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Comparative Analyses of Transcriptional Profiles in Mouse Organs Using a Pneumonic Plague Model after Infection with Wild-Type Yersinia pestis CO92 and Its Braun Lipoprotein Mutant

We employed Murine GeneChips to delineate the global transcriptional profiles of the livers, lungs, and spleens in a mouse pneumonic plague infection model with wild-type (WT) Y. pestis CO92 and its Braun lipoprotein (Δl p p) mutant with reduced virulence. These organs showed differential transcript...

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Autores principales: Galindo, Cristi L., Moen, Scott T., Kozlova, Elena V., Sha, Jian, Garner, Harold R., Agar, Stacy L., Chopra, Ashok K.
Formato: Texto
Lenguaje:English
Publicado: Hindawi Publishing Corporation 2009
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2817383/
https://www.ncbi.nlm.nih.gov/pubmed/20145715
http://dx.doi.org/10.1155/2009/914762
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author Galindo, Cristi L.
Moen, Scott T.
Kozlova, Elena V.
Sha, Jian
Garner, Harold R.
Agar, Stacy L.
Chopra, Ashok K.
author_facet Galindo, Cristi L.
Moen, Scott T.
Kozlova, Elena V.
Sha, Jian
Garner, Harold R.
Agar, Stacy L.
Chopra, Ashok K.
author_sort Galindo, Cristi L.
collection PubMed
description We employed Murine GeneChips to delineate the global transcriptional profiles of the livers, lungs, and spleens in a mouse pneumonic plague infection model with wild-type (WT) Y. pestis CO92 and its Braun lipoprotein (Δl p p) mutant with reduced virulence. These organs showed differential transcriptional responses to infection with WT Y. pestis, but the overall host functional processes affected were similar across all three tissues. Gene expression alterations were found in inflammation, cytokine signaling, and apoptotic cell death-associated genes. Comparison of WT and Δl p p mutant-infected mice indicated significant overlap in lipopolysaccharide- (LPS-) associated gene expression, but the absence of Lpp perturbed host cell signaling at critical regulatory junctions resulting in altered immune response and possibly host cell apoptosis. We generated a putative signaling pathway including major inflammatory components that could account for the synergistic action of LPS and Lpp and provided the mechanistic basis of attenuation caused by deletion of the lpp gene from Y. pestis in a mouse model of pneumonic plague.
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spelling pubmed-28173832010-02-09 Comparative Analyses of Transcriptional Profiles in Mouse Organs Using a Pneumonic Plague Model after Infection with Wild-Type Yersinia pestis CO92 and Its Braun Lipoprotein Mutant Galindo, Cristi L. Moen, Scott T. Kozlova, Elena V. Sha, Jian Garner, Harold R. Agar, Stacy L. Chopra, Ashok K. Comp Funct Genomics Research Article We employed Murine GeneChips to delineate the global transcriptional profiles of the livers, lungs, and spleens in a mouse pneumonic plague infection model with wild-type (WT) Y. pestis CO92 and its Braun lipoprotein (Δl p p) mutant with reduced virulence. These organs showed differential transcriptional responses to infection with WT Y. pestis, but the overall host functional processes affected were similar across all three tissues. Gene expression alterations were found in inflammation, cytokine signaling, and apoptotic cell death-associated genes. Comparison of WT and Δl p p mutant-infected mice indicated significant overlap in lipopolysaccharide- (LPS-) associated gene expression, but the absence of Lpp perturbed host cell signaling at critical regulatory junctions resulting in altered immune response and possibly host cell apoptosis. We generated a putative signaling pathway including major inflammatory components that could account for the synergistic action of LPS and Lpp and provided the mechanistic basis of attenuation caused by deletion of the lpp gene from Y. pestis in a mouse model of pneumonic plague. Hindawi Publishing Corporation 2009 2010-01-20 /pmc/articles/PMC2817383/ /pubmed/20145715 http://dx.doi.org/10.1155/2009/914762 Text en Copyright © 2009 Cristi L. Galindo et al. https://creativecommons.org/licenses/by/3.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Galindo, Cristi L.
Moen, Scott T.
Kozlova, Elena V.
Sha, Jian
Garner, Harold R.
Agar, Stacy L.
Chopra, Ashok K.
Comparative Analyses of Transcriptional Profiles in Mouse Organs Using a Pneumonic Plague Model after Infection with Wild-Type Yersinia pestis CO92 and Its Braun Lipoprotein Mutant
title Comparative Analyses of Transcriptional Profiles in Mouse Organs Using a Pneumonic Plague Model after Infection with Wild-Type Yersinia pestis CO92 and Its Braun Lipoprotein Mutant
title_full Comparative Analyses of Transcriptional Profiles in Mouse Organs Using a Pneumonic Plague Model after Infection with Wild-Type Yersinia pestis CO92 and Its Braun Lipoprotein Mutant
title_fullStr Comparative Analyses of Transcriptional Profiles in Mouse Organs Using a Pneumonic Plague Model after Infection with Wild-Type Yersinia pestis CO92 and Its Braun Lipoprotein Mutant
title_full_unstemmed Comparative Analyses of Transcriptional Profiles in Mouse Organs Using a Pneumonic Plague Model after Infection with Wild-Type Yersinia pestis CO92 and Its Braun Lipoprotein Mutant
title_short Comparative Analyses of Transcriptional Profiles in Mouse Organs Using a Pneumonic Plague Model after Infection with Wild-Type Yersinia pestis CO92 and Its Braun Lipoprotein Mutant
title_sort comparative analyses of transcriptional profiles in mouse organs using a pneumonic plague model after infection with wild-type yersinia pestis co92 and its braun lipoprotein mutant
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2817383/
https://www.ncbi.nlm.nih.gov/pubmed/20145715
http://dx.doi.org/10.1155/2009/914762
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