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Multiple mechanisms mediate enhanced immunity generated by mAb-inactivated F. tularensis immunogen

We have previously demonstrated that immunization with inactivated Francisella tularensis, a Category A intracellular mucosal pathogen, combined with IgG2a anti-F. tularensis monoclonal antibody, enhances protection against subsequent F. tularensis challenge. To understand the mechanism(s) involved,...

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Autores principales: Iglesias, Bibiana V., Bitsaktsis, Constantine, Pham, Giang, Drake, James R., Hazlett, Karsten R.O., Porter, Kristen, Gosselin, Edmund J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3570671/
https://www.ncbi.nlm.nih.gov/pubmed/23247654
http://dx.doi.org/10.1038/icb.2012.66
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author Iglesias, Bibiana V.
Bitsaktsis, Constantine
Pham, Giang
Drake, James R.
Hazlett, Karsten R.O.
Porter, Kristen
Gosselin, Edmund J.
author_facet Iglesias, Bibiana V.
Bitsaktsis, Constantine
Pham, Giang
Drake, James R.
Hazlett, Karsten R.O.
Porter, Kristen
Gosselin, Edmund J.
author_sort Iglesias, Bibiana V.
collection PubMed
description We have previously demonstrated that immunization with inactivated Francisella tularensis, a Category A intracellular mucosal pathogen, combined with IgG2a anti-F. tularensis monoclonal antibody, enhances protection against subsequent F. tularensis challenge. To understand the mechanism(s) involved, we examined the binding, internalization, presentation, and in vivo trafficking of inactivated F. tularensis in the presence and absence of opsonizing monoclonal antibody. We found that when inactivated F. tularensis is combined with anti-F. tularensis monoclonal antibody, presentation to F. tularensis-specific T cells is enhanced, this enhancement is Fc receptor-dependent, and requires a physical linkage between the monoclonal antibody and the inactivated F. tularensis immunogen. This enhanced presentation is due, in part, to enhanced binding and internalization of inactivated F. tularensis by antigen presenting cells, and involves interactions with multiple Fc receptor types. Furthermore, targeting inactivated F. tularensis to Fc receptors enhances dendritic cell maturation and extends the time period over which antigen presenting cells stimulate T cells. In vivo trafficking studies reveal enhanced transport of inactivated F. tularensis immunogen to the Nasal Associated Lymphoid Tissue in the presence of monoclonal antibody, which is FcRn-dependent. In summary, these are the first comprehensive studies using a single vaccine protection model/immunogen to establish the array of mechanisms involved in enhanced immunity/protection mediated by an Fc receptor-targeted mucosal immunogen. These results demonstrate that multiple cellular/immune mechanisms contribute to Fc receptor-enhanced immunity.
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spelling pubmed-35706712013-08-01 Multiple mechanisms mediate enhanced immunity generated by mAb-inactivated F. tularensis immunogen Iglesias, Bibiana V. Bitsaktsis, Constantine Pham, Giang Drake, James R. Hazlett, Karsten R.O. Porter, Kristen Gosselin, Edmund J. Immunol Cell Biol Article We have previously demonstrated that immunization with inactivated Francisella tularensis, a Category A intracellular mucosal pathogen, combined with IgG2a anti-F. tularensis monoclonal antibody, enhances protection against subsequent F. tularensis challenge. To understand the mechanism(s) involved, we examined the binding, internalization, presentation, and in vivo trafficking of inactivated F. tularensis in the presence and absence of opsonizing monoclonal antibody. We found that when inactivated F. tularensis is combined with anti-F. tularensis monoclonal antibody, presentation to F. tularensis-specific T cells is enhanced, this enhancement is Fc receptor-dependent, and requires a physical linkage between the monoclonal antibody and the inactivated F. tularensis immunogen. This enhanced presentation is due, in part, to enhanced binding and internalization of inactivated F. tularensis by antigen presenting cells, and involves interactions with multiple Fc receptor types. Furthermore, targeting inactivated F. tularensis to Fc receptors enhances dendritic cell maturation and extends the time period over which antigen presenting cells stimulate T cells. In vivo trafficking studies reveal enhanced transport of inactivated F. tularensis immunogen to the Nasal Associated Lymphoid Tissue in the presence of monoclonal antibody, which is FcRn-dependent. In summary, these are the first comprehensive studies using a single vaccine protection model/immunogen to establish the array of mechanisms involved in enhanced immunity/protection mediated by an Fc receptor-targeted mucosal immunogen. These results demonstrate that multiple cellular/immune mechanisms contribute to Fc receptor-enhanced immunity. 2012-12-18 2013-02 /pmc/articles/PMC3570671/ /pubmed/23247654 http://dx.doi.org/10.1038/icb.2012.66 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Iglesias, Bibiana V.
Bitsaktsis, Constantine
Pham, Giang
Drake, James R.
Hazlett, Karsten R.O.
Porter, Kristen
Gosselin, Edmund J.
Multiple mechanisms mediate enhanced immunity generated by mAb-inactivated F. tularensis immunogen
title Multiple mechanisms mediate enhanced immunity generated by mAb-inactivated F. tularensis immunogen
title_full Multiple mechanisms mediate enhanced immunity generated by mAb-inactivated F. tularensis immunogen
title_fullStr Multiple mechanisms mediate enhanced immunity generated by mAb-inactivated F. tularensis immunogen
title_full_unstemmed Multiple mechanisms mediate enhanced immunity generated by mAb-inactivated F. tularensis immunogen
title_short Multiple mechanisms mediate enhanced immunity generated by mAb-inactivated F. tularensis immunogen
title_sort multiple mechanisms mediate enhanced immunity generated by mab-inactivated f. tularensis immunogen
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3570671/
https://www.ncbi.nlm.nih.gov/pubmed/23247654
http://dx.doi.org/10.1038/icb.2012.66
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