Planejamento de inibidores da cruzaína baseado em fragmentos

Detalhes bibliográficos
Autor(a) principal: Fonseca, Emanuella Maria Barreto
Data de Publicação: 2011
Tipo de documento: Dissertação
Idioma: por
Título da fonte: Repositório Institucional da UFSCAR
Texto Completo: https://repositorio.ufscar.br/handle/ufscar/6506
Resumo: The Chagas disease, described in 1909 by the Brazilian sanitary physician, scientist and bacteriologist Dr. Carlos Chagas, is caused by the Trypanosomatid parasite Trypanosoma cruzi. Current treatments involve the use of drugs benznidazole and nifurtimox, which are effective only in the early stage of the disease (acute phase), but have severe side effects. The enzyme cruzain is a validated target for searching small molecules to act against Chagas disease. Cruzain inhibition has been studied for the discovery and development of new drugs. In this work, the planning strategy was based on molecular fragments, using a computational approach for selecting them. Using GRID/CPCA, important residues such as Ser207 and Asp69 were identified in an adjacent cavity to the S2 sub-site of the enzyme. These residues can take part on hydrogen-bond interactions and have not been explored in the search for inhibitors for this target. In addition, we identified patterns of molecular recognition of the enzyme, based on the structures deposited in the Protein Data Bank, which are co-crystallized with inhibitors at the site of the enzyme. These inhibitors were used to guide the search via SMARTS pattern to build a fragment database. Docking and molecular dynamics were used to select the fragments for an in vitro assay. Many fragments were acquired and tested against cruzain using the technique of fluorescence spectroscopy. One fragment (Nequimed147) showed activity, inhibiting the enzyme with IC50 equal to 2.39 mM, resulting in a ligand efficiency of 0.23 kcal mol-1 weight atom-1. Based on this fragment, new inhibitors were identified with IC50 between 1.25 and 4.29 mM. Their ligand efficiencies were in the range of 0.21 and 0.26 kcal mol-1 weight atom-1 whose molecular recognition features are suitable for the search of new enzyme inhibitors likely to bind the cavity near the S2 sub-site that has not been explored yet.
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spelling Fonseca, Emanuella Maria BarretoMontanari, Carlos Albertohttp://lattes.cnpq.br/9200533791228786http://lattes.cnpq.br/1789418915938702ae16c402-458b-4920-9d81-1b57bfabaffa2016-06-02T20:36:34Z2011-10-262016-06-02T20:36:34Z2011-07-27FONSECA, Emanuella Maria Barreto. Fragment based drug design of cruzain inhibitors. 2011. 91 f. Dissertação (Mestrado em Ciências Exatas e da Terra) - Universidade Federal de São Carlos, São Carlos, 2011.https://repositorio.ufscar.br/handle/ufscar/6506The Chagas disease, described in 1909 by the Brazilian sanitary physician, scientist and bacteriologist Dr. Carlos Chagas, is caused by the Trypanosomatid parasite Trypanosoma cruzi. Current treatments involve the use of drugs benznidazole and nifurtimox, which are effective only in the early stage of the disease (acute phase), but have severe side effects. The enzyme cruzain is a validated target for searching small molecules to act against Chagas disease. Cruzain inhibition has been studied for the discovery and development of new drugs. In this work, the planning strategy was based on molecular fragments, using a computational approach for selecting them. Using GRID/CPCA, important residues such as Ser207 and Asp69 were identified in an adjacent cavity to the S2 sub-site of the enzyme. These residues can take part on hydrogen-bond interactions and have not been explored in the search for inhibitors for this target. In addition, we identified patterns of molecular recognition of the enzyme, based on the structures deposited in the Protein Data Bank, which are co-crystallized with inhibitors at the site of the enzyme. These inhibitors were used to guide the search via SMARTS pattern to build a fragment database. Docking and molecular dynamics were used to select the fragments