29316-
dc.description.abstractBackground: To overcome the hurdles of cisplatin, majorly its toxicity and resistance, there has been extensive search for alternative anti-cancer metal-based compounds. Here, three Cu(II)-complexes, Cu(Sal-Gly)(phen), Cu(Sal-Gly)(pheamine), Cu(Sal-Gly)(phepoxy) are characterized for their interaction with DNA, cytotoxicity and mechanism of action. Methods: The binding ability of the complexes to Calf-Thymus DNA was evaluated by competition fluorescence studies with thiazole-orange, UV-Vis and circular dichroism spectroscopic titrations. Cytotoxicity was evaluated by MTT analysis. The DNA damage was analyzed through cleavage of supercoiled DNA via agarose gel-electrophoresis, and 8-oxo-guanidine and gamma H2AX staining in cells. Apoptosis was detected via DNA condensation/fragmentation, mitochondrial membrane potential, Annexin V staining and caspase 3/7 activity. Formation of reactive oxygen species was determined by DCFDA- and GSSG/GSH-analysis. Results: Binding constants to DNA were evaluated as 1.7 x 10(6) (Cu(Sal-Gly)(phen)), 2.5 x 10(6) (Cu(Sal-Gly)(pheamine)) and 3.2 x 10(5) (Cu(Sal-Gly)(phepoxy)). All compounds induced DNA damage. Apoptosis was the main form of cell death. There was an increase in ROS, which is most likely responsible for the observed DNA-damage. Although the compounds were cytotoxic to all tested cancer cell lines, only Cu(Sal-Gly)(pheamine) displayed significantly lower toxicity towards non-cancer cells, its associated phenotypes differing from the other two Cu-complexes. Thus, Cu(Sal-Gly)(pheamine) was further assayed for molecular changes in response to drug treatment using a custom designed RT-qPCR array. Results showed that Harakiri was significantly upregulated. Presence of p53 was not required for apoptosis in response to Cu-complexes. Conclusions and general significance: These Cu-complexes, namely Cu(Sal-Gly)(pheamine), may be considered promising anticancer agents with activity in cancer cells even with deficient p53 status.en_US
dc.description.sponsorshipPortuguese Foundation for Science and Technology UID/QUI/00100/2013en_US
dc.description.sponsorshipIST-UTL Center of the Portuguese Mass Spectrometry Networks REM2013 - RECI/QEQ-QIN/0189/2012en_US
dc.language.isoenen_US
dc.publisherElsevieren_US
dc.rightsinfo:eu-repo/semantics/closedAccessen_US
dc.subjectBiochemistry & molecular biologyen_US
dc.subjectBiophysicsen_US
dc.subjectCopper complexesen_US
dc.subjectSchiff base compoundsen_US
dc.subjectPhenanthrolineen_US
dc.subjectInteractions with DNAen_US
dc.subjectAnti-cancer drugsen_US
dc.subjectMechanism of cytotoxicity of Cu-compoundsen_US
dc.subjectCells in-vitroen_US
dc.subjectSalicylideneamino acidato complexesen_US
dc.subjectHuman cancer-cellsen_US
dc.subjectDna-bindingen_US
dc.subjectHeterocyclic basesen_US
dc.subjectCrystal-structuresen_US
dc.subjectCleavage activityen_US
dc.subjectTopoisomerase inhibitionen_US
dc.subjectChemical nucleasesen_US
dc.subjectOxidative stressen_US
dc.subject.meshA549 cellsen_US
dc.subject.meshAnimalsen_US
dc.subject.meshAnnexin A5en_US
dc.subject.meshAntineoplastic agentsen_US
dc.subject.meshApoptosisen_US
dc.subject.meshCaspase 3en_US
dc.subject.meshCaspase 7en_US
dc.subject.meshCattleen_US
dc.subject.meshCell Lineen_US
dc.subject.meshTumoren_US
dc.subject.meshCopperen_US
