Tetracycline Derivatives Inhibit Plasmodial Cysteine Protease Falcipain-2 through Binding to a Distal Allosteric Site

Detalhes bibliográficos
Autor(a) principal: Hernández González, Jorge Enrique [UNESP]
Data de Publicação: 2022
Outros Autores: Alberca, Lucas N., Masforrol González, Yordanka, Reyes Acosta, Osvaldo, Talevi, Alan, Salas-Sarduy, Emir
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Institucional da UNESP
Texto Completo: http://dx.doi.org/10.1021/acs.jcim.1c01189
http://hdl.handle.net/11449/230172
Resumo: Allosteric inhibitors regulate enzyme activity from remote and usually specific pockets. As they promise an avenue for less toxic and safer drugs, the identification and characterization of allosteric inhibitors has gained great academic and biomedical interest in recent years. Research on falcipain-2 (FP-2), the major papain-like cysteine hemoglobinase of Plasmodium falciparum, might benefit from this strategy to overcome the low selectivity against human cathepsins shown by active site-directed inhibitors. Encouraged by our previous finding that methacycline inhibits FP-2 noncompetitively, here we assessed other five tetracycline derivatives against this target and characterized their inhibition mechanism. As previously shown for methacycline, tetracycline derivatives inhibited FP-2 in a noncompetitive fashion, with Ki values ranging from 121 to 190 μM. A possible binding to the S′ side of the FP-2 active site, similar to that described by X-ray crystallography (PDB: 6SSZ) for the noncompetitive inhibitor E-chalcone 48 (EC48), was experimentally discarded by kinetic analysis using a large peptidyl substrate spanning the whole active site. By combining lengthy molecular dynamics (MD) simulations that allowed methacycline to diffuse from solution to different FP-2 surface regions and free energy calculations, we predicted the most likely binding mode of the ligand. Of note, the proposed binding pose explains the low differences in Ki values observed for the tested tetracycline derivatives and the calculated binding free energies match the experimental values. Overall, this study has implications for the design of novel allosteric inhibitors against FP-2 and sets the basis for further optimization of the tetracycline scaffold to produce more potent and selective inhibitors.
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spelling Tetracycline Derivatives Inhibit Plasmodial Cysteine Protease Falcipain-2 through Binding to a Distal Allosteric SiteAllosteric inhibitors regulate enzyme activity from remote and usually specific pockets. As they promise an avenue for less toxic and safer drugs, the identification and characterization of allosteric inhibitors has gained great academic and biomedical interest in recent years. Research on falcipain-2 (FP-2), the major papain-like cysteine hemoglobinase of Plasmodium falciparum, might benefit from this strategy to overcome the low selectivity against human cathepsins shown by active site-directed inhibitors. Encouraged by our previous finding that methacycline inhibits FP-2 noncompetitively, here we assessed other five tetracycline derivatives against this target and characterized their inhibition mechanism. As previously shown for methacycline, tetracycline derivatives inhibited FP-2 in a noncompetitive fashion, with Ki values ranging from 121 to 190 μM. A possible binding to the S′ side of the FP-2 active site, similar to that described by X-ray crystallography (PDB: 6SSZ) for the noncompetitive inhibitor E-chalcone 48 (EC48), was experimentally discarded by kinetic analysis using a large peptidyl substrate spanning the whole active site. By combining lengthy molecular dynamics (MD) simulations that allowed methacycline to diffuse from solution to different FP-2 surface regions and free energy calculations, we predicted the most likely binding mode of the ligand. Of note, the proposed binding pose explains the low differences in Ki values observed for the tested tetracycline derivatives and the calculated binding free energies match the experimental values. Overall, this study has implications for the design of novel allosteric inhibitors against FP-2 and sets the basis for further optimization of the tetracycline scaffold to produce more potent and selective inhibitors.Departamento de Física Instituto de Biociências Letras e Ciências Exatas Universidade Estadual Paulista Júlio de Mesquita Filho, Rua Cristóvão Colombo, 2265, Jardim Nazareth, São José do Rio PretoLaboratory of Bioactive Compounds Research and Development (LIDeB) Department of Biological Sciences Exact Sciences College Universidad Nacional de la PlataChemistry and Physics Department Center for Genetic Engineering and BiotechnologyInst. de Invest. Biotecnologicas Dr. Rodolfo Ugalde-Universidad Nacional de San Martin-CONICET, San MartínDepartamento de Física Instituto de Biociências Letras e Ciências Exatas Universidade Estadual Paulista Júlio de Mesquita Filho, Rua Cristóvão Colombo, 2265, Jardim Nazareth, São José do Rio PretoUniversidade Estadual Paulista (UNESP)Universidad Nacional de la PlataCenter for Genetic Engineering and BiotechnologyInst. de Invest. Biotecnologicas Dr. Rodolfo Ugalde-Universidad Nacional de San Martin-CONICETHernández González, Jorge Enrique [UNESP]Alberca, Lucas N.Masforrol González, YordankaReyes Acosta, OsvaldoTalevi, AlanSalas-Sarduy, Emir2022-04-29T08:38:15Z2022-04-29T08:38:15Z2022-01-10info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/article159-175http://dx.doi.org/10.1021/acs.jcim.1c01189Journal of Chemical Information and Modeling, v. 62, n. 1, p. 159-175, 2022.1520-51421549-9596http://hdl.handle.net/11449/23017210.1021/acs.jcim.1c011892-s2.0-85122320076Scopusreponame:Repositório Institucional da UNESPinstname:Universidade Estadual Paulista (UNESP)instacron:UNESPengJournal of Chemical Information and Modelinginfo:eu-repo/semantics/openAccess2022-04-29T08:38:15Zoai:repositorio.unesp.br:11449/230172Repositório InstitucionalPUBhttp://repositorio.unesp.br/oai/requestopendoar:29462024-05-23T11:41:19.057268Repositório Institucional da UNESP - Universidade Estadual Paulista (UNESP)false
