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In vitro cytotoxicity evaluation of plastoquinone analogues against colorectal and breast cancers along with in silico insights

dc.contributor.coauthorSever, B.
dc.contributor.coauthorBayrak, N.
dc.contributor.coauthorYıldız, M.
dc.contributor.coauthorYıldırım, H.
dc.contributor.coauthorTateishi, H.
dc.contributor.coauthorOtsuka, M.
dc.contributor.coauthorFujita M.
dc.contributor.coauthorTuyun, A.F.
dc.contributor.departmentDepartment of Molecular Biology and Genetics
dc.contributor.kuauthorÇiftçi, Halil İbrahim
dc.contributor.kuprofileResearcher
dc.contributor.otherDepartment of Molecular Biology and Genetics
dc.contributor.schoolcollegeinstituteCollege of Sciences
dc.date.accessioned2024-11-09T13:27:27Z
dc.date.issued2022
dc.description.abstractColorectal cancer (CRC) and breast cancer are leading causes of death globally, due to significant challenges in detection and management. The late-stage diagnosis and treatment failures require the discovery of potential anticancer agents to achieve a satisfactory therapeutic effect. We have previously reported a series of plastoquinone analogues to understand their cytotoxic profile. Among these derivatives, three of them (AQ-11, AQ-12, and AQ-15) were selected by the National Cancer Institute (NCI) to evaluate their in vitro antiproliferative activity against a panel of 60 human tumor cell lines. AQ-12 exhibited significant antiproliferative activity against HCT-116 CRC and MCF-7 breast cancer cells at a single dose and further five doses. MTT assay was also performed for AQ-12 at different concentrations against these two cells, implying that AQ-12 exerted notable cytotoxicity toward HCT-116 (IC50 = 5.11 ± 2.14 ?M) and MCF-7 (IC50 = 6.06 ± 3.09 ?M) cells in comparison with cisplatin (IC50 = 23.68 ± 6.81 ?M and 19.67 ± 5.94 ?M, respectively). This compound also augmented apoptosis in HCT-116 (62.30%) and MCF-7 (64.60%) cells comparable to cisplatin (67.30% and 78.80%, respectively). Molecular docking studies showed that AQ-12 bound to DNA, forming hydrogen bonding through the quinone scaffold. In silico pharmacokinetic determinants indicated that AQ-12 demonstrated drug-likeness with a remarkable pharmacokinetic profile for future mechanistic anti-CRC and anti-breast cancer activity studies.
dc.description.fulltextYES
dc.description.indexedbyWoS
dc.description.indexedbyScopus
dc.description.indexedbyPubMed
dc.description.issue10
dc.description.openaccessYES
dc.description.publisherscopeInternational
dc.description.sponsoredbyTubitakEuTÜBİTAK
dc.description.sponsoredbyTubitakEuEU
dc.description.sponsorshipScientific Research Projects Coordination Unit of Istanbul University
dc.description.sponsorshipScientific and Technological Research Council of Turkey (TÜBİTAK)
dc.description.sponsorship2236 CoCirculation2
dc.description.sponsorshipEuropean Union (EU)
dc.description.sponsorshipHorizon 2020
dc.description.versionPublisher version
dc.description.volume15
dc.formatpdf
dc.identifier.doi10.3390/ph15101266
dc.identifier.embargoNO
dc.identifier.filenameinventorynoIR04036
dc.identifier.issn1424-8247
dc.identifier.linkhttps://doi.org/10.3390/ph15101266
dc.identifier.quartileQ2
dc.identifier.scopus2-s2.0-85140916394
dc.identifier.urihttps://hdl.handle.net/20.500.14288/3516
dc.identifier.wos875037900001
dc.keywordsApoptosis
dc.keywordsBreast cancer
dc.keywordsColorectal cancer
dc.keywordsCytotoxicity
dc.keywordsDNA binding
dc.keywordsGrowth inhibition
dc.keywordsNCI-60
dc.keywordsPharmacokinetic determinants
dc.keywordsPlastoquinone
dc.languageEnglish
dc.publisherMultidisciplinary Digital Publishing Institute (MDPI)
dc.relation.grantnoFBA-2016-20662
dc.relation.grantno121C063
dc.relation.urihttp://cdm21054.contentdm.oclc.org/cdm/ref/collection/IR/id/10915
dc.sourcePharmaceuticals
dc.subjectPharmacology and pharmacy
dc.titleIn vitro cytotoxicity evaluation of plastoquinone analogues against colorectal and breast cancers along with in silico insights
dc.typeJournal Article
dspace.entity.typePublication
local.contributor.authorid0000-0002-9796-7669
local.contributor.kuauthorÇiftçi, Halil İbrahim
relation.isOrgUnitOfPublicationaee2d329-aabe-4b58-ba67-09dbf8575547
relation.isOrgUnitOfPublication.latestForDiscoveryaee2d329-aabe-4b58-ba67-09dbf8575547

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