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Fimbriae reprogram host gene expression – Divergent effects of P and type 1 fimbriae

Pathogens rely on a complex virulence gene repertoire to successfully attack their hosts. We were therefore surprised to find that a single fimbrial gene reconstitution can return the virulence-attenuated commensal strain Escherichia coli 83972 to virulence, defined by a disease phenotype in human h...

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Autores principales: Ambite, Ines, Butler, Daniel S. C., Stork, Christoph, Grönberg-Hernández, Jenny, Köves, Bela, Zdziarski, Jaroslaw, Pinkner, Jerome, Hultgren, Scott J., Dobrindt, Ulrich, Wullt, Björn, Svanborg, Catharina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6557620/
https://www.ncbi.nlm.nih.gov/pubmed/31181116
http://dx.doi.org/10.1371/journal.ppat.1007671
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author Ambite, Ines
Butler, Daniel S. C.
Stork, Christoph
Grönberg-Hernández, Jenny
Köves, Bela
Zdziarski, Jaroslaw
Pinkner, Jerome
Hultgren, Scott J.
Dobrindt, Ulrich
Wullt, Björn
Svanborg, Catharina
author_facet Ambite, Ines
Butler, Daniel S. C.
Stork, Christoph
Grönberg-Hernández, Jenny
Köves, Bela
Zdziarski, Jaroslaw
Pinkner, Jerome
Hultgren, Scott J.
Dobrindt, Ulrich
Wullt, Björn
Svanborg, Catharina
author_sort Ambite, Ines
collection PubMed
description Pathogens rely on a complex virulence gene repertoire to successfully attack their hosts. We were therefore surprised to find that a single fimbrial gene reconstitution can return the virulence-attenuated commensal strain Escherichia coli 83972 to virulence, defined by a disease phenotype in human hosts. E. coli 83972pap stably reprogrammed host gene expression, by activating an acute pyelonephritis-associated, IRF7-dependent gene network. The PapG protein was internalized by human kidney cells and served as a transcriptional agonist of IRF-7, IFN-β and MYC, suggesting direct involvement of the fimbrial adhesin in this process. IRF-7 was further identified as a potent upstream regulator (-log (p-value) = 61), consistent with the effects in inoculated patients. In contrast, E. coli 83972fim transiently attenuated overall gene expression in human hosts, enhancing the effects of E. coli 83972. The inhibition of RNA processing and ribosomal assembly indicated a homeostatic rather than a pathogenic end-point. In parallel, the expression of specific ion channels and neuropeptide gene networks was transiently enhanced, in a FimH-dependent manner. The studies were performed to establish protective asymptomatic bacteriuria in human hosts and the reconstituted E. coli 83972 variants were developed to improve bacterial fitness for the human urinary tract. Unexpectedly, P fimbriae were able to drive a disease response, suggesting that like oncogene addiction in cancer, pathogens may be addicted to single super-virulence factors.
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spelling pubmed-65576202019-06-17 Fimbriae reprogram host gene expression – Divergent effects of P and type 1 fimbriae Ambite, Ines Butler, Daniel S. C. Stork, Christoph Grönberg-Hernández, Jenny Köves, Bela Zdziarski, Jaroslaw Pinkner, Jerome Hultgren, Scott J. Dobrindt, Ulrich Wullt, Björn Svanborg, Catharina PLoS Pathog Research Article Pathogens rely on a complex virulence gene repertoire to successfully attack their hosts. We were therefore surprised to find that a single fimbrial gene reconstitution can return the virulence-attenuated commensal strain Escherichia coli 83972 to virulence, defined by a disease phenotype in human hosts. E. coli 83972pap stably reprogrammed host gene expression, by activating an acute pyelonephritis-associated, IRF7-dependent gene network. The PapG protein was internalized by human kidney cells and served as a transcriptional agonist of IRF-7, IFN-β and MYC, suggesting direct involvement of the fimbrial adhesin in this process. IRF-7 was further identified as a potent upstream regulator (-log (p-value) = 61), consistent with the effects in inoculated patients. In contrast, E. coli 83972fim transiently attenuated overall gene expression in human hosts, enhancing the effects of E. coli 83972. The inhibition of RNA processing and ribosomal assembly indicated a homeostatic rather than a pathogenic end-point. In parallel, the expression of specific ion channels and neuropeptide gene networks was transiently enhanced, in a FimH-dependent manner. The studies were performed to establish protective asymptomatic bacteriuria in human hosts and the reconstituted E. coli 83972 variants were developed to improve bacterial fitness for the human urinary tract. Unexpectedly, P fimbriae were able to drive a disease response, suggesting that like oncogene addiction in cancer, pathogens may be addicted to single super-virulence factors. Public Library of Science 2019-06-10 /pmc/articles/PMC6557620/ /pubmed/31181116 http://dx.doi.org/10.1371/journal.ppat.1007671 Text en © 2019 Ambite et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Ambite, Ines
Butler, Daniel S. C.
Stork, Christoph
Grönberg-Hernández, Jenny
Köves, Bela
Zdziarski, Jaroslaw
Pinkner, Jerome
Hultgren, Scott J.
Dobrindt, Ulrich
Wullt, Björn
Svanborg, Catharina
Fimbriae reprogram host gene expression – Divergent effects of P and type 1 fimbriae
title Fimbriae reprogram host gene expression – Divergent effects of P and type 1 fimbriae
title_full Fimbriae reprogram host gene expression – Divergent effects of P and type 1 fimbriae
title_fullStr Fimbriae reprogram host gene expression – Divergent effects of P and type 1 fimbriae
title_full_unstemmed Fimbriae reprogram host gene expression – Divergent effects of P and type 1 fimbriae
title_short Fimbriae reprogram host gene expression – Divergent effects of P and type 1 fimbriae
title_sort fimbriae reprogram host gene expression – divergent effects of p and type 1 fimbriae
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6557620/
https://www.ncbi.nlm.nih.gov/pubmed/31181116
http://dx.doi.org/10.1371/journal.ppat.1007671
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