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Artículo

A combined ligand and target-based virtual screening strategy to repurpose drugs as putrescine uptake inhibitors with trypanocidal activity

Llanos, Manuel A.; Alberca, Lucas NicolásIcon ; Ruiz, María DanielaIcon ; Sbaraglini, María L.; Miranda, Cristian GabrielIcon ; Pino Martínez, Agustina MaríaIcon ; Fraccaroli, Laura VirginiaIcon ; Carrillo, CarolinaIcon ; Alba Soto, Catalina DirneyIcon ; Gavernet, LucianaIcon ; Talevi, AlanIcon
Fecha de publicación: 12/2022
Editorial: Springer
Revista: Journal of Computer-Aided Molecular Design
ISSN: 0920-654X
Idioma: Inglés
Tipo de recurso: Artículo publicado
Clasificación temática:
Enfermedades Infecciosas; Bioquímica y Biología Molecular

Resumen

Chagas disease, also known as American trypanosomiasis, is a neglected tropical disease caused by the protozoa Trypanosoma cruzi, affecting nearly 7 million people only in the Americas. Polyamines are essential compounds for parasite growth, survival, and differentiation. However, because trypanosomatids are auxotrophic for polyamines, they must be obtained from the host by specific transporters. In this investigation, an ensemble of QSAR classifiers able to identify polyamine analogs with trypanocidal activity was developed. Then, a multi-template homology model of the dimeric polyamine transporter of T. cruzi, TcPAT12, was created with Rosetta, and then refined by enhanced sampling molecular dynamics simulations. Using representative snapshots extracted from the trajectory, a docking model able to discriminate between active and inactive compounds was developed and validated. Both models were applied in a parallel virtual screening campaign to repurpose known drugs as anti-trypanosomal compounds inhibiting polyamine transport in T. cruzi. Montelukast, Quinestrol, Danazol, and Dutasteride were selected for in vitro testing, and all of them inhibited putrescine uptake in biochemical assays, confirming the predictive ability of the computational models. Furthermore, all the confirmed hits proved to inhibit epimastigote proliferation, and Quinestrol and Danazol were able to inhibit, in the low micromolar range, the viability of trypomastigotes and the intracellular growth of amastigotes.
Palabras clave: CHAGAS DISEASE , DOCKING , MOLECULAR DYNAMICS , QSAR , TCPAT12 , VIRTUAL SCREENING
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info:eu-repo/semantics/restrictedAccess Excepto donde se diga explícitamente, este item se publica bajo la siguiente descripción: Creative Commons Attribution-NonCommercial-ShareAlike 2.5 Unported (CC BY-NC-SA 2.5)
Identificadores
URI: http://hdl.handle.net/11336/208733
URL: https://link.springer.com/10.1007/s10822-022-00491-0
DOI: http://dx.doi.org/10.1007/s10822-022-00491-0
Colecciones
Articulos(ICT - MILSTEIN)
Articulos de INST.DE CS. Y TECNOLOGIA "DR. CESAR MILSTEIN"
Articulos(IMPAM)
Articulos de INSTITUTO DE INVESTIGACIONES EN MICROBIOLOGIA Y PARASITOLOGIA MEDICA
Citación
Llanos, Manuel A.; Alberca, Lucas Nicolás; Ruiz, María Daniela; Sbaraglini, María L.; Miranda, Cristian Gabriel; et al.; A combined ligand and target-based virtual screening strategy to repurpose drugs as putrescine uptake inhibitors with trypanocidal activity; Springer; Journal of Computer-Aided Molecular Design; 37; 2; 12-2022; 75-90
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