Your search keyword '"Zinc15"' showing total 3 results

1. Structure-Based Virtual Screening and In Vitro Evaluation of New Trypanosoma cruzi Cruzain Inhibitors

Author

Joaquín Cordero-Martínez, Verónica Alcántara-Farfán, Gildardo Rivera, Verónica Herrera-Mayorga, Francisco Reyes-Espinosa, Benjamín Nogueda-Torres, Edgar E. Lara-Ramírez, Charmina Aguirre-Alvarado, Karla Fabiola Chacón-Vargas, Lorena Rodríguez-Páez, and Virgilio Bocanegra-García

Subjects

0301 basic medicine, Chagas disease, Proteases, cruzain, Trypanosoma cruzi, Pharmacology, 01 natural sciences, Catalysis, Inorganic Chemistry, lcsh:Chemistry, 03 medical and health sciences, inhibitors, medicine, Physical and Theoretical Chemistry, Molecular Biology, IC50, lcsh:QH301-705.5, Spectroscopy, chemistry.chemical_classification, Virtual screening, biology, 010405 organic chemistry, Chemistry, Organic Chemistry, General Medicine, molecular docking, biology.organism_classification, medicine.disease, In vitro, 0104 chemical sciences, Computer Science Applications, Zinc15, 030104 developmental biology, Enzyme, lcsh:Biology (General), lcsh:QD1-999, Structure based

Abstract

Chagas disease (CD), or American trypanosomiasis, causes more than 10,000 deaths per year in the Americas. Current medical therapy for CD has low efficacy in the chronic phase of the disease and serious adverse effects, therefore, it is necessary to search for new pharmacological treatments. In this work, the ZINC15 database was filtered using the N-acylhydrazone moiety and a subsequent structure-based virtual screening was performed using the cruzain enzyme of Trypanosoma cruzi to predict new potential cruzain inhibitors. After a rational selection process, four compounds, Z2 (ZINC9873043), Z3 (ZINC9870651), Z5 (ZINC9715287), and Z6 (ZINC9861447), were chosen to evaluate their in vitro trypanocidal activity and enzyme inhibition. Compound Z5 showed the best trypanocidal activity against epimatigote (IC50 = 36.26 &plusmn, 9.9 &mu, M) and trypomastigote (IC50 = 166.21 &plusmn, 14.5 &mu, M and 185.1 &plusmn, 8.5 &mu, M on NINOA and INC-5 strains, respectively) forms of Trypanosoma cruzi. In addition, Z5 showed a better inhibitory effect on Trypanosoma cruzi proteases than S1 (STK552090, 8-chloro-N-(3-morpholinopropyl)-5H-pyrimido[5,4-b]-indol-4-amine), a known cruzain inhibitor. This study encourages the use of computational tools for the rational search for trypanocidal drugs.

Published

2019

2. Structure-Based Virtual Screening and In Vitro Evaluation of New

Author

Verónica, Herrera-Mayorga, Edgar E, Lara-Ramírez, Karla F, Chacón-Vargas, Charmina, Aguirre-Alvarado, Lorena, Rodríguez-Páez, Verónica, Alcántara-Farfán, Joaquín, Cordero-Martínez, Benjamín, Nogueda-Torres, Francisco, Reyes-Espinosa, Virgilio, Bocanegra-García, and Gildardo, Rivera

Subjects

Models, Molecular, cruzain, Trypanosoma cruzi, Protozoan Proteins, molecular docking, Crystallography, X-Ray, Trypanocidal Agents, Article, Molecular Docking Simulation, Cysteine Endopeptidases, Structure-Activity Relationship, inhibitors, Zinc15, Enzyme Inhibitors, Databases, Chemical

Abstract

Chagas disease (CD), or American trypanosomiasis, causes more than 10,000 deaths per year in the Americas. Current medical therapy for CD has low efficacy in the chronic phase of the disease and serious adverse effects; therefore, it is necessary to search for new pharmacological treatments. In this work, the ZINC15 database was filtered using the N-acylhydrazone moiety and a subsequent structure-based virtual screening was performed using the cruzain enzyme of Trypanosoma cruzi to predict new potential cruzain inhibitors. After a rational selection process, four compounds, Z2 (ZINC9873043), Z3 (ZINC9870651), Z5 (ZINC9715287), and Z6 (ZINC9861447), were chosen to evaluate their in vitro trypanocidal activity and enzyme inhibition. Compound Z5 showed the best trypanocidal activity against epimatigote (IC50 = 36.26 ± 9.9 μM) and trypomastigote (IC50 = 166.21 ± 14.5 μM and 185.1 ± 8.5 μM on NINOA and INC-5 strains, respectively) forms of Trypanosoma cruzi. In addition, Z5 showed a better inhibitory effect on Trypanosoma cruzi proteases than S1 (STK552090, 8-chloro-N-(3-morpholinopropyl)-5H-pyrimido[5,4-b]-indol-4-amine), a known cruzain inhibitor. This study encourages the use of computational tools for the rational search for trypanocidal drugs.

Published

2019

3. Structure-Based Virtual Screening and In Vitro Evaluation of New Trypanosoma cruzi Cruzain Inhibitors.

Author

Reyes-Espinosa, Francisco, Bocanegra-García, Virgilio, Rivera, Gildardo, Herrera-Mayorga, Verónica, Lara-Ramírez, Edgar E., Chacón-Vargas, Karla F., Nogueda-Torres, Benjamín, Rodríguez-Páez, Lorena, Alcántara-Farfán, Verónica, Cordero-Martínez, Joaquín, and Aguirre-Alvarado, Charmina

Subjects

*CHAGAS' disease, *TRYPANOSOMIASIS, *TRYPANOSOMA cruzi, *ENZYMES, *CHEMICALS

Abstract

Chagas disease (CD), or American trypanosomiasis, causes more than 10,000 deaths per year in the Americas. Current medical therapy for CD has low efficacy in the chronic phase of the disease and serious adverse effects; therefore, it is necessary to search for new pharmacological treatments. In this work, the ZINC15 database was filtered using the N-acylhydrazone moiety and a subsequent structure-based virtual screening was performed using the cruzain enzyme of Trypanosoma cruzi to predict new potential cruzain inhibitors. After a rational selection process, four compounds, Z2 (ZINC9873043), Z3 (ZINC9870651), Z5 (ZINC9715287), and Z6 (ZINC9861447), were chosen to evaluate their in vitro trypanocidal activity and enzyme inhibition. Compound Z5 showed the best trypanocidal activity against epimatigote (IC50 = 36.26 ± 9.9 μM) and trypomastigote (IC50 = 166.21 ± 14.5 μM and 185.1 ± 8.5 μM on NINOA and INC-5 strains, respectively) forms of Trypanosoma cruzi. In addition, Z5 showed a better inhibitory effect on Trypanosoma cruzi proteases than S1 (STK552090, 8-chloro-N-(3-morpholinopropyl)-5H-pyrimido[5,4-b]-indol-4-amine), a known cruzain inhibitor. This study encourages the use of computational tools for the rational search for trypanocidal drugs. [ABSTRACT FROM AUTHOR]

Published

2019