Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae

Detalhes bibliográficos
Autor(a) principal: Ribeiro, Suzana Meira
Data de Publicação: 2014
Tipo de documento: Tese
Idioma: por
Título da fonte: Biblioteca Digital de Teses e Dissertações da UCB
Texto Completo: https://bdtd.ucb.br:8443/jspui/handle/tede/1996
Resumo: Multi-drug resistant Klebsiella pneumoniae that produce the enzyme K. pneumoniae carbapenemase (KPC) are becoming a common cause of infections in health care centers. Furthermore, Klebsiella can develop multicellular biofilms, which lead to elevated adaptive antibiotic resistance. Here, it was described the antimicrobial and anti-biofilm activities of synthetic cationic peptides against K. pneumoniae strains susceptible and carbapenens resistant through in vitro and in vivo assays. By using static microplate assays, it was observed that the concentration of the peptides IDR-1018, DJK-5 and DJK-6 required to prevent biofilm formation by these clinical isolates was below the minimum inhibitory concentration (MIC) of these peptides. Flow cell experiments confirmed the anti-biofilm activity of the peptides against 2 day-old biofilms of different KPC producing isolates and, in some cases, the peptides induced biofilm cell death. Combinations of DJK-6 together with ??-lactam antibiotics, including the carbapenem meropenem, also prevented planktonic growth and biofilm formation of KPC producing strain 1825971. Interestingly, the peptide DJK-6 was able to enhance, by at least 16-fold, the ability of meropenem to eradicate pre-formed biofilms formed by this strain. Although, this combination between meropenem, DJK-6 was effective in vitro, any reduction of bacterial load was observed in murine lung model of infection. Similarly, the peptides HHC-10, IDR-1018 e IDR-1002 was effective in vitro, but ineffective in vivo. The results in vivo, using the peptides HHC-10 and IDR-1018 after infection were contrasting (significant reduction or non-reduction of bacterial load) between two models of lung infection. Others approaches using the peptides IDR-1018 prophylactically or the peptide IDR-1002 (effective in inhibit bacterial growth) before the induction of the infection, as a preventive approach or IDR-1002 (peptide that reduced the bacterial counts in vitro) after infection, also was unable to reduce the bacterial load in lungs of mice. Despite ineffective in acute model of lung infection, the use of cationic peptides, such DJK-6, to potentiate the activity of ??-lactams including meropenem, represents a promising strategy to prevent biofilm formation or eliminate existent biofilms both in medical devices and in body surfaces.
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spelling Franco, Oct??vio Luizhttp://lattes.cnpq.br/8598274096498065Moreno, Susana Elisahttp://lattes.cnpq.br/6666844765040039http://lattes.cnpq.br/2831320496409047Ribeiro, Suzana Meira2016-12-19T17:56:31Z2014-05-19RIBEIRO, Suzana Meira. Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae. 2014. 94f. Tese( Programa Strictu Sensu em Ci??ncias Gen??micas e Biotecnologia) - Universidade Cat??lica de Bras??lia, Bras??lia, 2014.https://bdtd.ucb.br:8443/jspui/handle/tede/1996Multi-drug resistant Klebsiella pneumoniae that produce the enzyme K. pneumoniae carbapenemase (KPC) are becoming a common cause of infections in health care centers. Furthermore, Klebsiella can develop multicellular biofilms, which lead to elevated adaptive antibiotic resistance. Here, it was described the antimicrobial and anti-biofilm activities of synthetic cationic peptides against K. pneumoniae strains susceptible and carbapenens resistant through in vitro and in vivo assays. By using static microplate assays, it was observed that the concentration of the peptides IDR-1018, DJK-5 and DJK-6 required to prevent biofilm formation by these clinical isolates was below the minimum inhibitory concentration (MIC) of these peptides. Flow cell experiments confirmed the anti-biofilm activity of the peptides against 2 day-old biofilms of different KPC producing isolates and, in some cases, the peptides induced biofilm cell death. Combinations of DJK-6 together with ??-lactam antibiotics, including the carbapenem meropenem, also prevented planktonic growth and biofilm formation of KPC producing strain 1825971. Interestingly, the peptide DJK-6 was able to enhance, by at least 16-fold, the ability of meropenem to eradicate pre-formed biofilms formed by this strain. Although, this combination between meropenem, DJK-6 was effective in vitro, any reduction of bacterial load was observed in murine lung model of infection. Similarly, the peptides HHC-10, IDR-1018 e IDR-1002 was effective in vitro, but ineffective in vivo. The results in vivo, using the peptides HHC-10 and IDR-1018 after infection were contrasting (significant reduction or non-reduction of bacterial load) between two models of lung infection. Others approaches using the peptides IDR-1018 prophylactically or the peptide IDR-1002 (effective in inhibit bacterial growth) before the induction of the infection, as a preventive approach or IDR-1002 (peptide that reduced the bacterial counts in vitro) after infection, also was unable to reduce the bacterial load in lungs of mice. Despite ineffective in acute model of lung infection, the use of cationic peptides, such DJK-6, to potentiate the activity of ??