Polysaccharide Chain Length of Lipopolysaccharides From Salmonella Minnesota Is a Determinant of Aggregate Stability, Plasma Residence Time and Proinflammatory Propensity in vivo

Lipopolysaccharides (LPS) originate from the outer membrane of Gram-negative bacteria and trigger an inflammatory response via the innate immune system. LPS consist of a lipid A moiety directly responsible for the stimulation of the proinflammatory cascade and a polysaccharide chain of variable leng...

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Autores principales: Sali, Wahib, Patoli, Danish, Pais de Barros, Jean-Paul, Labbé, Jérôme, Deckert, Valérie, Duhéron, Vincent, Le Guern, Naig, Blache, Denis, Chaumont, Denis, Lesniewska, Eric, Gasquet, Benoit, Paul, Catherine, Moreau, Mathieu, Denat, Franck, Masson, David, Lagrost, Laurent, Gautier, Thomas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2019
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6688513/
https://www.ncbi.nlm.nih.gov/pubmed/31428071
http://dx.doi.org/10.3389/fmicb.2019.01774
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author Sali, Wahib
Patoli, Danish
Pais de Barros, Jean-Paul
Labbé, Jérôme
Deckert, Valérie
Duhéron, Vincent
Le Guern, Naig
Blache, Denis
Chaumont, Denis
Lesniewska, Eric
Gasquet, Benoit
Paul, Catherine
Moreau, Mathieu
Denat, Franck
Masson, David
Lagrost, Laurent
Gautier, Thomas
author_facet Sali, Wahib
Patoli, Danish
Pais de Barros, Jean-Paul
Labbé, Jérôme
Deckert, Valérie
Duhéron, Vincent
Le Guern, Naig
Blache, Denis
Chaumont, Denis
Lesniewska, Eric
Gasquet, Benoit
Paul, Catherine
Moreau, Mathieu
Denat, Franck
Masson, David
Lagrost, Laurent
Gautier, Thomas
author_sort Sali, Wahib
collection PubMed
description Lipopolysaccharides (LPS) originate from the outer membrane of Gram-negative bacteria and trigger an inflammatory response via the innate immune system. LPS consist of a lipid A moiety directly responsible for the stimulation of the proinflammatory cascade and a polysaccharide chain of variable length. LPS form aggregates of variable size and structure in aqueous media, and the aggregation/disaggregation propensity of LPS is known as a key determinant of their biological activity. The aim of the present study was to determine to which extent the length of the polysaccharide chain can affect the nature of LPS structures, their pharmacokinetics, and eventually their proinflammatory properties in vivo. LPS variants of Salmonella Minnesota with identical lipid A but with different polysaccharide moieties were used. The physical properties of LPS aggregates were analyzed by zetametry, dynamic light scattering, and microscopy. The stability of LPS aggregates was tested in the presence of plasma, whole blood, and cultured cell lines. LPS pharmacokinetics was performed in wild-type mice. The accumulation in plasma of rough LPS (R-LPS) with a short polysaccharidic chain was lower, and its hepatic uptake was faster as compared to smooth LPS (S-LPS) with a long polysaccharidic chain. The inflammatory response was weaker with R-LPS than with S-LPS. As compared to S-LPS, R-LPS formed larger aggregates, with a higher hydrophobicity index, a more negative zeta potential, and a higher critical aggregation concentration. The lower stability of R-LPS aggregates could be illustrated in vitro by a higher extent of association of LPS to plasma lipoproteins, faster binding to blood cells, and increased uptake by macrophages and hepatocytes, compared to S-LPS. Our data indicate that a long polysaccharide chain is associated with the formation of more stable aggregates with extended residence time in plasma and higher inflammatory potential. These results show that polysaccharide chain length, and overall aggregability of LPS might be helpful to predict the proinflammatory effect that can be expected in experimental settings using LPS preparations. In addition, better knowledge and control of LPS aggregation and disaggregation might lead to new strategies to enhance LPS detoxification in septic patients.
