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dc.date.accessioned 2023-06-16T16:56:05Z
dc.date.available 2023-06-16T16:56:05Z
dc.date.issued 2023
dc.identifier.uri http://sedici.unlp.edu.ar/handle/10915/154460
dc.description.abstract Organoruthenium pyrithione (1-hydroxypyridine-2-thione) complexes have been shown in our recent studies to be a promising family of compounds for development of new anticancer drugs. The complex [(n⁶-p-cymene)Ru(pyrithionato)(pta)]PF₆ contains phosphine ligand pta (1,3,5- triaza-7-phosphaadamantane) as a functionality that improves the stability of the complex and its aqueous solubility. Here, we report our efforts to find pta alternatives and discover new structural elements to improve the biological properties of ruthenium anticancer drugs. The pta ligand was replaced by a selection of phosphine, phosphite, and arsine ligands to identify new functionalities, leading to improvement in inhibitory potency towards enzyme glutathione S-transferase. In addition, cytotoxicity in breast, bone, and colon cancers was investigated. en
dc.language en es
dc.subject Ruthenium es
dc.subject Pyrithione es
dc.subject Phosphines es
dc.subject Anticancer activity es
dc.subject Glutathione S-transferase es
dc.title Exploring pta alternatives in the development of ruthenium–arene anticancer compounds en
dc.type Articulo es
sedici.identifier.other https://doi.org/10.3390/molecules28062499 es
sedici.identifier.issn 1420-3049 es
sedici.creator.person Kljun, Jakob es
sedici.creator.person Rebernik, Mihaela es
sedici.creator.person Balsa, Lucía Mariana es
sedici.creator.person Kladnik, Jerneja es
sedici.creator.person Rapuš, Uroš es
sedici.creator.person Trobec, Tomaž es
sedici.creator.person Sepčić, Kristina es
sedici.creator.person Frangež, Robert es
sedici.creator.person León, Ignacio Esteban es
sedici.creator.person Turel, Iztok es
sedici.subject.materias Química es
sedici.description.fulltext true es
mods.originInfo.place Centro de Química Inorgánica es
sedici.subtype Articulo es
sedici.rights.license Creative Commons Attribution 4.0 International (CC BY 4.0)
sedici.rights.uri http://creativecommons.org/licenses/by/4.0/
sedici.description.peerReview peer-review es
sedici.relation.journalTitle Molecules es
sedici.relation.journalVolumeAndIssue vol. 28, no. 6 es


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Creative Commons Attribution 4.0 International (CC BY 4.0) Excepto donde se diga explícitamente, este item se publica bajo la siguiente licencia Creative Commons Attribution 4.0 International (CC BY 4.0)