-lactams including meropenem, represents a promising strategy to prevent biofilm formation or eliminate existent biofilms both in medical devices and in body surfaces.Klebsiella pneumoniae resistente a m??ltiplos antibi??ticos, que produzem a enzima K. pneumoniae carbapenemase (KPC), est??o se tornando uma causa comum de infec????es em centros de cuidado a sa??de. Al??m disso, K. pneumoniae pode desenvolver biofilmes multicelulares, que levam o aumento da resist??ncia adaptativa a antibi??ticos. Aqui foi descrito a atividade antimicrobiana e antibiofilme de pept??deos cati??nicos sint??ticos contra isolados de K. pneumoniae suscept??vel e resistente a carbapenens em ensaios in vitro e in vivo. Usando ensaios de microplaca est??tico, foi observado que a concentra????o dos pept??deos IDR-1018, DJK-5 e DJK-6, requerida para prevenir a forma????o de biofilmes de isolados resistentes foi abaixo da concentra????o inibit??ria m??nima (CIM) desses pept??deos. Experimentos de fluxo de c??lula confirmaram a atividade antibiofilme dos pept??deos contra biofilmes pr??-formados de diferentes isolados de K. pneumoniae produtores de KPC e, em alguns casos, os pept??deos induziram morte celular. Combina????es de DJK-6 e antibi??ticos ??-lact??micos, incluindo o carbapenem meropenem, tamb??m preveniram o crescimento planct??nico e a forma????o de biofilmes do isolado produtor de KPC 1825971. Interessantemente, o pept??deo DJK-6 foi capaz de aumentar, em pelo menos 16 vezes, a habilidade de meropenem erradicar biofilmes pr??-formados desse isolado. Embora, essa combina????o tenha sido efetiva in vitro, nenhuma redu????o da carga bacteriana foi observada em modelo murino de infec????o pulmonar por K. pneumoniae. Os resultados dos pept??deos HHC-10 e IDR-1018 (os quais inibiram o crescimento bacteriano in vitro a concentra????o que apresentou baixa citotoxicidade) foram contrastantes entre os dois modelos de infec????o pulmonar (significando redu????o ou n??o redu????o da carga bacteriana). Outras abordagens utilizando os pept??deos IDR-1018 profilaticamente ou o pept??deo IDR-1002 (efetivo em inibir o crescimento bacteriano in vitro) ap??s a infec????o, tamb??m foram incapazes de reduzir a carga bacteriana em pulm??es de camundongos. Apesar da inefetividade em modelo agudo de infec????o pulmonar, o uso de pept??deos cati??nicos, tal como DJK-6, para potencializar a atividade de ??-lact??micos, incluindo meropenem, representa uma estrat??gia promissora para prevenir a forma????o de biofilmes ou eliminar biofilmes existentes tanto em equipamentos m??dicos quanto em superf??cies do corpo.Submitted by Kelson Anthony de Menezes (kelson@ucb.br) on 2016-12-19T17:56:31Z No. of bitstreams: 1 SuzanaMeiraRibeiroTese2014.pdf: 4980549 bytes, checksum: df9c1eaadc1ba65bf7c17235d91dc3d7 (MD5)Made available in DSpace on 2016-12-19T17:56:31Z (GMT). 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dc.title.por.fl_str_mv Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae
title Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae
spellingShingle Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae
Ribeiro, Suzana Meira
Biotecnologia
Biofilmes
Pept??deos cati??nicos
Carbapenemase
Gen??tica
Genoma
CIENCIAS BIOLOGICAS::GENETICA
title_short Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae
title_full Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae
title_fullStr Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae
title_full_unstemmed Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae
title_sort Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae
author Ribeiro, Suzana Meira
author_facet Ribeiro, Suzana Meira
author_role author
dc.contributor.advisor1.fl_str_mv Franco, Oct??vio Luiz
dc.contributor.advisor1Lattes.fl_str_mv http://lattes.cnpq.br/8598274096498065
dc.contributor.advisor2.fl_str_mv Moreno, Susana Elisa
dc.contributor.advisor2Lattes.fl_str_mv http://lattes.cnpq.br/6666844765040039
dc.contributor.authorLattes.fl_str_mv http://lattes.cnpq.br/2831320496409047
dc.contributor.author.fl_str_mv Ribeiro, Suzana Meira
contributor_str_mv Franco, Oct??vio Luiz
Moreno, Susana Elisa
dc.subject.por.fl_str_mv Biotecnologia
Biofilmes
Pept??deos cati??nicos
Carbapenemase
Gen??tica
Genoma
topic Biotecnologia
Biofilmes
Pept??deos cati??nicos
Carbapenemase
Gen??tica
Genoma
CIENCIAS BIOLOGICAS::GENETICA
dc.subject.cnpq.fl_str_mv CIENCIAS BIOLOGICAS::GENETICA
