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Assessing the function of pneumococcal neuraminidases NanA, NanB and NanC in in vitro and in vivo lung infection models using monoclonal antibodies

Streptococcus pneumoniae isolates express up to three neuraminidases (sialidases), NanA, NanB and NanC, all of which cleave the terminal sialic acid of glycan-structures that decorate host cell surfaces. Most research has focused on the role of NanA with limited investigations evaluating the roles o...

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Autores principales: Janesch, Philipp, Rouha, Harald, Badarau, Adriana, Stulik, Lukas, Mirkina, Irina, Caccamo, Marisa, Havlicek, Katharina, Maierhofer, Barbara, Weber, Susanne, Groß, Karin, Steinhäuser, Jacqueline, Zerbs, Manuel, Varga, Cecilia, Dolezilkova, Ivana, Maier, Sabine, Zauner, Gerhild, Nielson, Nels, Power, Christine A., Nagy, Eszter
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6177239/
https://www.ncbi.nlm.nih.gov/pubmed/30289054
http://dx.doi.org/10.1080/21505594.2018.1520545
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author Janesch, Philipp
Rouha, Harald
Badarau, Adriana
Stulik, Lukas
Mirkina, Irina
Caccamo, Marisa
Havlicek, Katharina
Maierhofer, Barbara
Weber, Susanne
Groß, Karin
Steinhäuser, Jacqueline
Zerbs, Manuel
Varga, Cecilia
Dolezilkova, Ivana
Maier, Sabine
Zauner, Gerhild
Nielson, Nels
Power, Christine A.
Nagy, Eszter
author_facet Janesch, Philipp
Rouha, Harald
Badarau, Adriana
Stulik, Lukas
Mirkina, Irina
Caccamo, Marisa
Havlicek, Katharina
Maierhofer, Barbara
Weber, Susanne
Groß, Karin
Steinhäuser, Jacqueline
Zerbs, Manuel
Varga, Cecilia
Dolezilkova, Ivana
Maier, Sabine
Zauner, Gerhild
Nielson, Nels
Power, Christine A.
Nagy, Eszter
author_sort Janesch, Philipp
collection PubMed
description Streptococcus pneumoniae isolates express up to three neuraminidases (sialidases), NanA, NanB and NanC, all of which cleave the terminal sialic acid of glycan-structures that decorate host cell surfaces. Most research has focused on the role of NanA with limited investigations evaluating the roles of all three neuraminidases in host-pathogen interactions. We generated two highly potent monoclonal antibodies (mAbs), one that blocks the enzymatic activity of NanA and one cross-neutralizing NanB and NanC. Total neuraminidase activity of clinical S. pneumoniae isolates could be inhibited by this mAb combination in enzymatic assays. To detect desialylation of cell surfaces by pneumococcal neuraminidases, primary human tracheal/bronchial mucocilial epithelial tissues were infected with S. pneumoniae and stained with peanut lectin. Simultaneous targeting of the neuraminidases was required to prevent desialylation, suggesting that inhibition of NanA alone is not sufficient to preserve terminal lung glycans. Importantly, we also found that all three neuraminidases increased the interaction of S. pneumoniae with human airway epithelial cells. Lectin-staining of lung tissues of mice pre-treated with mAbs before intranasal challenge with S. pneumoniae confirmed that both anti-NanA and anti-NanBC mAbs were required to effectively block desialylation of the respiratory epithelium in vivo. Despite this, no effect on survival, reduction in pulmonary bacterial load, or significant changes in cytokine responses were observed. This suggests that neuraminidases have no pivotal role in this murine pneumonia model that is induced by high bacterial challenge inocula and does not progress from colonization as it happens in the human host.
