Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages

Detalhes bibliográficos
Autor(a) principal: Tavares, Aldo Henrique F.P.
Data de Publicação: 2007
Outros Autores: Silva, Simoneide S., Dantas, Alessandra, Campos, Élida G., Andrade, Rosângela V., Maranhão, Andréa Q., Brígido, Marcelo M., Passos-Silva, Danielle G., Fachin, Ana L., Teixeira, Santuza M.R., Passos, Geraldo A.S., Soares, Célia M.A., Bocca, Anamélia L., Carvalho, Maria Jose´ A., Silva-Pereira, Ildinete, Felipe, Maria Sueli S.
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Institucional da UCB
Texto Completo: http://twingo.ucb.br:8080/jspui/handle/10869/399
https://repositorio.ucb.br:9443/jspui/handle/123456789/7583
Resumo: Paracoccidioides brasiliensis, a thermal dimorphic fungus, is the etiologic agent of the most common systemic mycosis in Latin America, aracoccidioidomycosis. The yeast form of P. brasiliensis acts as a facultative intracellular pathogen being able to survive and replicate within the phagosome of nonactivated murine and human macrophages. This ability has been proposed to be crucial to the development of disease. Thus, P. brasiliensis may have evolved mechanisms that counteract the constraints imposed by phagocytic cells. By using cDNA microarray technology we evaluated the early transcriptional response of this fungus to the environment of peritoneal murine macrophages in order to shed light on the mechanisms used by P. brasiliensis to survive within phagocytic cells. Of the 1152 genes analyzed, we identified 152 genes that were differentially transcribed. Intracellularly expressed genes were primarily associated with glucose and amino acid limitation, cell wall construction, and oxidative stress. For the first time, a comprehensive gene expression tool is used for the expression analysis of P. brasiliensis genes when interacting with macrophages. Overall, our data show a transcriptional plasticity of P. brasiliensis in response to the harsh environment of macrophages which may lead to adaptation and consequent survival of this pathogen.
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spelling Tavares, Aldo Henrique F.P.Silva, Simoneide S.Dantas, AlessandraCampos, Élida G.Andrade, Rosângela V.Maranhão, Andréa Q.Brígido, Marcelo M.Passos-Silva, Danielle G.Fachin, Ana L.Teixeira, Santuza M.R.Passos, Geraldo A.S.Soares, Célia M.A.Bocca, Anamélia L.Carvalho, Maria Jose´ A.Silva-Pereira, IldineteFelipe, Maria Sueli S.2016-10-10T03:51:58Z2016-10-10T03:51:58Z2007TAVARES, Aldo Henrique F. P. et al. Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages. Microbes and Infection, v. 9, p. 583-590, 2007.12864579http://twingo.ucb.br:8080/jspui/handle/10869/399https://repositorio.ucb.br:9443/jspui/handle/123456789/7583Paracoccidioides brasiliensis, a thermal dimorphic fungus, is the etiologic agent of the most common systemic mycosis in Latin America, aracoccidioidomycosis. The yeast form of P. brasiliensis acts as a facultative intracellular pathogen being able to survive and replicate within the phagosome of nonactivated murine and human macrophages. This ability has been proposed to be crucial to the development of disease. Thus, P. brasiliensis may have evolved mechanisms that counteract the constraints imposed by phagocytic cells. By using cDNA microarray technology we evaluated the early transcriptional response of this fungus to the environment of peritoneal murine macrophages in order to shed light on the mechanisms used by P. brasiliensis to survive within phagocytic cells. Of the 1152 genes analyzed, we identified 152 genes that were differentially transcribed. Intracellularly expressed genes were primarily associated with glucose and amino acid limitation, cell wall construction, and oxidative stress. For the first time, a comprehensive gene expression tool is used for the expression analysis of P. brasiliensis genes when interacting with macrophages. Overall, our data show a transcriptional plasticity of P. brasiliensis in response to the harsh environment of macrophages which may lead to adaptation and consequent survival of this pathogen.Made available in DSpace on 2016-10-10T03:51:58Z (GMT). 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dc.title.pt_BR.fl_str_mv Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages
title Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages
spellingShingle Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages
Tavares, Aldo Henrique F.P.
Paracoccidioides brasiliensis
Intracellular
Macrophage
Microarray
title_short Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages
title_full Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages
title_fullStr Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages
title_full_unstemmed Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages
title_sort Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages
author Tavares, Aldo Henrique F.P.
author_facet Tavares, Aldo Henrique F.P.
Silva, Simoneide S.
Dantas, Alessandra
Campos, Élida G.
Andrade, Rosângela V.
Maranhão, Andréa Q.
Brígido, Marcelo M.
Passos-Silva, Danielle G.
Fachin, Ana L.
Teixeira, Santuza M.R.
Passos, Geraldo A.S.
Soares, Célia M.A.
Bocca, Anamélia L.
Carvalho, Maria Jose´ A.
