Perturbation of the Dimer Interface of Triosephosphate Isomerase and its Effect on Trypanosoma cruzi

BACKGROUND: Chagas disease affects around 18 million people in the American continent. Unfortunately, there is no satisfactory treatment for the disease. The drugs currently used are not specific and exert serious toxic effects. Thus, there is an urgent need for drugs that are effective. Looking for...

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Autores principales: Olivares-Illana, Vanesa, Rodríguez-Romero, Adela, Becker, Ingeborg, Berzunza, Miriam, García, Juventino, Pérez-Montfort, Ruy, Cabrera, Nallely, López-Calahorra, Francisco, de Gómez-Puyou, Marieta Tuena, Gómez-Puyou, Armando
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2007
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2041813/
https://www.ncbi.nlm.nih.gov/pubmed/17989778
http://dx.doi.org/10.1371/journal.pntd.0000001
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author Olivares-Illana, Vanesa
Rodríguez-Romero, Adela
Becker, Ingeborg
Berzunza, Miriam
García, Juventino
Pérez-Montfort, Ruy
Cabrera, Nallely
López-Calahorra, Francisco
de Gómez-Puyou, Marieta Tuena
Gómez-Puyou, Armando
author_facet Olivares-Illana, Vanesa
Rodríguez-Romero, Adela
Becker, Ingeborg
Berzunza, Miriam
García, Juventino
Pérez-Montfort, Ruy
Cabrera, Nallely
López-Calahorra, Francisco
de Gómez-Puyou, Marieta Tuena
Gómez-Puyou, Armando
author_sort Olivares-Illana, Vanesa
collection PubMed
description BACKGROUND: Chagas disease affects around 18 million people in the American continent. Unfortunately, there is no satisfactory treatment for the disease. The drugs currently used are not specific and exert serious toxic effects. Thus, there is an urgent need for drugs that are effective. Looking for molecules to eliminate the parasite, we have targeted a central enzyme of the glycolytic pathway: triosephosphate isomerase (TIM). The homodimeric enzyme is catalytically active only as a dimer. Because there are significant differences in the interface of the enzymes from the parasite and humans, we searched for small molecules that specifically disrupt contact between the two subunits of the enzyme from Trypanosoma cruzi but not those of TIM from Homo sapiens (HTIM), and tested if they kill the parasite. METHODOLOGY/PRINCIPAL FINDINGS: Dithiodianiline (DTDA) at nanomolar concentrations completely inactivates recombinant TIM of T. cruzi (TcTIM). It also inactivated HTIM, but at concentrations around 400 times higher. DTDA was also tested on four TcTIM mutants with each of its four cysteines replaced with either valine or alanine. The sensitivity of the mutants to DTDA was markedly similar to that of the wild type. The crystal structure of the TcTIM soaked in DTDA at 2.15 Å resolution, and the data on the mutants showed that inactivation resulted from alterations of the dimer interface. DTDA also prevented the growth of Escherichia coli cells transformed with TcTIM, had no effect on normal E. coli, and also killed T. cruzi epimastigotes in culture. CONCLUSIONS/SIGNIFICANCE: By targeting on the dimer interface of oligomeric enzymes from parasites, it is possible to discover small molecules that selectively thwart the life of the parasite. Also, the conformational changes that DTDA induces in the dimer interface of the trypanosomal enzyme are unique and identify a region of the interface that could be targeted for drug discovery.
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spelling pubmed-20418132007-11-07 Perturbation of the Dimer Interface of Triosephosphate Isomerase and its Effect on Trypanosoma cruzi Olivares-Illana, Vanesa Rodríguez-Romero, Adela Becker, Ingeborg Berzunza, Miriam García, Juventino Pérez-Montfort, Ruy Cabrera, Nallely López-Calahorra, Francisco de Gómez-Puyou, Marieta Tuena Gómez-Puyou, Armando PLoS Negl Trop Dis Research Article BACKGROUND: Chagas disease affects around 18 million people in the American continent. Unfortunately, there is no satisfactory treatment for the disease. The drugs currently used are not specific and exert serious toxic effects. Thus, there is an urgent need for drugs that are effective. Looking for molecules to eliminate the parasite, we have targeted a central enzyme of the glycolytic pathway: triosephosphate isomerase (TIM). The homodimeric enzyme is catalytically active only as a dimer. Because there are significant differences in the interface of the enzymes from the parasite and humans, we searched for small molecules that specifically disrupt contact between the two subunits of the enzyme from Trypanosoma cruzi but not those of TIM from Homo sapiens (HTIM), and tested if they kill the parasite. METHODOLOGY/PRINCIPAL FINDINGS: Dithiodianiline (DTDA) at nanomolar concentrations completely inactivates recombinant TIM of T. cruzi (TcTIM). It also inactivated HTIM, but at concentrations around 400 times higher. DTDA was also tested on four TcTIM mutants with each of its four cysteines replaced with either valine or alanine. The sensitivity of the mutants to DTDA was markedly similar to that of the wild type. The crystal structure of the TcTIM soaked in DTDA at 2.15 Å resolution, and the data on the mutants showed that inactivation resulted from alterations of the dimer interface. DTDA also prevented the growth of Escherichia coli cells transformed with TcTIM, had no effect on normal E. coli, and also killed T. cruzi epimastigotes in culture. CONCLUSIONS/SIGNIFICANCE: By targeting on the dimer interface of oligomeric enzymes from parasites, it is possible to discover small molecules that selectively thwart the life of the parasite. Also, the conformational changes that DTDA induces in the dimer interface of the trypanosomal enzyme are unique and identify a region of the interface that could be targeted for drug discovery. Public Library of Science 2007-10-31 /pmc/articles/PMC2041813/ /pubmed/17989778 http://dx.doi.org/10.1371/journal.pntd.0000001 Text en Olivares-Illana 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
Olivares-Illana, Vanesa
Rodríguez-Romero, Adela
Becker, Ingeborg
Berzunza, Miriam
García, Juventino
Pérez-Montfort, Ruy
Cabrera, Nallely
López-Calahorra, Francisco
de Gómez-Puyou, Marieta Tuena
Gómez-Puyou, Armando
Perturbation of the Dimer Interface of Triosephosphate Isomerase and its Effect on Trypanosoma cruzi
title Perturbation of the Dimer Interface of Triosephosphate Isomerase and its Effect on Trypanosoma cruzi
title_full Perturbation of the Dimer Interface of Triosephosphate Isomerase and its Effect on Trypanosoma cruzi
title_fullStr Perturbation of the Dimer Interface of Triosephosphate Isomerase and its Effect on Trypanosoma cruzi
title_full_unstemmed Perturbation of the Dimer Interface of Triosephosphate Isomerase and its Effect on Trypanosoma cruzi
title_short Perturbation of the Dimer Interface of Triosephosphate Isomerase and its Effect on Trypanosoma cruzi
title_sort perturbation of the dimer interface of triosephosphate isomerase and its effect on trypanosoma cruzi
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2041813/
https://www.ncbi.nlm.nih.gov/pubmed/17989778
http://dx.doi.org/10.1371/journal.pntd.0000001
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