Estudos estruturais de compostos de telúrio e de docking em catepsinas B, K, L, S

Detalhes bibliográficos
Autor(a) principal: Maganhi, Stella Hernandez
Data de Publicação: 2013
Tipo de documento: Tese
Idioma: por
Título da fonte: Repositório Institucional da UFSCAR
Texto Completo: https://repositorio.ufscar.br/handle/ufscar/6262
Resumo: Cathepsins are lysosomal cysteine proteases responsible for protein turnover in our organism. In non-lysosomal environment they are related to a number of diseases such as cancer, Alzheimer, autoimmune diseases and osteoporosis. Tellurium compounds have proved to be promising therapeutic agents against these diseases due to inhibition of the proteases through the formation of a Te S covalent bond with the sulfur of a catalytic cysteine. In this work the crystal and molecular structures of compounds (ptol)Te[C(H)=C(Cl)Ph]X2 (X = Cl, Br, I), butyldiiodo[(1Z)-(2- iodopent-1-en-yl)-4- tellane and their docking in Catepsine B are described. The results showed that these compounds, whose activity has not been measured, should have an inhibitory activity very similar to that of a known compound with a close structure. Moreover, it is shown that the substitution of a phenyl group for an aliphatic one should not have any influence on the activity of these kind of compounds. Also the structures of a series of dipnones were determined which were used as basis for the molecular modeling of others that could not be crystallized and for the docking studies in catepsins B, K, L and S. The results allowed establishing a model that explains their different inhibitory activities.
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spelling Maganhi, Stella HernandezSchpector, Júlio Zukermanhttp://lattes.cnpq.br/4252331837170383http://lattes.cnpq.br/1720675268286912e6f9cd88-ef13-4c2e-b0af-652d019ddf882016-06-02T20:34:42Z2013-06-072016-06-02T20:34:42Z2013-03-28https://repositorio.ufscar.br/handle/ufscar/6262Cathepsins are lysosomal cysteine proteases responsible for protein turnover in our organism. In non-lysosomal environment they are related to a number of diseases such as cancer, Alzheimer, autoimmune diseases and osteoporosis. Tellurium compounds have proved to be promising therapeutic agents against these diseases due to inhibition of the proteases through the formation of a Te S covalent bond with the sulfur of a catalytic cysteine. In this work the crystal and molecular structures of compounds (ptol)Te[C(H)=C(Cl)Ph]X2 (X = Cl, Br, I), butyldiiodo[(1Z)-(2- iodopent-1-en-yl)-4- tellane and their docking in Catepsine B are described. The results showed that these compounds, whose activity has not been measured, should have an inhibitory activity very similar to that of a known compound with a close structure. Moreover, it is shown that the substitution of a phenyl group for an aliphatic one should not have any influence on the activity of these kind of compounds. Also the structures of a series of dipnones were determined which were used as basis for the molecular modeling of others that could not be crystallized and for the docking studies in catepsins B, K, L and S. The results allowed establishing a model that explains their different inhibitory activities.As catepsinas são cisteíno proteases lisossômicas presentes no nosso organismo. Quando em ambiente não lisossômico, estão relacionadas a uma série de doenças como câncer, Alzheimer, doenças autoimunes e osteoporose. Neste contexto, compostos de telúrio têm sido promissores agentes terapêuticos contra estas doenças por apresentarem ação inibitória das catepsinas. Isso ocorre devido à formação de uma ligação covalente entre telúrio e o enxofre da cisteína catalítica. Neste trabalho são descritas as estruturas cristalinas e moleculares dos compostos (ptol)Te[C(H)=C(Cl)Ph]X2 (X = Cl, Br, I), butildiiodo[(1Z)-(2-iodopent-1-em-1-il) 4- telano, e o docking destes compostos em Catepsina B. Os resultados mostram que estes compostos, cujas atividades não foram medidas, poderão apresentar atividades inibitórias semelhantes à de um composto de estrutura similar e com atividade conhecida. Mais ainda, foi mostrado que a substituição de um grupo fenila por um grupo alifático não deverá ter influência na atividade deste tipo de compostos. Foram também determinadas as estruturas cristalinas e moleculares de três dipnonas. Estas estruturas serviram de base para a modelagem das estruturas de outros compostos que não puderam ser cristalizados e para a realização de docking nas catepsinas B, K, L, e S. Foi então estabelecido um modelo para explicar as diferentes atividades inibitórias dos compostos de telúrio.Universidade Federal de Minas Geraisapplication/pdfporUniversidade Federal de São