Non-peptidic Cruzain Inhibitors with Trypanocidal Activity Discovered by Virtual Screening and In Vitro Assay

A multi-step cascade strategy using integrated ligand- and target-based virtual screening methods was developed to select a small number of compounds from the ZINC database to be evaluated for trypanocidal activity. Winnowing the database to 23 selected compounds, 12 non-covalent binding cruzain inh...

Descripción completa

Detalles Bibliográficos
Autores principales: Wiggers, Helton J., Rocha, Josmar R., Fernandes, William B., Sesti-Costa, Renata, Carneiro, Zumira A., Cheleski, Juliana, da Silva, Albérico B. F., Juliano, Luiz, Cezari, Maria H. S., Silva, João S., McKerrow, James H., Montanari, Carlos A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3750009/
https://www.ncbi.nlm.nih.gov/pubmed/23991231
http://dx.doi.org/10.1371/journal.pntd.0002370
_version_ 1782477061472911360
author Wiggers, Helton J.
Rocha, Josmar R.
Fernandes, William B.
Sesti-Costa, Renata
Carneiro, Zumira A.
Cheleski, Juliana
da Silva, Albérico B. F.
Juliano, Luiz
Cezari, Maria H. S.
Silva, João S.
McKerrow, James H.
Montanari, Carlos A.
author_facet Wiggers, Helton J.
Rocha, Josmar R.
Fernandes, William B.
Sesti-Costa, Renata
Carneiro, Zumira A.
Cheleski, Juliana
da Silva, Albérico B. F.
Juliano, Luiz
Cezari, Maria H. S.
Silva, João S.
McKerrow, James H.
Montanari, Carlos A.
author_sort Wiggers, Helton J.
collection PubMed
description A multi-step cascade strategy using integrated ligand- and target-based virtual screening methods was developed to select a small number of compounds from the ZINC database to be evaluated for trypanocidal activity. Winnowing the database to 23 selected compounds, 12 non-covalent binding cruzain inhibitors with affinity values (K (i)) in the low micromolar range (3–60 µM) acting through a competitive inhibition mechanism were identified. This mechanism has been confirmed by determining the binding mode of the cruzain inhibitor Nequimed176 through X-ray crystallographic studies. Cruzain, a validated therapeutic target for new chemotherapy for Chagas disease, also shares high similarity with the mammalian homolog cathepsin L. Because increased activity of cathepsin L is related to invasive properties and has been linked to metastatic cancer cells, cruzain inhibitors from the same library were assayed against it. Affinity values were in a similar range (4–80 µM), yielding poor selectivity towards cruzain but raising the possibility of investigating such inhibitors for their effect on cell proliferation. In order to select the most promising enzyme inhibitors retaining trypanocidal activity for structure-activity relationship (SAR) studies, the most potent cruzain inhibitors were assayed against T. cruzi-infected cells. Two compounds were found to have trypanocidal activity. Using compound Nequimed42 as precursor, an SAR was established in which the 2-acetamidothiophene-3-carboxamide group was identified as essential for enzyme and parasite inhibition activities. The IC(50) value for compound Nequimed42 acting against the trypomastigote form of the Tulahuen lacZ strain was found to be 10.6±0.1 µM, tenfold lower than that obtained for benznidazole, which was taken as positive control. In addition, by employing the strategy of molecular simplification, a smaller compound derived from Nequimed42 with a ligand efficiency (LE) of 0.33 kcal mol(−1) atom(−1) (compound Nequimed176) is highlighted as a novel non-peptidic, non-covalent cruzain inhibitor as a trypanocidal agent candidate for optimization.
format Online
Article
Text
id pubmed-3750009
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-37500092013-08-29 Non-peptidic Cruzain Inhibitors with Trypanocidal Activity Discovered by Virtual Screening and In Vitro Assay Wiggers, Helton J. Rocha, Josmar R. Fernandes, William B. Sesti-Costa, Renata Carneiro, Zumira A. Cheleski, Juliana da Silva, Albérico B. F. Juliano, Luiz Cezari, Maria H. S. Silva, João S. McKerrow, James H. Montanari, Carlos A. PLoS Negl Trop Dis Research Article A multi-step cascade strategy using integrated ligand- and target-based virtual screening methods was developed to select a small number of compounds from the ZINC database to be evaluated for trypanocidal activity. Winnowing