Type IV pilus retraction enables sustained bacteremia and plays a key role in the outcome of meningococcal sepsis in a humanized mouse model

Neisseria meningitidis (the meningococcus) remains a major cause of bacterial meningitis and fatal sepsis. This commensal bacterium of the human nasopharynx can cause invasive diseases when it leaves its niche and reaches the bloodstream. Blood-borne meningococci have the ability to adhere to human...

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Autores principales: Barnier, Jean-Philippe, Euphrasie, Daniel, Join-Lambert, Olivier, Audry, Mathilde, Schonherr-Hellec, Sophia, Schmitt, Taliah, Bourdoulous, Sandrine, Coureuil, Mathieu, Nassif, Xavier, El Behi, Mohamed
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/PMC7909687/
https://www.ncbi.nlm.nih.gov/pubmed/33592056
http://dx.doi.org/10.1371/journal.ppat.1009299
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author Barnier, Jean-Philippe
Euphrasie, Daniel
Join-Lambert, Olivier
Audry, Mathilde
Schonherr-Hellec, Sophia
Schmitt, Taliah
Bourdoulous, Sandrine
Coureuil, Mathieu
Nassif, Xavier
El Behi, Mohamed
author_facet Barnier, Jean-Philippe
Euphrasie, Daniel
Join-Lambert, Olivier
Audry, Mathilde
Schonherr-Hellec, Sophia
Schmitt, Taliah
Bourdoulous, Sandrine
Coureuil, Mathieu
Nassif, Xavier
El Behi, Mohamed
author_sort Barnier, Jean-Philippe
collection PubMed
description Neisseria meningitidis (the meningococcus) remains a major cause of bacterial meningitis and fatal sepsis. This commensal bacterium of the human nasopharynx can cause invasive diseases when it leaves its niche and reaches the bloodstream. Blood-borne meningococci have the ability to adhere to human endothelial cells and rapidly colonize microvessels. This crucial step enables dissemination into tissues and promotes deregulated inflammation and coagulation, leading to extensive necrotic purpura in the most severe cases. Adhesion to blood vessels relies on type IV pili (TFP). These long filamentous structures are highly dynamic as they can rapidly elongate and retract by the antagonistic action of two ATPases, PilF and PilT. However, the consequences of TFP dynamics on the pathophysiology and the outcome of meningococcal sepsis in vivo have been poorly studied. Here, we show that human graft microvessels are replicative niches for meningococci, that seed the bloodstream and promote sustained bacteremia and lethality in a humanized mouse model. Intriguingly, although pilus-retraction deficient N. meningitidis strain (ΔpilT) efficiently colonizes human graft tissue, this mutant did not promote sustained bacteremia nor induce mouse lethality. This effect was not due to a decreased inflammatory response, nor defects in bacterial clearance by the innate immune system. Rather, TFP-retraction was necessary to promote the release of TFP-dependent contacts between bacteria and, in turn, the detachment from colonized microvessels. The resulting sustained bacteremia was directly correlated with lethality. Altogether, these results demonstrate that pilus retraction plays a key role in the occurrence and outcome of meningococcal sepsis by supporting sustained bacteremia. These findings open new perspectives on the role of circulating bacteria in the pathological alterations leading to lethal sepsis.
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spelling pubmed-79096872021-03-05 Type IV pilus retraction enables sustained bacteremia and plays a key role in the outcome of meningococcal sepsis in a humanized mouse model Barnier, Jean-Philippe Euphrasie, Daniel Join-Lambert, Olivier Audry, Mathilde Schonherr-Hellec, Sophia Schmitt, Taliah Bourdoulous, Sandrine Coureuil, Mathieu Nassif, Xavier El Behi, Mohamed PLoS Pathog Research Article Neisseria meningitidis (the meningococcus) remains a major cause of bacterial meningitis and fatal sepsis. This commensal bacterium of the human nasopharynx can cause invasive diseases when it leaves its niche and reaches the bloodstream. Blood-borne meningococci have the ability to adhere to human endothelial cells and rapidly colonize microvessels. This crucial step enables dissemination into tissues and promotes deregulated inflammation and coagulation, leading to extensive necrotic purpura in the most severe cases. Adhesion to blood vessels relies on type IV pili (TFP). These long filamentous structures are highly dynamic as they can rapidly elongate and retract by the antagonistic action of two ATPases, PilF and PilT. However, the consequences of TFP dynamics on the pathophysiology and the outcome of meningococcal sepsis in vivo have been poorly studied. Here, we show that human graft microvessels are replicative niches for meningococci, that seed the bloodstream and promote sustained bacteremia and lethality in a humanized mouse model. Intriguingly, although pilus-retraction deficient N. meningitidis strain (ΔpilT) efficiently colonizes human graft tissue, this mutant did not promote sustained bacteremia nor induce mouse lethality. This effect was not due to a decreased inflammatory response, nor defects in bacterial clearance by the innate immune system. Rather, TFP-retraction was necessary to promote the release of TFP-dependent contacts between bacteria and, in turn, the detachment from colonized microvessels. The resulting sustained bacteremia was directly correlated with lethality. Altogether, these results demonstrate that pilus retraction plays a key role in the occurrence and outcome of meningococcal sepsis by supporting sustained bacteremia. These findings open new perspectives on the role of circulating bacteria in the pathological alterations leading to lethal sepsis. Public Library of Science 2021-02-16 /pmc/articles/PMC7909687/ /pubmed/33592056 http://dx.doi.org/10.1371/journal.ppat.1009299 Text en © 2021 Barnier 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
Barnier, Jean-Philippe
Euphrasie, Daniel
Join-Lambert, Olivier
Audry, Mathilde
Schonherr-Hellec, Sophia
Schmitt, Taliah
Bourdoulous, Sandrine
Coureuil, Mathieu
Nassif, Xavier
El Behi, Mohamed
Type IV pilus retraction enables sustained bacteremia and plays a key role in the outcome of meningococcal sepsis in a humanized mouse model
title Type IV pilus retraction enables sustained bacteremia and plays a key role in the outcome of meningococcal sepsis in a humanized mouse model
title_full Type IV pilus retraction enables sustained bacteremia and plays a key role in the outcome of meningococcal sepsis in a humanized mouse model
title_fullStr Type IV pilus retraction enables sustained bacteremia and plays a key role in the outcome of meningococcal sepsis in a humanized mouse model
title_full_unstemmed Type IV pilus retraction enables sustained bacteremia and plays a key role in the outcome of meningococcal sepsis in a humanized mouse model
title_short Type IV pilus retraction enables sustained bacteremia and plays a key role in the outcome of meningococcal sepsis in a humanized mouse model
title_sort type iv pilus retraction enables sustained bacteremia and plays a key role in the outcome of meningococcal sepsis in a humanized mouse model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7909687/
https://www.ncbi.nlm.nih.gov/pubmed/33592056
http://dx.doi.org/10.1371/journal.ppat.1009299
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