Molecular models of NS3 protease variants of the Hepatitis C virus

Detalhes bibliográficos
Autor(a) principal: da Silveira, NJF
Data de Publicação: 2005
Outros Autores: Arcuri, H. A., Bonalumi, C. E., de Souza, F. P., Mello, IMVGC, Rahal, Paula [UNESP], Pinho, JRR, de Azevedo, W. F.
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Institucional da UNESP
Texto Completo: http://dx.doi.org/10.1186/1472-6807-5-1
http://hdl.handle.net/11449/21342
Resumo: Background: Hepatitis C virus (HCV) currently infects approximately three percent of the world population. In view of the lack of vaccines against HCV, there is an urgent need for an efficient treatment of the disease by an effective antiviral drug. Rational drug design has not been the primary way for discovering major therapeutics. Nevertheless, there are reports of success in the development of inhibitor using a structure-based approach. One of the possible targets for drug development against HCV is the NS3 protease variants. Based on the three-dimensional structure of these variants we expect to identify new NS3 protease inhibitors. In order to speed up the modeling process all NS3 protease variant models were generated in a Beowulf cluster. The potential of the structural bioinformatics for development of new antiviral drugs is discussed.Results: the atomic coordinates of crystallographic structure 1CU1 and 1DY9 were used as starting model for modeling of the NS3 protease variant structures. The NS3 protease variant structures are composed of six subdomains, which occur in sequence along the polypeptide chain. The protease domain exhibits the dual beta-barrel fold that is common among members of the chymotrypsin serine protease family. The helicase domain contains two structurally related beta-alpha-beta subdomains and a third subdomain of seven helices and three short beta strands. The latter domain is usually referred to as the helicase alpha-helical subdomain. The rmsd value of bond lengths and bond angles, the average G-factor and Verify 3D values are presented for NS3 protease variant structures.Conclusions: This project increases the certainty that homology modeling is an useful tool in structural biology and that it can be very valuable in annotating genome sequence information and contributing to structural and functional genomics from virus. The structural models will be used to guide future efforts in the structure-based drug design of a new generation of NS3 protease variants inhibitors. All models in the database are publicly accessible via our interactive website, providing us with large amount of structural models for use in protein-ligand docking analysis.
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spelling Molecular models of NS3 protease variants of the Hepatitis C virusBackground: Hepatitis C virus (HCV) currently infects approximately three percent of the world population. In view of the lack of vaccines against HCV, there is an urgent need for an efficient treatment of the disease by an effective antiviral drug. Rational drug design has not been the primary way for discovering major therapeutics. Nevertheless, there are reports of success in the development of inhibitor using a structure-based approach. One of the possible targets for drug development against HCV is the NS3 protease variants. Based on the three-dimensional structure of these variants we expect to identify new NS3 protease inhibitors. In order to speed up the modeling process all NS3 protease variant models were generated in a Beowulf cluster. The potential of the structural bioinformatics for development of new antiviral drugs is discussed.Results: the atomic coordinates of crystallographic structure 1CU1 and 1DY9 were used as starting model for modeling of the NS3 protease variant structures. The NS3 protease variant structures are composed of six subdomains, which occur in sequence along the polypeptide chain. The protease domain exhibits the dual beta-barrel fold that is common among members of the chymotrypsin serine protease family. The helicase domain contains two structurally related beta-alpha-beta subdomains and a third subdomain of seven helices and three short beta strands. The latter domain is usually referred to as the helicase alpha-helical subdomain. The rmsd value of bond lengths and bond angles, the average G-factor and Verify 3D values are presented for NS3 protease variant structures.Conclusions: This project increases the certainty that homology modeling is an useful tool in structural biology and that it can be very valuable in annotating genome sequence information and contributing to structural and functional genomics from virus. The structural models will be used to guide future efforts in the structure-based drug design of a new generation of NS3 protease variants inhibitors. All models in the database are publicly accessible via our interactive website, providing us with large amount of structural models for use in protein-ligand docking analysis.UNESP, Dept Phys, IBILCE, Sao Jose do Rio Preto, SP, BrazilUSP, Dept Microbiol, Inst Biomed Sci, BR-09500900 São Paulo, BrazilAdolfo Lutz Inst, São Paulo, BrazilUNESP, Dept Biol, IBILCE, Sao Jose do Rio Preto, SP, BrazilInstituto Butantan, Ctr Appl Toxicol, São Paulo, BrazilUNESP, Dept Phys, IBILCE, Sao Jose do Rio Preto, SP, BrazilUNESP, Dept Biol, IBILCE, Sao Jose do Rio Preto, SP, BrazilBiomed Central Ltd.Universidade Estadual Paulista (Unesp)Universidade de São Paulo (USP)Instituto Adolfo Lutz (IAL)Instituto Butantanda Silveira, NJFArcuri, H. A.Bonalumi, C. E.de Souza, F. P.Mello, IMVGCRahal, Paula [UNESP]Pinho, JRRde Azevedo, W. F.2014-05-20T14:00:20Z2014-05-20T14:00:20Z2005-01-21info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/article8application/pdfhttp://dx.doi.org/10.1186/1472-6807-5-1Bmc Structural Biology. London: Biomed Central Ltd., v. 5, 8 p., 2005.1471-2237http://hdl.handle.net/11449/2134210.1186/1472-6807-5-1WOS:000234256300001WOS000234256300001.pdf79910823626712120000-0001-5693-6148Web of Sciencereponame:Repositório Institucional da UNESPinstname:Universidade Estadual Paulista (UNESP)instacron:UNESPengBmc Structural Biologyinfo:eu-repo/semantics/openAccess2023-12-29T06:19:33Zoai:repositorio.unesp.br:11449/21342Repositório InstitucionalPUBhttp://repositorio.unesp.br/oai/requestopendoar:29462024-08-05T21:35:54.865971Repositório Institucional da UNESP - Universidade Estadual Paulista (UNESP)false
dc.title.none.fl_str_mv Molecular models of NS3 protease variants of the Hepatitis C virus
title Molecular models of NS3 protease variants of the Hepatitis C virus
spellingShingle Molecular models of NS3 protease variants of the Hepatitis C virus
da Silveira, NJF
title_short Molecular models of NS3 protease variants of the Hepatitis C virus
title_full Molecular models of NS3 protease variants of the Hepatitis C virus
title_fullStr Molecular models of NS3 protease variants of the Hepatitis C virus
title_full_unstemmed Molecular models of NS3 protease variants of the Hepatitis C virus
title_sort Molecular models of NS3 protease variants of the Hepatitis C virus
author da Silveira, NJF
author_facet da Silveira, NJF
Arcuri, H. A.