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spelling pubmed-61772392018-10-10 Assessing the function of pneumococcal neuraminidases NanA, NanB and NanC in in vitro and in vivo lung infection models using monoclonal antibodies Janesch, Philipp Rouha, Harald Badarau, Adriana Stulik, Lukas Mirkina, Irina Caccamo, Marisa Havlicek, Katharina Maierhofer, Barbara Weber, Susanne Groß, Karin Steinhäuser, Jacqueline Zerbs, Manuel Varga, Cecilia Dolezilkova, Ivana Maier, Sabine Zauner, Gerhild Nielson, Nels Power, Christine A. Nagy, Eszter Virulence Research Paper Streptococcus pneumoniae isolates express up to three neuraminidases (sialidases), NanA, NanB and NanC, all of which cleave the terminal sialic acid of glycan-structures that decorate host cell surfaces. Most research has focused on the role of NanA with limited investigations evaluating the roles of all three neuraminidases in host-pathogen interactions. We generated two highly potent monoclonal antibodies (mAbs), one that blocks the enzymatic activity of NanA and one cross-neutralizing NanB and NanC. Total neuraminidase activity of clinical S. pneumoniae isolates could be inhibited by this mAb combination in enzymatic assays. To detect desialylation of cell surfaces by pneumococcal neuraminidases, primary human tracheal/bronchial mucocilial epithelial tissues were infected with S. pneumoniae and stained with peanut lectin. Simultaneous targeting of the neuraminidases was required to prevent desialylation, suggesting that inhibition of NanA alone is not sufficient to preserve terminal lung glycans. Importantly, we also found that all three neuraminidases increased the interaction of S. pneumoniae with human airway epithelial cells. Lectin-staining of lung tissues of mice pre-treated with mAbs before intranasal challenge with S. pneumoniae confirmed that both anti-NanA and anti-NanBC mAbs were required to effectively block desialylation of the respiratory epithelium in vivo. Despite this, no effect on survival, reduction in pulmonary bacterial load, or significant changes in cytokine responses were observed. This suggests that neuraminidases have no pivotal role in this murine pneumonia model that is induced by high bacterial challenge inocula and does not progress from colonization as it happens in the human host. Taylor & Francis 2018-10-05 /pmc/articles/PMC6177239/ /pubmed/30289054 http://dx.doi.org/10.1080/21505594.2018.1520545 Text en © 2018 The Author(s). Published by Informa UK Limited, trading as Taylor & Francis Group. 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 work is properly cited.
spellingShingle Research Paper
Janesch, Philipp
Rouha, Harald
Badarau, Adriana
Stulik, Lukas
Mirkina, Irina
Caccamo, Marisa
Havlicek, Katharina
Maierhofer, Barbara
Weber, Susanne
Groß, Karin
Steinhäuser, Jacqueline
Zerbs, Manuel
Varga, Cecilia
Dolezilkova, Ivana
Maier, Sabine
Zauner, Gerhild
Nielson, Nels
Power, Christine A.
Nagy, Eszter
Assessing the function of pneumococcal neuraminidases NanA, NanB and NanC in in vitro and in vivo lung infection models using monoclonal antibodies
title Assessing the function of pneumococcal neuraminidases NanA, NanB and NanC in in vitro and in vivo lung infection models using monoclonal antibodies
title_full Assessing the function of pneumococcal neuraminidases NanA, NanB and NanC in in vitro and in vivo lung infection models using monoclonal antibodies
title_fullStr Assessing the function of pneumococcal neuraminidases NanA, NanB and NanC in in vitro and in vivo lung infection models using monoclonal antibodies
title_full_unstemmed Assessing the function of pneumococcal neuraminidases NanA, NanB and NanC in in vitro and in vivo lung infection models using monoclonal antibodies
title_short Assessing the function of pneumococcal neuraminidases NanA, NanB and NanC in in vitro and in vivo lung infection models using monoclonal antibodies
title_sort assessing the function of pneumococcal neuraminidases nana, nanb and nanc in in vitro and in vivo lung infection models using monoclonal antibodies
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6177239/
https://www.ncbi.nlm.nih.gov/pubmed/30289054
http://dx.doi.org/10.1080/21505594.2018.1520545
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