Silva-Pereira, Ildinete
Felipe, Maria Sueli S.
author_role author
author2 Silva, Simoneide S.
Dantas, Alessandra
Campos, Élida G.
Andrade, Rosângela V.
Maranhão, Andréa Q.
Brígido, Marcelo M.
Passos-Silva, Danielle G.
Fachin, Ana L.
Teixeira, Santuza M.R.
Passos, Geraldo A.S.
Soares, Célia M.A.
Bocca, Anamélia L.
Carvalho, Maria Jose´ A.
Silva-Pereira, Ildinete
Felipe, Maria Sueli S.
author2_role author
author
author
author
author
author
author
author
author
author
author
author
author
author
author
dc.contributor.author.fl_str_mv Tavares, Aldo Henrique F.P.
Silva, Simoneide S.
Dantas, Alessandra
Campos, Élida G.
Andrade, Rosângela V.
Maranhão, Andréa Q.
Brígido, Marcelo M.
Passos-Silva, Danielle G.
Fachin, Ana L.
Teixeira, Santuza M.R.
Passos, Geraldo A.S.
Soares, Célia M.A.
Bocca, Anamélia L.
Carvalho, Maria Jose´ A.
Silva-Pereira, Ildinete
Felipe, Maria Sueli S.
dc.subject.por.fl_str_mv Paracoccidioides brasiliensis
Intracellular
Macrophage
Microarray
topic Paracoccidioides brasiliensis
Intracellular
Macrophage
Microarray
dc.description.abstract.por.fl_txt_mv Paracoccidioides brasiliensis, a thermal dimorphic fungus, is the etiologic agent of the most common systemic mycosis in Latin America, aracoccidioidomycosis. The yeast form of P. brasiliensis acts as a facultative intracellular pathogen being able to survive and replicate within the phagosome of nonactivated murine and human macrophages. This ability has been proposed to be crucial to the development of disease. Thus, P. brasiliensis may have evolved mechanisms that counteract the constraints imposed by phagocytic cells. By using cDNA microarray technology we evaluated the early transcriptional response of this fungus to the environment of peritoneal murine macrophages in order to shed light on the mechanisms used by P. brasiliensis to survive within phagocytic cells. Of the 1152 genes analyzed, we identified 152 genes that were differentially transcribed. Intracellularly expressed genes were primarily associated with glucose and amino acid limitation, cell wall construction, and oxidative stress. For the first time, a comprehensive gene expression tool is used for the expression analysis of P. brasiliensis genes when interacting with macrophages. Overall, our data show a transcriptional plasticity of P. brasiliensis in response to the harsh environment of macrophages which may lead to adaptation and consequent survival of this pathogen.
dc.description.status.pt_BR.fl_txt_mv Publicado
description Paracoccidioides brasiliensis, a thermal dimorphic fungus, is the etiologic agent of the most common systemic mycosis in Latin America, aracoccidioidomycosis. The yeast form of P. brasiliensis acts as a facultative intracellular pathogen being able to survive and replicate within the phagosome of nonactivated murine and human macrophages. This ability has been proposed to be crucial to the development of disease. Thus, P. brasiliensis may have evolved mechanisms that counteract the constraints imposed by phagocytic cells. By using cDNA microarray technology we evaluated the early transcriptional response of this fungus to the environment of peritoneal murine macrophages in order to shed light on the mechanisms used by P. brasiliensis to survive within phagocytic cells. Of the 1152 genes analyzed, we identified 152 genes that were differentially transcribed. Intracellularly expressed genes were primarily associated with glucose and amino acid limitation, cell wall construction, and oxidative stress. For the first time, a comprehensive gene expression tool is used for the expression analysis of P. brasiliensis genes when interacting with macrophages. Overall, our data show a transcriptional plasticity of P. brasiliensis in response to the harsh environment of macrophages which may lead to adaptation and consequent survival of this pathogen.
publishDate 2007
dc.date.issued.fl_str_mv 2007
dc.date.accessioned.fl_str_mv 2016-10-10T03:51:58Z
dc.date.available.fl_str_mv 2016-10-10T03:51:58Z
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
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dc.identifier.citation.fl_str_mv TAVARES, Aldo Henrique F. P. et al. Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages. Microbes and Infection, v. 9, p. 583-590, 2007.
dc.identifier.uri.fl_str_mv http://twingo.ucb.br:8080/jspui/handle/10869/399
https://repositorio.ucb.br:9443/jspui/handle/123456789/7583
dc.identifier.issn.none.fl_str_mv 12864579
identifier_str_mv TAVARES, Aldo Henrique F. P. et al. Early transcriptional response of paracoccidioides brasiliensis upon internalization by murine macrophages. Microbes and Infection, v. 9, p. 583-590, 2007.
12864579
url http://twingo.ucb.br:8080/jspui/handle/10869/399
https://repositorio.ucb.br:9443/jspui/handle/123456789/7583
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