The Arginine Decarboxylase Pathways of Host and Pathogen Interact to Impact Inflammatory Pathways in the Lung

The arginine decarboxylase pathway, which converts arginine to agmatine, is present in both humans and most bacterial pathogens. In humans agmatine is a neurotransmitter with affinities towards α2-adrenoreceptors, serotonin receptors, and may inhibit nitric oxide synthase. In bacteria agmatine serve...

Descripción completa

Detalles Bibliográficos
Autores principales: Paulson, Nick B., Gilbertsen, Adam J., Dalluge, Joseph J., Welchlin, Cole W., Hughes, John, Han, Wei, Blackwell, Timothy S., Laguna, Theresa A., Williams, Bryan J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4211729/
https://www.ncbi.nlm.nih.gov/pubmed/25350753
http://dx.doi.org/10.1371/journal.pone.0111441
_version_ 1782341621714518016
author Paulson, Nick B.
Gilbertsen, Adam J.
Dalluge, Joseph J.
Welchlin, Cole W.
Hughes, John
Han, Wei
Blackwell, Timothy S.
Laguna, Theresa A.
Williams, Bryan J.
author_facet Paulson, Nick B.
Gilbertsen, Adam J.
Dalluge, Joseph J.
Welchlin, Cole W.
Hughes, John
Han, Wei
Blackwell, Timothy S.
Laguna, Theresa A.
Williams, Bryan J.
author_sort Paulson, Nick B.
collection PubMed
description The arginine decarboxylase pathway, which converts arginine to agmatine, is present in both humans and most bacterial pathogens. In humans agmatine is a neurotransmitter with affinities towards α2-adrenoreceptors, serotonin receptors, and may inhibit nitric oxide synthase. In bacteria agmatine serves as a precursor to polyamine synthesis and was recently shown to enhance biofilm development in some strains of the respiratory pathogen Pseudomonas aeruginosa. We determined agmatine is at the center of a competing metabolism in the human lung during airways infections and is influenced by the metabolic phenotypes of the infecting pathogens. Ultra performance liquid chromatography with mass spectrometry detection was used to measure agmatine in human sputum samples from patients with cystic fibrosis, spent supernatant from clinical sputum isolates, and from bronchoalvelolar lavage fluid from mice infected with P. aeruginosa agmatine mutants. Agmatine in human sputum peaks during illness, decreased with treatment and is positively correlated with inflammatory cytokines. Analysis of the agmatine metabolic phenotype in clinical sputum isolates revealed most deplete agmatine when grown in its presence; however a minority appeared to generate large amounts of agmatine presumably driving sputum agmatine to high levels. Agmatine exposure to inflammatory cells and in mice demonstrated its role as a direct immune activator with effects on TNF-α production, likely through NF-κB activation. P. aeruginosa mutants for agmatine detection and metabolism were constructed and show the real-time evolution of host-derived agmatine in the airways during acute lung infection. These experiments also demonstrated pathogen agmatine production can upregulate the inflammatory response. As some clinical isolates have adapted to hypersecrete agmatine, these combined data would suggest agmatine is a novel target for immune modulation in the host-pathogen dynamic.
format Online
Article
Text
id pubmed-4211729
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-42117292014-11-05 The Arginine Decarboxylase Pathways of Host and Pathogen Interact to Impact Inflammatory Pathways in the Lung Paulson, Nick B. Gilbertsen, Adam J. Dalluge, Joseph J. Welchlin, Cole W. Hughes, John Han, Wei Blackwell, Timothy S. Laguna, Theresa A. Williams, Bryan J. PLoS One Research Article The arginine decarboxylase pathway, which converts arginine to agmatine, is present in both humans and most bacterial pathogens. In humans agmatine is a neurotransmitter with affinities towards α2-adrenoreceptors, serotonin receptors, and may inhibit nitric oxide synthase. In bacteria agmatine serves as a precursor to polyamine synthesis and was recently shown to enhance biofilm development in some strains of the respiratory pathogen Pseudomonas aeruginosa. We determined agmatine is at the center of a competing metabolism in the human lung during airways infections and is influenced by the metabolic phenotypes of the infecting pathogens. Ultra performance liquid chromatography with mass spectrometry detection was used to measure agmatine in human sputum samples from patients with cystic fibrosis, spent supernatant from clinical sputum isolates, and from bronchoalvelolar lavage fluid from mice infected with P. aeruginosa agmatine mutants. Agmatine in human sputum peaks during illness, decreased with treatment and is positively correlated with inflammatory cytokines. Analysis of the agmatine metabolic phenotype in clinical sputum isolates revealed most deplete agmatine when grown in its presence; however a minority appeared to generate large amounts of agmatine presumably driving sputum agmatine to high levels. Agmatine exposure to inflammatory cells and in mice demonstrated its role as a direct immune activator with effects on TNF-α production, likely through NF-κB activation. P. aeruginosa mutants for agmatine detection and metabolism were constructed and show the real-time evolution of host-derived agmatine in the airways during acute lung infection. These experiments also demonstrated pathogen agmatine production can upregulate the inflammatory response. As some clinical isolates have adapted to hypersecrete agmatine, these combined data would suggest agmatine is a novel target for immune modulation in the host-pathogen dynamic. Public Library of Science 2014-10-28 /pmc/articles/PMC4211729/ /pubmed/25350753 http://dx.doi.org/10.1371/journal.pone.0111441 Text en © 2014 Paulson 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, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Paulson, Nick B.
Gilbertsen, Adam J.
Dalluge, Joseph J.
Welchlin, Cole W.
Hughes, John
Han, Wei
Blackwell, Timothy S.
Laguna, Theresa A.
Williams, Bryan J.
The Arginine Decarboxylase Pathways of Host and Pathogen Interact to Impact Inflammatory Pathways in the Lung
title The Arginine Decarboxylase Pathways of Host and Pathogen Interact to Impact Inflammatory Pathways in the Lung
title_full The Arginine Decarboxylase Pathways of Host and Pathogen Interact to Impact Inflammatory Pathways in the Lung
title_fullStr The Arginine Decarboxylase Pathways of Host and Pathogen Interact to Impact Inflammatory Pathways in the Lung
title_full_unstemmed The Arginine Decarboxylase Pathways of Host and Pathogen Interact to Impact Inflammatory Pathways in the Lung
title_short The Arginine Decarboxylase Pathways of Host and Pathogen Interact to Impact Inflammatory Pathways in the Lung
title_sort arginine decarboxylase pathways of host and pathogen interact to impact inflammatory pathways in the lung
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4211729/
https://www.ncbi.nlm.nih.gov/pubmed/25350753
http://dx.doi.org/10.1371/journal.pone.0111441
work_keys_str_mv AT paulsonnickb theargininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT gilbertsenadamj theargininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT dallugejosephj theargininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT welchlincolew theargininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT hughesjohn theargininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT hanwei theargininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT blackwelltimothys theargininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT lagunatheresaa theargininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT williamsbryanj theargininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT paulsonnickb argininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT gilbertsenadamj argininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT dallugejosephj argininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT welchlincolew argininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT hughesjohn argininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT hanwei argininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT blackwelltimothys argininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT lagunatheresaa argininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung
AT williamsbryanj argininedecarboxylasepathwaysofhostandpathogeninteracttoimpactinflammatorypathwaysinthelung

Ejemplares similares