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  2. Johannes Gutenberg-Universität Mainz
  3. DFG-OA-Publizieren (2012 - 2017)
Please use this identifier to cite or link to this item: http://doi.org/10.25358/openscience-8050
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dc.contributor.authorSaaed, Mohamed-
dc.contributor.authorJacob, Stefan-
dc.contributor.authorSandjo, Louis P.-
dc.contributor.authorSugimoto, Yoshikazu-
dc.contributor.authorKhalid, Hassan E.-
dc.contributor.authorOpatz, Till-
dc.contributor.authorThines, Eckhard-
dc.contributor.authorEfferth, Thomas-
dc.date.accessioned2022-10-17T07:24:25Z-
dc.date.available2022-10-17T07:24:25Z-
dc.date.issued2015
dc.identifier.urihttps://openscience.ub.uni-mainz.de/handle/20.500.12030/8065-
dc.description.abstractMultidrug resistance is a prevailing phenomenon leading to chemotherapy treatment failure in cancer patients. In the current study two known cytotoxic pseudoguaianolide sesquiterpene lactones; neoambrosin (1) and damsin (2) that circumvent MDR were identified. The two cytotoxic compounds were isolated using column chromatography, characterized using 1D and 2D NMR, MS, and compared with literature values. The isolated compounds were investigated for their cytotoxic potential using resazurin assays and thereafter confirmed with immunoblotting and in silico studies. MDR cells overexpressing ABC transporters (P-glycoprotein, BCRP, ABCB5) did not confer cross-resistance toward (1) and (2), indicating that these compounds are not appropriate substrates for any of the three ABC transporters analyzed. Resistance mechanisms investigated also included; the loss of the functions of the TP53 and the mutated EGFR. The HCT116 p53-/- cells were sensitive to 1 but resistant to 2. It was interesting to note that resistant cells transfected with oncogenic ΔEGFR exhibited hypersensitivity CS toward (1) and (2) (degrees of resistances were 0.18 and 0.15 for (1) and (2), respectively). Immunoblotting and in silico analyses revealed that 1 and 2 silenced c-Src kinase activity. It was hypothesized that inhibition of c-Src kinase activity may explain CS in EGFR-transfected cells. In conclusion, the significant cytotoxicity of 1 and 2 against different drug-resistant tumor cell lines indicate that they may be promising candidates to treat refractory tumors.en_GB
dc.description.sponsorshipDFG, Open Access-Publizieren Universität Mainz / Universitätsmedizinde
dc.language.isoengde
dc.rightsCC BY*
dc.rights.urihttps://creativecommons.org/licenses/by/4.0/*
dc.subject.ddc570 Biowissenschaftende_DE
dc.subject.ddc570 Life sciencesen_GB
dc.titleCytotoxicity of the sesquiterpene lactones neoambrosin and damsin from ambrosia maritima against multidrug-resistant cancer cellsen_GB
dc.typeZeitschriftenaufsatzde
dc.identifier.doihttp://doi.org/10.25358/openscience-8050-
jgu.type.dinitypearticleen_GB
jgu.type.versionPublished versionde
jgu.type.resourceTextde
jgu.organisation.departmentFB 09 Chemie, Pharmazie u. Geowissensch.de
jgu.organisation.departmentFB 10 Biologiede
jgu.organisation.number7950-
jgu.organisation.number7970-
jgu.organisation.nameJohannes Gutenberg-Universität Mainz-
jgu.rights.accessrightsopenAccess-
jgu.journal.titleFrontiers in pharmacologyde
jgu.journal.volume6de
jgu.pages.alternativeArt. 267de
jgu.publisher.year2015-
jgu.publisher.nameFrontiers Mediade
jgu.publisher.placeLausannede
jgu.publisher.urihttp://dx.doi.org/10.3389/fphar.2015.00267de
jgu.publisher.issn1663-9812de
jgu.organisation.placeMainz-
jgu.subject.ddccode570de
opus.date.modified2017-05-12T09:22:02Z
opus.subject.dfgcode00-000
opus.organisation.stringFB 09: Chemie, Pharmazie und Geowissenschaften: Institut für Organische Chemiede_DE
opus.organisation.stringFB 09: Chemie, Pharmazie und Geowissenschaften: Institut für Pharmaziede_DE
opus.organisation.stringFB 10: Biologie: Institut für Mikrobiologie und Weinforschungde_DE
opus.identifier.opusid52623
opus.institute.number0905
opus.institute.number0908
opus.institute.number1008
opus.metadataonlyfalse
opus.type.contenttypeKeinede_DE
opus.type.contenttypeNoneen_EN
opus.affiliatedOpatz, Till
opus.affiliatedThines, Eckhard
opus.affiliatedEfferth, Thomas
jgu.publisher.doi10.3389/fphar.2015.00267de
jgu.organisation.rorhttps://ror.org/023b0x485-
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