dc.title.none.fl_str_mv Tetracycline Derivatives Inhibit Plasmodial Cysteine Protease Falcipain-2 through Binding to a Distal Allosteric Site
title Tetracycline Derivatives Inhibit Plasmodial Cysteine Protease Falcipain-2 through Binding to a Distal Allosteric Site
spellingShingle Tetracycline Derivatives Inhibit Plasmodial Cysteine Protease Falcipain-2 through Binding to a Distal Allosteric Site
Hernández González, Jorge Enrique [UNESP]
title_short Tetracycline Derivatives Inhibit Plasmodial Cysteine Protease Falcipain-2 through Binding to a Distal Allosteric Site
title_full Tetracycline Derivatives Inhibit Plasmodial Cysteine Protease Falcipain-2 through Binding to a Distal Allosteric Site
title_fullStr Tetracycline Derivatives Inhibit Plasmodial Cysteine Protease Falcipain-2 through Binding to a Distal Allosteric Site
title_full_unstemmed Tetracycline Derivatives Inhibit Plasmodial Cysteine Protease Falcipain-2 through Binding to a Distal Allosteric Site
title_sort Tetracycline Derivatives Inhibit Plasmodial Cysteine Protease Falcipain-2 through Binding to a Distal Allosteric Site
author Hernández González, Jorge Enrique [UNESP]
author_facet Hernández González, Jorge Enrique [UNESP]
Alberca, Lucas N.
Masforrol González, Yordanka
Reyes Acosta, Osvaldo
Talevi, Alan
Salas-Sarduy, Emir
author_role author
author2 Alberca, Lucas N.
Masforrol González, Yordanka
Reyes Acosta, Osvaldo
Talevi, Alan
Salas-Sarduy, Emir
author2_role author
author
author
author
author
dc.contributor.none.fl_str_mv Universidade Estadual Paulista (UNESP)
Universidad Nacional de la Plata
Center for Genetic Engineering and Biotechnology
Inst. de Invest. Biotecnologicas Dr. Rodolfo Ugalde-Universidad Nacional de San Martin-CONICET
dc.contributor.author.fl_str_mv Hernández González, Jorge Enrique [UNESP]
Alberca, Lucas N.
Masforrol González, Yordanka
Reyes Acosta, Osvaldo
Talevi, Alan
Salas-Sarduy, Emir
description Allosteric inhibitors regulate enzyme activity from remote and usually specific pockets. As they promise an avenue for less toxic and safer drugs, the identification and characterization of allosteric inhibitors has gained great academic and biomedical interest in recent years. Research on falcipain-2 (FP-2), the major papain-like cysteine hemoglobinase of Plasmodium falciparum, might benefit from this strategy to overcome the low selectivity against human cathepsins shown by active site-directed inhibitors. Encouraged by our previous finding that methacycline inhibits FP-2 noncompetitively, here we assessed other five tetracycline derivatives against this target and characterized their inhibition mechanism. As previously shown for methacycline, tetracycline derivatives inhibited FP-2 in a noncompetitive fashion, with Ki values ranging from 121 to 190 μM. A possible binding to the S′ side of the FP-2 active site, similar to that described by X-ray crystallography (PDB: 6SSZ) for the noncompetitive inhibitor E-chalcone 48 (EC48), was experimentally discarded by kinetic analysis using a large peptidyl substrate spanning the whole active site. By combining lengthy molecular dynamics (MD) simulations that allowed methacycline to diffuse from solution to different FP-2 surface regions and free energy calculations, we predicted the most likely binding mode of the ligand. Of note, the proposed binding pose explains the low differences in Ki values observed for the tested tetracycline derivatives and the calculated binding free energies match the experimental values. Overall, this study has implications for the design of novel allosteric inhibitors against FP-2 and sets the basis for further optimization of the tetracycline scaffold to produce more potent and selective inhibitors.
publishDate 2022
dc.date.none.fl_str_mv 2022-04-29T08:38:15Z
2022-04-29T08:38:15Z
2022-01-10
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/article
format article
status_str publishedVersion
dc.identifier.uri.fl_str_mv http://dx.doi.org/10.1021/acs.jcim.1c01189
Journal of Chemical Information and Modeling, v. 62, n. 1, p. 159-175, 2022.
1520-5142
1549-9596
http://hdl.handle.net/11449/230172
10.1021/acs.jcim.1c01189
2-s2.0-85122320076
url http://dx.doi.org/10.1021/acs.jcim.1c01189
http://hdl.handle.net/11449/230172
identifier_str_mv Journal of Chemical Information and Modeling, v. 62, n. 1, p. 159-175, 2022.
1520-5142
1549-9596
10.1021/acs.jcim.1c01189
2-s2.0-85122320076
dc.language.iso.fl_str_mv eng
language eng
dc.relation.none.fl_str_mv Journal of Chemical Information and Modeling
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv 159-175
dc.source.none.fl_str_mv Scopus
reponame:Repositório Institucional da UNESP
instname:Universidade Estadual Paulista (UNESP)
instacron:UNESP
instname_str Universidade Estadual Paulista (UNESP)
instacron_str UNESP
institution UNESP
reponame_str Repositório Institucional da UNESP
collection Repositório Institucional da UNESP
repository.name.fl_str_mv Repositório Institucional da UNESP - Universidade Estadual Paulista (UNESP)
repository.mail.fl_str_mv
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