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Crystal structures of Triosephosphate Isomerases from Taenia solium and Schistosoma mansoni provide insights for vaccine rationale and drug design against helminth parasites

Triosephosphate isomerases (TPIs) from Taenia solium (TsTPI) and Schistosoma mansoni (SmTPI) are potential vaccine and drug targets against cysticercosis and schistosomiasis, respectively. This is due to the dependence of parasitic helminths on glycolysis and because those proteins elicit an immune...

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Autores principales: Jimenez-Sandoval, Pedro, Castro-Torres, Eduardo, González-González, Rogelio, Díaz-Quezada, Corina, Gurrola, Misraim, Camacho-Manriquez, Laura D., Leyva-Navarro, Lucia, Brieba, Luis G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6980832/
https://www.ncbi.nlm.nih.gov/pubmed/31923219
http://dx.doi.org/10.1371/journal.pntd.0007815
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author Jimenez-Sandoval, Pedro
Castro-Torres, Eduardo
González-González, Rogelio
Díaz-Quezada, Corina
Gurrola, Misraim
Camacho-Manriquez, Laura D.
Leyva-Navarro, Lucia
Brieba, Luis G.
author_facet Jimenez-Sandoval, Pedro
Castro-Torres, Eduardo
González-González, Rogelio
Díaz-Quezada, Corina
Gurrola, Misraim
Camacho-Manriquez, Laura D.
Leyva-Navarro, Lucia
Brieba, Luis G.
author_sort Jimenez-Sandoval, Pedro
collection PubMed
description Triosephosphate isomerases (TPIs) from Taenia solium (TsTPI) and Schistosoma mansoni (SmTPI) are potential vaccine and drug targets against cysticercosis and schistosomiasis, respectively. This is due to the dependence of parasitic helminths on glycolysis and because those proteins elicit an immune response, presumably due to their surface localization. Here we report the crystal structures of TsTPI and SmTPI in complex with 2-phosphoglyceric acid (2-PGA). Both TPIs fold into a dimeric (β-α)(8) barrel in which the dimer interface consists of α-helices 2, 3, and 4, and swapping of loop 3. TPIs from parasitic helminths harbor a region of three amino acids knows as the SXD/E insert (S155 to E157 and S157 to D159 in TsTPI and SmTPI, respectively). This insert is located between α5 and β6 and is proposed to be the main TPI epitope. This region is part of a solvent-exposed 3(10)–helix that folds into a hook-like structure. The crystal structures of TsTPI and SmTPI predicted conformational epitopes that could be used for vaccine design. Surprisingly, the epitopes corresponding to the SXD/E inserts are not the ones with the greatest immunological potential. SmTPI, but not TsTPI, habors a sole solvent exposed cysteine (SmTPI-S230) and alterations in this residue decrease catalysis. The latter suggests that thiol-conjugating agents could be used to target SmTPI. In sum, the crystal structures of SmTPI and TsTPI are a blueprint for targeted schistosomiasis and cysticercosis drug and vaccine development.
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spelling pubmed-69808322020-02-07 Crystal structures of Triosephosphate Isomerases from Taenia solium and Schistosoma mansoni provide insights for vaccine rationale and drug design against helminth parasites Jimenez-Sandoval, Pedro Castro-Torres, Eduardo González-González, Rogelio Díaz-Quezada, Corina Gurrola, Misraim Camacho-Manriquez, Laura D. Leyva-Navarro, Lucia Brieba, Luis G. PLoS Negl Trop Dis Research Article Triosephosphate isomerases (TPIs) from Taenia solium (TsTPI) and Schistosoma mansoni (SmTPI) are potential vaccine and drug targets against cysticercosis and schistosomiasis, respectively. This is due to the dependence of parasitic helminths on glycolysis and because those proteins elicit an immune response, presumably due to their surface localization. Here we report the crystal structures of TsTPI and SmTPI in complex with 2-phosphoglyceric acid (2-PGA). Both TPIs fold into a dimeric (β-α)(8) barrel in which the dimer interface consists of α-helices 2, 3, and 4, and swapping of loop 3. TPIs from parasitic helminths harbor a region of three amino acids knows as the SXD/E insert (S155 to E157 and S157 to D159 in TsTPI and SmTPI, respectively). This insert is located between α5 and β6 and is proposed to be the main TPI epitope. This region is part of a solvent-exposed 3(10)–helix that folds into a hook-like structure. The crystal structures of TsTPI and SmTPI predicted conformational epitopes that could be used for vaccine design. Surprisingly, the epitopes corresponding to the SXD/E inserts are not the ones with the greatest immunological potential. SmTPI, but not TsTPI, habors a sole solvent exposed cysteine (SmTPI-S230) and alterations in this residue decrease catalysis. The latter suggests that thiol-conjugating agents could be used to target SmTPI. In sum, the crystal structures of SmTPI and TsTPI are a blueprint for targeted schistosomiasis and cysticercosis drug and vaccine development. Public Library of Science 2020-01-10 /pmc/articles/PMC6980832/ /pubmed/31923219 http://dx.doi.org/10.1371/journal.pntd.0007815 Text en © 2020 Jimenez-Sandoval 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 (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Jimenez-Sandoval, Pedro
Castro-Torres, Eduardo
González-González, Rogelio
Díaz-Quezada, Corina
Gurrola, Misraim
Camacho-Manriquez, Laura D.
Leyva-Navarro, Lucia
Brieba, Luis G.
Crystal structures of Triosephosphate Isomerases from Taenia solium and Schistosoma mansoni provide insights for vaccine rationale and drug design against helminth parasites
title Crystal structures of Triosephosphate Isomerases from Taenia solium and Schistosoma mansoni provide insights for vaccine rationale and drug design against helminth parasites
title_full Crystal structures of Triosephosphate Isomerases from Taenia solium and Schistosoma mansoni provide insights for vaccine rationale and drug design against helminth parasites
title_fullStr Crystal structures of Triosephosphate Isomerases from Taenia solium and Schistosoma mansoni provide insights for vaccine rationale and drug design against helminth parasites
title_full_unstemmed Crystal structures of Triosephosphate Isomerases from Taenia solium and Schistosoma mansoni provide insights for vaccine rationale and drug design against helminth parasites
title_short Crystal structures of Triosephosphate Isomerases from Taenia solium and Schistosoma mansoni provide insights for vaccine rationale and drug design against helminth parasites
title_sort crystal structures of triosephosphate isomerases from taenia solium and schistosoma mansoni provide insights for vaccine rationale and drug design against helminth parasites
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6980832/
https://www.ncbi.nlm.nih.gov/pubmed/31923219
http://dx.doi.org/10.1371/journal.pntd.0007815
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