A plasmid locus associated with Klebsiella clinical infections encodes a microbiome-dependent gut fitness factor

Klebsiella pneumoniae (Kp) is an important cause of healthcare-associated infections, which increases patient morbidity, mortality, and hospitalization costs. Gut colonization by Kp is consistently associated with subsequent Kp disease, and patients are predominantly infected with their colonizing s...

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Autores principales: Vornhagen, Jay, Bassis, Christine M., Ramakrishnan, Srividya, Hein, Robert, Mason, Sophia, Bergman, Yehudit, Sunshine, Nicole, Fan, Yunfan, Holmes, Caitlyn L., Timp, Winston, Schatz, Michael C., Young, Vincent B., Simner, Patricia J., Bachman, Michael A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8115787/
https://www.ncbi.nlm.nih.gov/pubmed/33930099
http://dx.doi.org/10.1371/journal.ppat.1009537
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author Vornhagen, Jay
Bassis, Christine M.
Ramakrishnan, Srividya
Hein, Robert
Mason, Sophia
Bergman, Yehudit
Sunshine, Nicole
Fan, Yunfan
Holmes, Caitlyn L.
Timp, Winston
Schatz, Michael C.
Young, Vincent B.
Simner, Patricia J.
Bachman, Michael A.
author_facet Vornhagen, Jay
Bassis, Christine M.
Ramakrishnan, Srividya
Hein, Robert
Mason, Sophia
Bergman, Yehudit
Sunshine, Nicole
Fan, Yunfan
Holmes, Caitlyn L.
Timp, Winston
Schatz, Michael C.
Young, Vincent B.
Simner, Patricia J.
Bachman, Michael A.
author_sort Vornhagen, Jay
collection PubMed
description Klebsiella pneumoniae (Kp) is an important cause of healthcare-associated infections, which increases patient morbidity, mortality, and hospitalization costs. Gut colonization by Kp is consistently associated with subsequent Kp disease, and patients are predominantly infected with their colonizing strain. Our previous comparative genomics study, between disease-causing and asymptomatically colonizing Kp isolates, identified a plasmid-encoded tellurite (TeO(3)(-2))-resistance (ter) operon as strongly associated with infection. However, TeO(3)(-2) is extremely rare and toxic to humans. Thus, we used a multidisciplinary approach to determine the biological link between ter and Kp infection. First, we used a genomic and bioinformatic approach to extensively characterize Kp plasmids encoding the ter locus. These plasmids displayed substantial variation in plasmid incompatibility type and gene content. Moreover, the ter operon was genetically independent of other plasmid-encoded virulence and antibiotic resistance loci, both in our original patient cohort and in a large set (n = 88) of publicly available ter operon-encoding Kp plasmids, indicating that the ter operon is likely playing a direct, but yet undescribed role in Kp disease. Next, we employed multiple mouse models of infection and colonization to show that 1) the ter operon is dispensable during bacteremia, 2) the ter operon enhances fitness in the gut, 3) this phenotype is dependent on the colony of origin of mice, and 4) antibiotic disruption of the gut microbiota eliminates the requirement for ter. Furthermore, using 16S rRNA gene sequencing, we show that the ter operon enhances Kp fitness in the gut in the presence of specific indigenous microbiota, including those predicted to produce short chain fatty acids. Finally, administration of exogenous short-chain fatty acids in our mouse model of colonization was sufficient to reduce fitness of a ter mutant. These findings indicate that the ter operon, strongly associated with human infection, encodes factors that resist stress induced by the indigenous gut microbiota during colonization. This work represents a substantial advancement in our molecular understanding of Kp pathogenesis and gut colonization, directly relevant to Kp disease in healthcare settings.
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spelling pubmed-81157872021-05-24 A plasmid locus associated with Klebsiella clinical infections encodes a microbiome-dependent gut fitness factor Vornhagen, Jay Bassis, Christine M. Ramakrishnan, Srividya Hein, Robert Mason, Sophia Bergman, Yehudit Sunshine, Nicole Fan, Yunfan Holmes, Caitlyn L. Timp, Winston Schatz, Michael C. Young, Vincent B. Simner, Patricia J. Bachman, Michael A. PLoS Pathog Research Article Klebsiella pneumoniae (Kp) is an important cause of healthcare-associated infections, which increases patient morbidity, mortality, and hospitalization costs. Gut colonization by Kp is consistently associated with subsequent Kp disease, and patients are predominantly infected with their colonizing strain. Our previous comparative genomics study, between disease-causing and asymptomatically colonizing Kp isolates, identified a plasmid-encoded tellurite (TeO(3)(-2))-resistance (ter) operon as strongly associated with infection. However, TeO(3)(-2) is extremely rare and toxic to humans. Thus, we used a multidisciplinary approach to determine the biological link between ter and Kp infection. First, we used a genomic and bioinformatic approach to extensively characterize Kp plasmids encoding the ter locus. These plasmids displayed substantial variation in plasmid incompatibility type and gene content. Moreover, the ter operon was genetically independent of other plasmid-encoded virulence and antibiotic resistance loci, both in our original patient cohort and in a large set (n = 88) of publicly available ter operon-encoding Kp plasmids, indicating that the ter operon is likely playing a direct, but yet undescribed role in Kp disease. Next, we employed multiple mouse models of infection and colonization to show that 1) the ter operon is dispensable during bacteremia, 2) the ter operon enhances fitness in the gut, 3) this phenotype is dependent on the colony of origin of mice, and 4) antibiotic disruption of the gut microbiota eliminates the requirement for ter. Furthermore, using 16S rRNA gene sequencing, we show that the ter operon enhances Kp fitness in the gut in the presence of specific indigenous microbiota, including those predicted to produce short chain fatty acids. Finally, administration of exogenous short-chain fatty acids in our mouse model of colonization was sufficient to reduce fitness of a ter mutant. These findings indicate that the ter operon, strongly associated with human infection, encodes factors that resist stress induced by the indigenous gut microbiota during colonization. This work represents a substantial advancement in our molecular understanding of Kp pathogenesis and gut colonization, directly relevant to Kp disease in healthcare settings. Public Library of Science 2021-04-30 /pmc/articles/PMC8115787/ /pubmed/33930099 http://dx.doi.org/10.1371/journal.ppat.1009537 Text en © 2021 Vornhagen et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://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
Vornhagen, Jay
Bassis, Christine M.
Ramakrishnan, Srividya
Hein, Robert
Mason, Sophia
Bergman, Yehudit
Sunshine, Nicole
Fan, Yunfan
Holmes, Caitlyn L.
Timp, Winston
Schatz, Michael C.
Young, Vincent B.
Simner, Patricia J.
Bachman, Michael A.
A plasmid locus associated with Klebsiella clinical infections encodes a microbiome-dependent gut fitness factor
title A plasmid locus associated with Klebsiella clinical infections encodes a microbiome-dependent gut fitness factor
title_full A plasmid locus associated with Klebsiella clinical infections encodes a microbiome-dependent gut fitness factor
title_fullStr A plasmid locus associated with Klebsiella clinical infections encodes a microbiome-dependent gut fitness factor
title_full_unstemmed A plasmid locus associated with Klebsiella clinical infections encodes a microbiome-dependent gut fitness factor
title_short A plasmid locus associated with Klebsiella clinical infections encodes a microbiome-dependent gut fitness factor
title_sort plasmid locus associated with klebsiella clinical infections encodes a microbiome-dependent gut fitness factor
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8115787/
https://www.ncbi.nlm.nih.gov/pubmed/33930099
http://dx.doi.org/10.1371/journal.ppat.1009537
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