dc.subject.meshDNAen_US
dc.subject.meshDNA damageen_US
dc.subject.meshDNA fragmentationen_US
dc.subject.meshHCT116 cellsen_US
dc.subject.meshHeLa cellsen_US
dc.subject.meshHumansen_US
dc.subject.meshMembrane potentialen_US
dc.subject.meshMitochondrialen_US
dc.subject.meshReactive oxygen speciesen_US
dc.subject.meshTumor suppressor protein p53en_US
dc.subject.meshUp-regulatioen_US
dc.titleSynthesis, biological characterization and evaluation of molecular mechanisms of novel copper complexes as anticancer agentsen_US
dc.typeArticleen_US
dc.identifier.wos000392680200021tr_TR
dc.identifier.scopus2-s2.0-84999143653tr_TR
dc.relation.tubitakTÜBITAKtr_TR
dc.relation.publicationcategoryMakale - Uluslararası Hakemli Dergitr_TR
dc.contributor.departmentUludağ Üniversitesi/Fen-Edebiyet Fakültesi/Biyoloji Bölümü.tr_TR
dc.contributor.departmentUludağ Üniversitesi/Tıp Fakültesi/Tıbbi Biyokimya Anabilim Dalı.tr_TR
dc.contributor.orcid0000-0002-3781-6834tr_TR
dc.identifier.startpage218tr_TR
dc.identifier.endpage234tr_TR
dc.identifier.volume1861tr_TR
dc.identifier.issue2tr_TR
dc.relation.journalBiochimica et Biophysica Acta General Subjectsen_US
dc.contributor.buuauthorCevatemre, Buse-
dc.contributor.buuauthorKarakaş, Didem-
dc.contributor.buuauthorUlukaya, Engin-
dc.contributor.researcheridAHD-2050-2022tr_TR
dc.contributor.researcheridL-6682-2018tr_TR
dc.contributor.researcheridK-5792-2018tr_TR
dc.relation.collaborationYurt dışıtr_TR
dc.relation.collaborationYurt içitr_TR
dc.identifier.pubmed27773706tr_TR
dc.subject.wosBiochemistry & molecular biologyen_US
dc.subject.wosBiophysicsen_US
dc.indexed.wosSCIEen_US
dc.indexed.scopusScopusen_US
dc.indexed.pubmedPubMeden_US
dc.wos.quartileQ2 (Biochemistry & molecular biology)en_US
dc.wos.quartileQ1 (Biophysics)en_US
dc.contributor.scopusid55693788600tr_TR
dc.contributor.scopusid56422040600tr_TR
dc.contributor.scopusid6602927353tr_TR
dc.subject.scopusComplex; Viscometry; Schiff Basesen_US
dc.subject.emtreeAntineoplastic agenten_US
dc.subject.emtreeCaspase 3en_US
dc.subject.emtreeCaspase 7en_US
dc.subject.emtreeCopper complexen_US
dc.subject.emtreeHistone H2AXen_US
dc.subject.emtreeProtein p53en_US
dc.subject.emtreeReactive oxygen metaboliteen_US
dc.subject.emtreeAntineoplastic agenten_US
dc.subject.emtreeCalf thymus DNAen_US
dc.subject.emtreeCopperen_US
dc.subject.emtreeDNAen_US
dc.subject.emtreeLipocortin 5en_US
dc.subject.emtreeApoptosisen_US
dc.subject.emtreeArticleen_US
dc.subject.emtreeCancer cell lineen_US
dc.subject.emtreeControlled studyen_US
dc.subject.emtreeDNA damageen_US
dc.subject.emtreeDNA fragmentationen_US
dc.subject.emtreeDouble stranded DNA breaken_US
dc.subject.emtreeDrug cytotoxicityen_US
dc.subject.emtreeDrug DNA interactionen_US
dc.subject.emtreeDrug structureen_US
dc.subject.emtreeDrug synthesisen_US
dc.subject.emtreeMitochondrial membrane potentialen_US
dc.subject.emtreePriority journalen_US
dc.subject.emtreeA-549 cell lineen_US
dc.subject.emtreeAnimalen_US
dc.subject.emtreeBovineen_US
dc.subject.emtreeChemistryen_US
dc.subject.emtreeDrug effectsen_US
dc.subject.emtreeHCT 116 cell lineen_US
dc.subject.emtreeHeLa cell lineen_US
dc.subject.emtreeHumanen_US
dc.subject.emtreeMetabolismen_US
dc.subject.emtreeTumor cell lineen_US
dc.subject.emtreeUpregulationen_US
dc.subject.emtreeDNA cleavageen_US
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