Bonalumi, C. E.
de Souza, F. P.
Mello, IMVGC
Rahal, Paula [UNESP]
Pinho, JRR
de Azevedo, W. F.
author_role author
author2 Arcuri, H. A.
Bonalumi, C. E.
de Souza, F. P.
Mello, IMVGC
Rahal, Paula [UNESP]
Pinho, JRR
de Azevedo, W. F.
author2_role author
author
author
author
author
author
author
dc.contributor.none.fl_str_mv Universidade Estadual Paulista (Unesp)
Universidade de São Paulo (USP)
Instituto Adolfo Lutz (IAL)
Instituto Butantan
dc.contributor.author.fl_str_mv da Silveira, NJF
Arcuri, H. A.
Bonalumi, C. E.
de Souza, F. P.
Mello, IMVGC
Rahal, Paula [UNESP]
Pinho, JRR
de Azevedo, W. F.
description Background: Hepatitis C virus (HCV) currently infects approximately three percent of the world population. In view of the lack of vaccines against HCV, there is an urgent need for an efficient treatment of the disease by an effective antiviral drug. Rational drug design has not been the primary way for discovering major therapeutics. Nevertheless, there are reports of success in the development of inhibitor using a structure-based approach. One of the possible targets for drug development against HCV is the NS3 protease variants. Based on the three-dimensional structure of these variants we expect to identify new NS3 protease inhibitors. In order to speed up the modeling process all NS3 protease variant models were generated in a Beowulf cluster. The potential of the structural bioinformatics for development of new antiviral drugs is discussed.Results: the atomic coordinates of crystallographic structure 1CU1 and 1DY9 were used as starting model for modeling of the NS3 protease variant structures. The NS3 protease variant structures are composed of six subdomains, which occur in sequence along the polypeptide chain. The protease domain exhibits the dual beta-barrel fold that is common among members of the chymotrypsin serine protease family. The helicase domain contains two structurally related beta-alpha-beta subdomains and a third subdomain of seven helices and three short beta strands. The latter domain is usually referred to as the helicase alpha-helical subdomain. The rmsd value of bond lengths and bond angles, the average G-factor and Verify 3D values are presented for NS3 protease variant structures.Conclusions: This project increases the certainty that homology modeling is an useful tool in structural biology and that it can be very valuable in annotating genome sequence information and contributing to structural and functional genomics from virus. The structural models will be used to guide future efforts in the structure-based drug design of a new generation of NS3 protease variants inhibitors. All models in the database are publicly accessible via our interactive website, providing us with large amount of structural models for use in protein-ligand docking analysis.
publishDate 2005
dc.date.none.fl_str_mv 2005-01-21
2014-05-20T14:00:20Z
2014-05-20T14:00:20Z
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/10.1186/1472-6807-5-1
Bmc Structural Biology. London: Biomed Central Ltd., v. 5, 8 p., 2005.
1471-2237
http://hdl.handle.net/11449/21342
10.1186/1472-6807-5-1
WOS:000234256300001
WOS000234256300001.pdf
7991082362671212
0000-0001-5693-6148
url http://dx.doi.org/10.1186/1472-6807-5-1
http://hdl.handle.net/11449/21342
identifier_str_mv Bmc Structural Biology. London: Biomed Central Ltd., v. 5, 8 p., 2005.
1471-2237
10.1186/1472-6807-5-1
WOS:000234256300001
WOS000234256300001.pdf
7991082362671212
0000-0001-5693-6148
dc.language.iso.fl_str_mv eng
language eng
dc.relation.none.fl_str_mv Bmc Structural Biology
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv 8
application/pdf
dc.publisher.none.fl_str_mv Biomed Central Ltd.
publisher.none.fl_str_mv Biomed Central Ltd.
dc.source.none.fl_str_mv Web of Science
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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