dc.description.abstract.eng.fl_txt_mv Multi-drug resistant Klebsiella pneumoniae that produce the enzyme K. pneumoniae carbapenemase (KPC) are becoming a common cause of infections in health care centers. Furthermore, Klebsiella can develop multicellular biofilms, which lead to elevated adaptive antibiotic resistance. Here, it was described the antimicrobial and anti-biofilm activities of synthetic cationic peptides against K. pneumoniae strains susceptible and carbapenens resistant through in vitro and in vivo assays. By using static microplate assays, it was observed that the concentration of the peptides IDR-1018, DJK-5 and DJK-6 required to prevent biofilm formation by these clinical isolates was below the minimum inhibitory concentration (MIC) of these peptides. Flow cell experiments confirmed the anti-biofilm activity of the peptides against 2 day-old biofilms of different KPC producing isolates and, in some cases, the peptides induced biofilm cell death. Combinations of DJK-6 together with ??-lactam antibiotics, including the carbapenem meropenem, also prevented planktonic growth and biofilm formation of KPC producing strain 1825971. Interestingly, the peptide DJK-6 was able to enhance, by at least 16-fold, the ability of meropenem to eradicate pre-formed biofilms formed by this strain. Although, this combination between meropenem, DJK-6 was effective in vitro, any reduction of bacterial load was observed in murine lung model of infection. Similarly, the peptides HHC-10, IDR-1018 e IDR-1002 was effective in vitro, but ineffective in vivo. The results in vivo, using the peptides HHC-10 and IDR-1018 after infection were contrasting (significant reduction or non-reduction of bacterial load) between two models of lung infection. Others approaches using the peptides IDR-1018 prophylactically or the peptide IDR-1002 (effective in inhibit bacterial growth) before the induction of the infection, as a preventive approach or IDR-1002 (peptide that reduced the bacterial counts in vitro) after infection, also was unable to reduce the bacterial load in lungs of mice. Despite ineffective in acute model of lung infection, the use of cationic peptides, such DJK-6, to potentiate the activity of ??-lactams including meropenem, represents a promising strategy to prevent biofilm formation or eliminate existent biofilms both in medical devices and in body surfaces.
dc.description.abstract.por.fl_txt_mv Klebsiella pneumoniae resistente a m??ltiplos antibi??ticos, que produzem a enzima K. pneumoniae carbapenemase (KPC), est??o se tornando uma causa comum de infec????es em centros de cuidado a sa??de. Al??m disso, K. pneumoniae pode desenvolver biofilmes multicelulares, que levam o aumento da resist??ncia adaptativa a antibi??ticos. Aqui foi descrito a atividade antimicrobiana e antibiofilme de pept??deos cati??nicos sint??ticos contra isolados de K. pneumoniae suscept??vel e resistente a carbapenens em ensaios in vitro e in vivo. Usando ensaios de microplaca est??tico, foi observado que a concentra????o dos pept??deos IDR-1018, DJK-5 e DJK-6, requerida para prevenir a forma????o de biofilmes de isolados resistentes foi abaixo da concentra????o inibit??ria m??nima (CIM) desses pept??deos. Experimentos de fluxo de c??lula confirmaram a atividade antibiofilme dos pept??deos contra biofilmes pr??-formados de diferentes isolados de K. pneumoniae produtores de KPC e, em alguns casos, os pept??deos induziram morte celular. Combina????es de DJK-6 e antibi??ticos ??-lact??micos, incluindo o carbapenem meropenem, tamb??m preveniram o crescimento planct??nico e a forma????o de biofilmes do isolado produtor de KPC 1825971. Interessantemente, o pept??deo DJK-6 foi capaz de aumentar, em pelo menos 16 vezes, a habilidade de meropenem erradicar biofilmes pr??-formados desse isolado. Embora, essa combina????o tenha sido efetiva in vitro, nenhuma redu????o da carga bacteriana foi observada em modelo murino de infec????o pulmonar por K. pneumoniae. Os resultados dos pept??deos HHC-10 e IDR-1018 (os quais inibiram o crescimento bacteriano in vitro a concentra????o que apresentou baixa citotoxicidade) foram contrastantes entre os dois modelos de infec????o pulmonar (significando redu????o ou n??o redu????o da carga bacteriana). Outras abordagens utilizando os pept??deos IDR-1018 profilaticamente ou o pept??deo IDR-1002 (efetivo em inibir o crescimento bacteriano in vitro) ap??s a infec????o, tamb??m foram incapazes de reduzir a carga bacteriana em pulm??es de camundongos. Apesar da inefetividade em modelo agudo de infec????o pulmonar, o uso de pept??deos cati??nicos, tal como DJK-6, para potencializar a atividade de ??-lact??micos, incluindo meropenem, representa uma estrat??gia promissora para prevenir a forma????o de biofilmes ou eliminar biofilmes existentes tanto em equipamentos m??dicos quanto em superf??cies do corpo.