for an in vitro assay. Many fragments were acquired and tested against cruzain using the technique of fluorescence spectroscopy. One fragment (Nequimed147) showed activity, inhibiting the enzyme with IC50 equal to 2.39 mM, resulting in a ligand efficiency of 0.23 kcal mol-1 weight atom-1. Based on this fragment, new inhibitors were identified with IC50 between 1.25 and 4.29 mM. Their ligand efficiencies were in the range of 0.21 and 0.26 kcal mol-1 weight atom-1 whose molecular recognition features are suitable for the search of new enzyme inhibitors likely to bind the cavity near the S2 sub-site that has not been explored yet.A Doença de Chagas, descrita em 1909 pelo médico sanitarista brasileiro Dr. Carlos Chagas, é causada pelo parasito tripanossomatídeo Trypanosoma cruzi. Os tratamentos atuais consistem no uso dos fármacos benzonidazol e nifurtimox que são eficazes apenas no estágio inicial da doença (fase aguda), mas possuem efeitos colaterais severos. A enzima cruzaína constitui um alvo validado contra a doença de Chagas e sua inibição vem sendo estudada para o planejamento de fármacos. Neste trabalho a estratégia adotada foi o planejamento baseado em fragmentos moleculares, através de uma abordagem computacional para a seleção dos mesmos. Utilizando a técnica GRID/CPCA, foram identificados resíduos importantes, como Ser207 e Asp69, em uma região adjacente ao sub-sítio S2 da enzima. Estes resíduos são capazes de realizar interações do tipo ligação de hidrogênio e ainda não foram explorados na busca de inibidores para esse alvo. Além disso, foram identificados padrões de reconhecimento molecular da enzima, baseado nas estruturas depositadas no Protein Data Bank com inibidores cocristalizados no sítio da enzima, que foram utilizados para fazer uma busca guiada com a utilização de padrão SMARTS para construção de um banco de fragmentos. As técnicas de docagem e dinâmica molecular foram usadas para selecionar os fragmentos, os quais foram adquiridos para os ensaios in vitro. Vários fragmentos foram testados contra a enzima cruzaína utilizando a técnica de fluorimetria, sendo que um deles (Nequimed147) mostrou-se capaz de inibir a enzima com IC50 igual a 2,39 mM, resultando em uma eficiência do ligante de 0,23 kcal mol-1 átomo pesado-1. Baseado nesse fragmento, novos inibidores foram identificados com potência entre 1,25 e 4,29 mM e eficiência do ligante entre 0,21 e 0,26 kcal mol-1 átomo pesado-1, com características apropriadas para o reconhecimento molecular pela enzima cruzaína na região do sub-sítio S2.Financiadora de Estudos e Projetosapplication/pdfporUniversidade Federal de São CarlosPrograma de Pós-Graduação em Química - PPGQUFSCarBRQuímica orgânicaChagas, Doença deModelagem molecularTrypanosoma CruziCIENCIAS EXATAS E DA TERRA::QUIMICAPlanejamento de inibidores da cruzaína baseado em fragmentosFragment based drug design of cruzain inhibitorsinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesis-1-199488e9a-d28d-4248-a854-9d36d6a2a25binfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFSCARinstname:Universidade Federal de São Carlos (UFSCAR)instacron:UFSCARORIGINAL3869.pdfapplication/pdf12129966https://repositorio.ufscar.br/bitstream/ufscar/6506/1/3869.pdf7f17c5b063ae127e4d58be4e1f14b434MD51THUMBNAIL3869.pdf.jpg3869.pdf.jpgIM Thumbnailimage/jpeg7483https://repositorio.ufscar.br/bitstream/ufscar/6506/2/3869.pdf.jpge515e229666dd0ebd2b5edc07e928501MD52ufscar/65062023-09-18 18:31:11.751oai:repositorio.ufscar.br:ufscar/6506Repositório InstitucionalPUBhttps://repositorio.ufscar.br/oai/requestopendoar:43222023-09-18T18:31:11Repositório Institucional da UFSCAR - Universidade Federal de São Carlos (UFSCAR)false
dc.title.por.fl_str_mv Planejamento de inibidores da cruzaína baseado em fragmentos
dc.title.alternative.eng.fl_str_mv Fragment based drug design of cruzain inhibitors
title Planejamento de inibidores da cruzaína baseado em fragmentos
spellingShingle Planejamento de inibidores da cruzaína baseado em fragmentos
Fonseca, Emanuella Maria Barreto
Química orgânica
Chagas, Doença de
Modelagem molecular
Trypanosoma Cruzi