the database to 23 selected compounds, 12 non-covalent binding cruzain inhibitors with affinity values (K (i)) in the low micromolar range (3–60 µM) acting through a competitive inhibition mechanism were identified. This mechanism has been confirmed by determining the binding mode of the cruzain inhibitor Nequimed176 through X-ray crystallographic studies. Cruzain, a validated therapeutic target for new chemotherapy for Chagas disease, also shares high similarity with the mammalian homolog cathepsin L. Because increased activity of cathepsin L is related to invasive properties and has been linked to metastatic cancer cells, cruzain inhibitors from the same library were assayed against it. Affinity values were in a similar range (4–80 µM), yielding poor selectivity towards cruzain but raising the possibility of investigating such inhibitors for their effect on cell proliferation. In order to select the most promising enzyme inhibitors retaining trypanocidal activity for structure-activity relationship (SAR) studies, the most potent cruzain inhibitors were assayed against T. cruzi-infected cells. Two compounds were found to have trypanocidal activity. Using compound Nequimed42 as precursor, an SAR was established in which the 2-acetamidothiophene-3-carboxamide group was identified as essential for enzyme and parasite inhibition activities. The IC(50) value for compound Nequimed42 acting against the trypomastigote form of the Tulahuen lacZ strain was found to be 10.6±0.1 µM, tenfold lower than that obtained for benznidazole, which was taken as positive control. In addition, by employing the strategy of molecular simplification, a smaller compound derived from Nequimed42 with a ligand efficiency (LE) of 0.33 kcal mol(−1) atom(−1) (compound Nequimed176) is highlighted as a novel non-peptidic, non-covalent cruzain inhibitor as a trypanocidal agent candidate for optimization. Public Library of Science 2013-08-22 /pmc/articles/PMC3750009/ /pubmed/23991231 http://dx.doi.org/10.1371/journal.pntd.0002370 Text en © 2013 Wiggers et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Wiggers, Helton J.
Rocha, Josmar R.
Fernandes, William B.
Sesti-Costa, Renata
Carneiro, Zumira A.
Cheleski, Juliana
da Silva, Albérico B. F.
Juliano, Luiz
Cezari, Maria H. S.
Silva, João S.
McKerrow, James H.
Montanari, Carlos A.
Non-peptidic Cruzain Inhibitors with Trypanocidal Activity Discovered by Virtual Screening and In Vitro Assay
title Non-peptidic Cruzain Inhibitors with Trypanocidal Activity Discovered by Virtual Screening and In Vitro Assay
title_full Non-peptidic Cruzain Inhibitors with Trypanocidal Activity Discovered by Virtual Screening and In Vitro Assay
title_fullStr Non-peptidic Cruzain Inhibitors with Trypanocidal Activity Discovered by Virtual Screening and In Vitro Assay
title_full_unstemmed Non-peptidic Cruzain Inhibitors with Trypanocidal Activity Discovered by Virtual Screening and In Vitro Assay
title_short Non-peptidic Cruzain Inhibitors with Trypanocidal Activity Discovered by Virtual Screening and In Vitro Assay
title_sort non-peptidic cruzain inhibitors with trypanocidal activity discovered by virtual screening and in vitro assay
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3750009/
https://www.ncbi.nlm.nih.gov/pubmed/23991231
http://dx.doi.org/10.1371/journal.pntd.0002370
work_keys_str_mv AT wiggersheltonj nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT rochajosmarr nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT fernandeswilliamb nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT sesticostarenata nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT carneirozumiraa nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT cheleskijuliana nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT dasilvaalbericobf nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT julianoluiz nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT cezarimariahs nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT silvajoaos nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT mckerrowjamesh nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay
AT montanaricarlosa nonpeptidiccruzaininhibitorswithtrypanocidalactivitydiscoveredbyvirtualscreeningandinvitroassay

Ejemplares similares