description Multi-drug resistant Klebsiella pneumoniae that produce the enzyme K. pneumoniae carbapenemase (KPC) are becoming a common cause of infections in health care centers. Furthermore, Klebsiella can develop multicellular biofilms, which lead to elevated adaptive antibiotic resistance. Here, it was described the antimicrobial and anti-biofilm activities of synthetic cationic peptides against K. pneumoniae strains susceptible and carbapenens resistant through in vitro and in vivo assays. By using static microplate assays, it was observed that the concentration of the peptides IDR-1018, DJK-5 and DJK-6 required to prevent biofilm formation by these clinical isolates was below the minimum inhibitory concentration (MIC) of these peptides. Flow cell experiments confirmed the anti-biofilm activity of the peptides against 2 day-old biofilms of different KPC producing isolates and, in some cases, the peptides induced biofilm cell death. Combinations of DJK-6 together with ??-lactam antibiotics, including the carbapenem meropenem, also prevented planktonic growth and biofilm formation of KPC producing strain 1825971. Interestingly, the peptide DJK-6 was able to enhance, by at least 16-fold, the ability of meropenem to eradicate pre-formed biofilms formed by this strain. Although, this combination between meropenem, DJK-6 was effective in vitro, any reduction of bacterial load was observed in murine lung model of infection. Similarly, the peptides HHC-10, IDR-1018 e IDR-1002 was effective in vitro, but ineffective in vivo. The results in vivo, using the peptides HHC-10 and IDR-1018 after infection were contrasting (significant reduction or non-reduction of bacterial load) between two models of lung infection. Others approaches using the peptides IDR-1018 prophylactically or the peptide IDR-1002 (effective in inhibit bacterial growth) before the induction of the infection, as a preventive approach or IDR-1002 (peptide that reduced the bacterial counts in vitro) after infection, also was unable to reduce the bacterial load in lungs of mice. Despite ineffective in acute model of lung infection, the use of cationic peptides, such DJK-6, to potentiate the activity of ??-lactams including meropenem, represents a promising strategy to prevent biofilm formation or eliminate existent biofilms both in medical devices and in body surfaces.
publishDate 2014
dc.date.issued.fl_str_mv 2014-05-19
dc.date.accessioned.fl_str_mv 2016-12-19T17:56:31Z
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/doctoralThesis
status_str publishedVersion
format doctoralThesis
dc.identifier.citation.fl_str_mv RIBEIRO, Suzana Meira. Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae. 2014. 94f. Tese( Programa Strictu Sensu em Ci??ncias Gen??micas e Biotecnologia) - Universidade Cat??lica de Bras??lia, Bras??lia, 2014.
dc.identifier.uri.fl_str_mv https://bdtd.ucb.br:8443/jspui/handle/tede/1996
identifier_str_mv RIBEIRO, Suzana Meira. Avalia????o da atividade antimicrobiana e antibiofilme de pequenos pept??deos cati??nicos contra Klebsiella pneumoniae. 2014. 94f. Tese( Programa Strictu Sensu em Ci??ncias Gen??micas e Biotecnologia) - Universidade Cat??lica de Bras??lia, Bras??lia, 2014.
url https://bdtd.ucb.br:8443/jspui/handle/tede/1996
dc.language.iso.fl_str_mv por
language por
dc.relation.program.fl_str_mv -2827197273900952156
dc.relation.confidence.fl_str_mv 500
500
600
dc.relation.department.fl_str_mv -6392058866414562720
dc.relation.cnpq.fl_str_mv -5518144268585252051
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 Cat??lica de Bras??lia
dc.publisher.program.fl_str_mv Programa Strictu Sensu em Ci??ncias Gen??micas e Biotecnologia
dc.publisher.initials.fl_str_mv UCB
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