CarlosPrograma de Pós-Graduação em Química - PPGQUFSCarBRCristalografiaDockingTelúrioRaios xCatepsinasModelagem molecularCIENCIAS EXATAS E DA TERRA::QUIMICAEstudos estruturais de compostos de telúrio e de docking em catepsinas B, K, L, Sinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/doctoralThesis-1-1e0a7cf72-f4fb-48f4-93c2-3e7bc492b3cbinfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFSCARinstname:Universidade Federal de São Carlos (UFSCAR)instacron:UFSCARORIGINAL5168.pdfapplication/pdf8720586https://repositorio.ufscar.br/bitstream/ufscar/6262/1/5168.pdf0dc0ddbacccaf3e2f1fcfb515b343484MD51TEXT5168.pdf.txt5168.pdf.txtExtracted texttext/plain0https://repositorio.ufscar.br/bitstream/ufscar/6262/4/5168.pdf.txtd41d8cd98f00b204e9800998ecf8427eMD54THUMBNAIL5168.pdf.jpg5168.pdf.jpgIM Thumbnailimage/jpeg8891https://repositorio.ufscar.br/bitstream/ufscar/6262/5/5168.pdf.jpga13401d116dc7253940c615c79b207a9MD55ufscar/62622023-09-18 18:30:35.998oai:repositorio.ufscar.br:ufscar/6262Repositório InstitucionalPUBhttps://repositorio.ufscar.br/oai/requestopendoar:43222023-09-18T18:30:35Repositório Institucional da UFSCAR - Universidade Federal de São Carlos (UFSCAR)false
dc.title.por.fl_str_mv Estudos estruturais de compostos de telúrio e de docking em catepsinas B, K, L, S
title Estudos estruturais de compostos de telúrio e de docking em catepsinas B, K, L, S
spellingShingle Estudos estruturais de compostos de telúrio e de docking em catepsinas B, K, L, S
Maganhi, Stella Hernandez
Cristalografia
Docking
Telúrio
Raios x
Catepsinas
Modelagem molecular
CIENCIAS EXATAS E DA TERRA::QUIMICA
title_short Estudos estruturais de compostos de telúrio e de docking em catepsinas B, K, L, S
title_full Estudos estruturais de compostos de telúrio e de docking em catepsinas B, K, L, S
title_fullStr Estudos estruturais de compostos de telúrio e de docking em catepsinas B, K, L, S
title_full_unstemmed Estudos estruturais de compostos de telúrio e de docking em catepsinas B, K, L, S
title_sort Estudos estruturais de compostos de telúrio e de docking em catepsinas B, K, L, S
author Maganhi, Stella Hernandez
author_facet Maganhi, Stella Hernandez
author_role author
dc.contributor.authorlattes.por.fl_str_mv http://lattes.cnpq.br/1720675268286912
dc.contributor.author.fl_str_mv Maganhi, Stella Hernandez
dc.contributor.advisor1.fl_str_mv Schpector, Júlio Zukerman
dc.contributor.advisor1Lattes.fl_str_mv http://lattes.cnpq.br/4252331837170383
dc.contributor.authorID.fl_str_mv e6f9cd88-ef13-4c2e-b0af-652d019ddf88
contributor_str_mv Schpector, Júlio Zukerman
dc.subject.por.fl_str_mv Cristalografia
Docking
Telúrio
Raios x
Catepsinas
Modelagem molecular
topic Cristalografia
Docking
Telúrio
Raios x
Catepsinas
Modelagem molecular
CIENCIAS EXATAS E DA TERRA::QUIMICA
dc.subject.cnpq.fl_str_mv CIENCIAS EXATAS E DA TERRA::QUIMICA
description Cathepsins are lysosomal cysteine proteases responsible for protein turnover in our organism. In non-lysosomal environment they are related to a number of diseases such as cancer, Alzheimer, autoimmune diseases and osteoporosis. Tellurium compounds have proved to be promising therapeutic agents against these diseases due to inhibition of the proteases through the formation of a Te S covalent bond with the sulfur of a catalytic cysteine. In this work the crystal and molecular structures of compounds (ptol)Te[C(H)=C(Cl)Ph]X2 (X = Cl, Br, I), butyldiiodo[(1Z)-(2- iodopent-1-en-yl)-4- tellane and their docking in Catepsine B are described. The results showed that these compounds, whose activity has not been measured, should have an inhibitory activity very similar to that of a known compound with a close structure. Moreover, it is shown that the substitution of a phenyl group for an aliphatic one should not have any influence on the activity of these kind of compounds. Also the structures of a series of dipnones were determined which were used as basis for the molecular modeling of others that could not be crystallized and for the docking studies in catepsins B, K, L and S. The results allowed establishing a model that explains their different inhibitory activities.
publishDate 2013
dc.date.available.fl_str_mv 2013-06-07
2016-06-02T20:34:42Z
dc.date.issued.fl_str_mv 2013-03-28
dc.date.accessioned.fl_str_mv 2016-06-02T20:34:42Z
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
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dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
dc.publisher.none.fl_str_mv Universidade Federal de São Carlos
dc.publisher.program.fl_str_mv Programa de Pós-Graduação em Química - PPGQ
dc.publisher.initials.fl_str_mv UFSCar
dc.publisher.country.fl_str_mv BR
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