CIENCIAS EXATAS E DA TERRA::QUIMICA
title_short Planejamento de inibidores da cruzaína baseado em fragmentos
title_full Planejamento de inibidores da cruzaína baseado em fragmentos
title_fullStr Planejamento de inibidores da cruzaína baseado em fragmentos
title_full_unstemmed Planejamento de inibidores da cruzaína baseado em fragmentos
title_sort Planejamento de inibidores da cruzaína baseado em fragmentos
author Fonseca, Emanuella Maria Barreto
author_facet Fonseca, Emanuella Maria Barreto
author_role author
dc.contributor.authorlattes.por.fl_str_mv http://lattes.cnpq.br/1789418915938702
dc.contributor.author.fl_str_mv Fonseca, Emanuella Maria Barreto
dc.contributor.advisor1.fl_str_mv Montanari, Carlos Alberto
dc.contributor.advisor1Lattes.fl_str_mv http://lattes.cnpq.br/9200533791228786
dc.contributor.authorID.fl_str_mv ae16c402-458b-4920-9d81-1b57bfabaffa
contributor_str_mv Montanari, Carlos Alberto
dc.subject.por.fl_str_mv Química orgânica
Chagas, Doença de
Modelagem molecular
Trypanosoma Cruzi
topic Química orgânica
Chagas, Doença de
Modelagem molecular
Trypanosoma Cruzi
CIENCIAS EXATAS E DA TERRA::QUIMICA
dc.subject.cnpq.fl_str_mv CIENCIAS EXATAS E DA TERRA::QUIMICA
description The Chagas disease, described in 1909 by the Brazilian sanitary physician, scientist and bacteriologist Dr. Carlos Chagas, is caused by the Trypanosomatid parasite Trypanosoma cruzi. Current treatments involve the use of drugs benznidazole and nifurtimox, which are effective only in the early stage of the disease (acute phase), but have severe side effects. The enzyme cruzain is a validated target for searching small molecules to act against Chagas disease. Cruzain inhibition has been studied for the discovery and development of new drugs. In this work, the planning strategy was based on molecular fragments, using a computational approach for selecting them. Using GRID/CPCA, important residues such as Ser207 and Asp69 were identified in an adjacent cavity to the S2 sub-site of the enzyme. These residues can take part on hydrogen-bond interactions and have not been explored in the search for inhibitors for this target. In addition, we identified patterns of molecular recognition of the enzyme, based on the structures deposited in the Protein Data Bank, which are co-crystallized with inhibitors at the site of the enzyme. These inhibitors were used to guide the search via SMARTS pattern to build a fragment database. Docking and molecular dynamics were used to select the fragments for an in vitro assay. Many fragments were acquired and tested against cruzain using the technique of fluorescence spectroscopy. One fragment (Nequimed147) showed activity, inhibiting the enzyme with IC50 equal to 2.39 mM, resulting in a ligand efficiency of 0.23 kcal mol-1 weight atom-1. Based on this fragment, new inhibitors were identified with IC50 between 1.25 and 4.29 mM. Their ligand efficiencies were in the range of 0.21 and 0.26 kcal mol-1 weight atom-1 whose molecular recognition features are suitable for the search of new enzyme inhibitors likely to bind the cavity near the S2 sub-site that has not been explored yet.
publishDate 2011
dc.date.available.fl_str_mv 2011-10-26
2016-06-02T20:36:34Z
dc.date.issued.fl_str_mv 2011-07-27
dc.date.accessioned.fl_str_mv 2016-06-02T20:36:34Z
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dc.identifier.citation.fl_str_mv FONSECA, Emanuella Maria Barreto. Fragment based drug design of cruzain inhibitors. 2011. 91 f. Dissertação (Mestrado em Ciências Exatas e da Terra) - Universidade Federal de São Carlos, São Carlos, 2011.
dc.identifier.uri.fl_str_mv https://repositorio.ufscar.br/handle/ufscar/6506
identifier_str_mv FONSECA, Emanuella Maria Barreto. Fragment based drug design of cruzain inhibitors. 2011. 91 f. Dissertação (Mestrado em Ciências Exatas e da Terra) - Universidade Federal de São Carlos, São Carlos, 2011.
url https://repositorio.ufscar.br/handle/ufscar/6506
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dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
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