A multi-omic systems approach to elucidating Yersinia virulence mechanisms

A multi-omic systems approach to elucidating Yersinia virulence mechanisms

The underlying mechanisms that lead to dramatic differences between closely related pathogens are not always readily apparent. For example, the genomes of Yersinia pestis (YP) the causative agent of plague with a high mortality rate and Yersinia pseudotuberculosis (YPT) an enteric pathogen with a mo...

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Veröffentlicht in:Molecular bioSystems 2013-01, Vol.9 (1), p.44-54
Hauptverfasser: Ansong, Charles, Schrimpe-Rutledge, Alexandra C, Mitchell, Hugh D, Chauhan, Sadhana, Jones, Marcus B, Kim, Young-Mo, McAteer, Kathleen, Deatherage Kaiser, Brooke L, Dubois, Jennifer L, Brewer, Heather M, Frank, Bryan C, McDermott, Jason E, Metz, Thomas O, Peterson, Scott N, Smith, Richard D, Motin, Vladimir L, Adkins, Joshua N
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Sprache:eng
Schlagworte:
Animals
Body Temperature
Cluster Analysis
Gene Expression Profiling
Glutamic Acid
Host-Pathogen Interactions
Mammals
Models, Biological
Proteomics - methods
Siphonaptera
Transcriptome - genetics
Virulence
Yersinia - genetics
Yersinia - metabolism
Yersinia - pathogenicity
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container_end_page 54
container_issue 1
container_start_page 44
container_title Molecular bioSystems
container_volume 9
creator Ansong, Charles
Schrimpe-Rutledge, Alexandra C
Mitchell, Hugh D
Chauhan, Sadhana
Jones, Marcus B
Kim, Young-Mo
McAteer, Kathleen
Deatherage Kaiser, Brooke L
Dubois, Jennifer L
Brewer, Heather M
Frank, Bryan C
McDermott, Jason E
Metz, Thomas O
Peterson, Scott N
Smith, Richard D
Motin, Vladimir L
Adkins, Joshua N
description The underlying mechanisms that lead to dramatic differences between closely related pathogens are not always readily apparent. For example, the genomes of Yersinia pestis (YP) the causative agent of plague with a high mortality rate and Yersinia pseudotuberculosis (YPT) an enteric pathogen with a modest mortality rate are highly similar with some species specific differences; however the molecular causes of their distinct clinical outcomes remain poorly understood. In this study, a temporal multi-omic analysis of YP and YPT at physiologically relevant temperatures was performed to gain insights into how an acute and highly lethal bacterial pathogen, YP, differs from its less virulent progenitor, YPT. This analysis revealed higher gene and protein expression levels of conserved major virulence factors in YP relative to YPT, including the Yop virulon and the pH6 antigen. This suggests that adaptation in the regulatory architecture, in addition to the presence of unique genetic material, may contribute to the increased pathogenecity of YP relative to YPT. Additionally, global transcriptome and proteome responses of YP and YPT revealed conserved post-transcriptional control of metabolism and the translational machinery including the modulation of glutamate levels in Yersiniae. Finally, the omics data was coupled with a computational network analysis, allowing an efficient prediction of novel Yersinia virulence factors based on gene and protein expression patterns.
doi_str_mv 10.1039/c2mb25287b
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source MEDLINE; Royal Society Of Chemistry Journals 2008-; Alma/SFX Local Collection
subjects Animals
Body Temperature
Cluster Analysis
Gene Expression Profiling
Glutamic Acid
Host-Pathogen Interactions
Mammals
Models, Biological
Proteomics - methods
Siphonaptera
Transcriptome - genetics
Virulence
Yersinia - genetics
Yersinia - metabolism
Yersinia - pathogenicity
title A multi-omic systems approach to elucidating Yersinia virulence mechanisms
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