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spelling pubmed-66885132019-08-19 Polysaccharide Chain Length of Lipopolysaccharides From Salmonella Minnesota Is a Determinant of Aggregate Stability, Plasma Residence Time and Proinflammatory Propensity in vivo Sali, Wahib Patoli, Danish Pais de Barros, Jean-Paul Labbé, Jérôme Deckert, Valérie Duhéron, Vincent Le Guern, Naig Blache, Denis Chaumont, Denis Lesniewska, Eric Gasquet, Benoit Paul, Catherine Moreau, Mathieu Denat, Franck Masson, David Lagrost, Laurent Gautier, Thomas Front Microbiol Microbiology Lipopolysaccharides (LPS) originate from the outer membrane of Gram-negative bacteria and trigger an inflammatory response via the innate immune system. LPS consist of a lipid A moiety directly responsible for the stimulation of the proinflammatory cascade and a polysaccharide chain of variable length. LPS form aggregates of variable size and structure in aqueous media, and the aggregation/disaggregation propensity of LPS is known as a key determinant of their biological activity. The aim of the present study was to determine to which extent the length of the polysaccharide chain can affect the nature of LPS structures, their pharmacokinetics, and eventually their proinflammatory properties in vivo. LPS variants of Salmonella Minnesota with identical lipid A but with different polysaccharide moieties were used. The physical properties of LPS aggregates were analyzed by zetametry, dynamic light scattering, and microscopy. The stability of LPS aggregates was tested in the presence of plasma, whole blood, and cultured cell lines. LPS pharmacokinetics was performed in wild-type mice. The accumulation in plasma of rough LPS (R-LPS) with a short polysaccharidic chain was lower, and its hepatic uptake was faster as compared to smooth LPS (S-LPS) with a long polysaccharidic chain. The inflammatory response was weaker with R-LPS than with S-LPS. As compared to S-LPS, R-LPS formed larger aggregates, with a higher hydrophobicity index, a more negative zeta potential, and a higher critical aggregation concentration. The lower stability of R-LPS aggregates could be illustrated in vitro by a higher extent of association of LPS to plasma lipoproteins, faster binding to blood cells, and increased uptake by macrophages and hepatocytes, compared to S-LPS. Our data indicate that a long polysaccharide chain is associated with the formation of more stable aggregates with extended residence time in plasma and higher inflammatory potential. These results show that polysaccharide chain length, and overall aggregability of LPS might be helpful to predict the proinflammatory effect that can be expected in experimental settings using LPS preparations. In addition, better knowledge and control of LPS aggregation and disaggregation might lead to new strategies to enhance LPS detoxification in septic patients. Frontiers Media S.A. 2019-08-02 /pmc/articles/PMC6688513/ /pubmed/31428071 http://dx.doi.org/10.3389/fmicb.2019.01774 Text en Copyright © 2019 Sali, Patoli, Pais de Barros, Labbé, Deckert, Duhéron, Le Guern, Blache, Chaumont, Lesniewska, Gasquet, Paul, Moreau, Denat, Masson, Lagrost and Gautier. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Microbiology
Sali, Wahib
Patoli, Danish
Pais de Barros, Jean-Paul
Labbé, Jérôme
Deckert, Valérie
Duhéron, Vincent
Le Guern, Naig
Blache, Denis
Chaumont, Denis
Lesniewska, Eric
Gasquet, Benoit
Paul, Catherine
Moreau, Mathieu
Denat, Franck
Masson, David
Lagrost, Laurent
Gautier, Thomas
Polysaccharide Chain Length of Lipopolysaccharides From Salmonella Minnesota Is a Determinant of Aggregate Stability, Plasma Residence Time and Proinflammatory Propensity in vivo
title Polysaccharide Chain Length of Lipopolysaccharides From Salmonella Minnesota Is a Determinant of Aggregate Stability, Plasma Residence Time and Proinflammatory Propensity in vivo
title_full Polysaccharide Chain Length of Lipopolysaccharides From Salmonella Minnesota Is a Determinant of Aggregate Stability, Plasma Residence Time and Proinflammatory Propensity in vivo
title_fullStr Polysaccharide Chain Length of Lipopolysaccharides From Salmonella Minnesota Is a Determinant of Aggregate Stability, Plasma Residence Time and Proinflammatory Propensity in vivo
title_full_unstemmed Polysaccharide Chain Length of Lipopolysaccharides From Salmonella Minnesota Is a Determinant of Aggregate Stability, Plasma Residence Time and Proinflammatory Propensity in vivo
title_short Polysaccharide Chain Length of Lipopolysaccharides From Salmonella Minnesota Is a Determinant of Aggregate Stability, Plasma Residence Time and Proinflammatory Propensity in vivo
title_sort polysaccharide chain length of lipopolysaccharides from salmonella minnesota is a determinant of aggregate stability, plasma residence time and proinflammatory propensity in vivo
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6688513/
https://www.ncbi.nlm.nih.gov/pubmed/31428071
http://dx.doi.org/10.3389/fmicb.2019.01774
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