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Por favor, use este identificador para citar o enlazar este ítem: https://hdl.handle.net/20.500.12008/43904 Cómo citar
Título: Selenosugars targeting the infective stage of Trypanosoma brucei with high selectivity
Autor: Dibello, Estefanía
Oddone, Natalia
Franco, Jaime
Illyés, Tünde-Zita
Medeiros Pereyra, Andrea Lourdes
Kiss, Attila
Hogye, Fanni
Kövér, Katalin E.
Szilágyi, László
Comini, Marcelo A.
Tipo: Artículo
Descriptores: SELENOGLUCOSIDOS, TRYPANOSOMA BRUCEI, MACROFAGOS, ESTRES OXIDATIVO
Fecha de publicación: 2024
Resumen: Earlier evidences showed that diglycosyl diselenides are active against the infective stage of African trypanosomes (top hits IC50 0.5 and 1.5 μM) but poorly selective (selectivity index <10). Here we extended the study to 33 new seleno-glycoconjugates with the aim to improve potency and selectivity. Three selenoglycosides and three glycosyl selenenylsulfides displayed IC50 against bloodstream Trypanosoma brucei in the sub-μM range (IC50 0.35–0.77 μM) and four of them showed an improved selectivity (selectivity index >38-folds vs. murine and human macrohages). For the glycosyl selenylsulfides, the anti-trypanosomal activity was not significantly influenced by the nature of the moiety attached to the sulfur atom. Except for a quinoline-, and to a minor extent a nitro-derivative, the most selective hits induced a rapid (within 60 min) and marked perturbation of the LMWTredox homeostasis. The formation of selenenylsulfide glycoconjugates with free thiols has been identified as a potential mechanism involved in this process.
EN: International Journal for Parasitology Drugs and Drug Resistance v.24, 2024. -- e100529
Citación: Dibello, E., Oddone, N., Franco, J. y otros. "Selenosugars targeting the infective stage of Trypanosoma brucei with high selectivity". International Journal for Parasitology Drugs and Drug Resistance [en línea] v.24, 2024, e100529. DOI: 10.1016/j.ijpddr.2024.100529
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