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dc.creatorMihajlović, Ekatarina
dc.creatorBiancalana, Lorenzo
dc.creatorJelača, Sanja
dc.creatorChiaverini, Lorenzo
dc.creatorDojčinović, Biljana
dc.creatorDunđerović, Duško
dc.creatorZacchini, Stefano
dc.creatorMijatović, Sanja
dc.creatorMaksimović-Ivanić, Danijela
dc.creatorMarchetti, Fabio
dc.date.accessioned2024-05-13T10:54:46Z
dc.date.available2900-01-01
dc.date.issued2024
dc.identifier.issn0022-2623
dc.identifier.urihttp://radar.ibiss.bg.ac.rs/handle/123456789/6701
dc.description.abstractFETPY, an organo-diiron(I) complex, showed strong cytotoxicity across a panel of human and mouse cancer cell lines, combined with an outstanding selectivity compared to nonmalignant cells. Enhanced iron uptake in aggressive, low-differentiated cell lines, caused membrane lipid peroxidation, which resulted in ferroptosis in human ovarian cancer cells. FETPY induced significant morphological changes in murine B16–F1 and B16–F10 melanoma cells, leading to senescence and/or trans-differentiation into Schwann-like cells, thus significantly reducing their tumorigenic potential. Additionally, FETPY substantially suppressed tumor growth in low- and high-grade syngeneic melanoma models when administered in a therapeutic regimen. FETPY is featured by satisfactory water solubility (millimolar range), an amphiphilic character (Log Pow = −0.17), and excellent stability in a biological medium (DMEM). These important requisites for drug development are rarely met in iron complexes investigated so far as possible anticancer agents. Overall, FETPY holds promise as a safe and potent targeted antitumor agent.sr
dc.language.isoensr
dc.publisherAmerican Chemical Societysr
dc.relationinfo:eu-repo/grantAgreement/MESTD/inst-2020/200007/RS//sr
dc.relationFondi di Ateneo 2020sr
dc.rightsrestrictedAccesssr
dc.sourceJournal of Medicinal Chemistrysr
dc.titleFETPY: a Diiron(I) Thio–Carbyne Complex with Prominent Anticancer Activity In Vitro and In Vivosr
dc.typearticlesr
dc.rights.licenseARRsr
dc.rights.holder© 2024 American Chemical Societysr
dc.citation.issue9
dc.citation.volume67
dc.identifier.doi10.1021/acs.jmedchem.4c00377
dc.identifier.pmid38639401
dc.identifier.scopus2-s2.0-85191182533
dc.identifier.wos001226322400001
dc.citation.spage7553
dc.citation.epage7568
dc.type.versionpublishedVersionsr
dc.citation.rankM21a~


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