CD4+ T Cells Targeting Dominant and Cryptic Epitopes from Bacillus anthracis Lethal Factor

Anthrax is an endemic infection in many countries, particularly in the developing world. The causative agent, Bacillus anthracis, mediates disease through the secretion of binary exotoxins. Until recently, research into adaptive immunity targeting this bacterial pathogen has largely focused on the h...

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Autores principales: Ascough, Stephanie, Ingram, Rebecca J., Chu, Karen K. Y., Musson, Julie A., Moore, Stephen J., Gallagher, Theresa, Baillie, Les, Williamson, Ethel D., Robinson, John H., Maillere, Bernard, Boyton, Rosemary J., Altmann, Daniel M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2016
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4700811/
https://www.ncbi.nlm.nih.gov/pubmed/26779161
http://dx.doi.org/10.3389/fmicb.2015.01506
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author Ascough, Stephanie
Ingram, Rebecca J.
Chu, Karen K. Y.
Musson, Julie A.
Moore, Stephen J.
Gallagher, Theresa
Baillie, Les
Williamson, Ethel D.
Robinson, John H.
Maillere, Bernard
Boyton, Rosemary J.
Altmann, Daniel M.
author_facet Ascough, Stephanie
Ingram, Rebecca J.
Chu, Karen K. Y.
Musson, Julie A.
Moore, Stephen J.
Gallagher, Theresa
Baillie, Les
Williamson, Ethel D.
Robinson, John H.
Maillere, Bernard
Boyton, Rosemary J.
Altmann, Daniel M.
author_sort Ascough, Stephanie
collection PubMed
description Anthrax is an endemic infection in many countries, particularly in the developing world. The causative agent, Bacillus anthracis, mediates disease through the secretion of binary exotoxins. Until recently, research into adaptive immunity targeting this bacterial pathogen has largely focused on the humoral response to these toxins. There is, however, growing recognition that cellular immune responses involving IFNγ producing CD4+ T cells also contribute significantly to a protective memory response. An established concept in adaptive immunity to infection is that during infection of host cells, new microbial epitopes may be revealed, leading to immune recognition of so called ‘cryptic’ or ‘subdominant’ epitopes. We analyzed the response to both cryptic and immunodominant T cell epitopes derived from the toxin component lethal factor and presented by a range of HLA-DR alleles. Using IFNγ-ELISpot assays we characterized epitopes that elicited a response following immunization with synthetic peptide and the whole protein and tested their capacities to bind purified HLA-DR molecules in vitro. We found that DR1 transgenics demonstrated T cell responses to a greater number of domain III cryptic epitopes than other HLA-DR transgenics, and that this pattern was repeated with the immunodominant epitopes, as a greater proportion of these epitopes induced a T cell response when presented within the context of the whole protein. Immunodominant epitopes LF(457-476) and LF(467-487) were found to induce a T cell response to the peptide, as well as to the whole native LF protein in DR1 and DR15, but not in DR4 transgenics. The analysis of Domain I revealed the presence of several unique cryptic epitopes all of which showed a strong to moderate relative binding affinity to HLA-DR4 molecules. However, none of the cryptic epitopes from either domain III or I displayed notably high binding affinities across all HLA-DR alleles assayed. These responses were influenced by the specific HLA alleles presenting the peptide, and imply that construction of future epitope string vaccines which are immunogenic across a wide range of HLA alleles could benefit from a combination of both cryptic and immunodominant anthrax epitopes.
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spelling pubmed-47008112016-01-15 CD4+ T Cells Targeting Dominant and Cryptic Epitopes from Bacillus anthracis Lethal Factor Ascough, Stephanie Ingram, Rebecca J. Chu, Karen K. Y. Musson, Julie A. Moore, Stephen J. Gallagher, Theresa Baillie, Les Williamson, Ethel D. Robinson, John H. Maillere, Bernard Boyton, Rosemary J. Altmann, Daniel M. Front Microbiol Microbiology Anthrax is an endemic infection in many countries, particularly in the developing world. The causative agent, Bacillus anthracis, mediates disease through the secretion of binary exotoxins. Until recently, research into adaptive immunity targeting this bacterial pathogen has largely focused on the humoral response to these toxins. There is, however, growing recognition that cellular immune responses involving IFNγ producing CD4+ T cells also contribute significantly to a protective memory response. An established concept in adaptive immunity to infection is that during infection of host cells, new microbial epitopes may be revealed, leading to immune recognition of so called ‘cryptic’ or ‘subdominant’ epitopes. We analyzed the response to both cryptic and immunodominant T cell epitopes derived from the toxin component lethal factor and presented by a range of HLA-DR alleles. Using IFNγ-ELISpot assays we characterized epitopes that elicited a response following immunization with synthetic peptide and the whole protein and tested their capacities to bind purified HLA-DR molecules in vitro. We found that DR1 transgenics demonstrated T cell responses to a greater number of domain III cryptic epitopes than other HLA-DR transgenics, and that this pattern was repeated with the immunodominant epitopes, as a greater proportion of these epitopes induced a T cell response when presented within the context of the whole protein. Immunodominant epitopes LF(457-476) and LF(467-487) were found to induce a T cell response to the peptide, as well as to the whole native LF protein in DR1 and DR15, but not in DR4 transgenics. The analysis of Domain I revealed the presence of several unique cryptic epitopes all of which showed a strong to moderate relative binding affinity to HLA-DR4 molecules. However, none of the cryptic epitopes from either domain III or I displayed notably high binding affinities across all HLA-DR alleles assayed. These responses were influenced by the specific HLA alleles presenting the peptide, and imply that construction of future epitope string vaccines which are immunogenic across a wide range of HLA alleles could benefit from a combination of both cryptic and immunodominant anthrax epitopes. Frontiers Media S.A. 2016-01-05 /pmc/articles/PMC4700811/ /pubmed/26779161 http://dx.doi.org/10.3389/fmicb.2015.01506 Text en Copyright © 2016 Ascough, Ingram, Chu, Musson, Moore, Gallagher, Baillie, Williamson, Robinson, Maillere, Boyton and Altmann. 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) or licensor 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
Ascough, Stephanie
Ingram, Rebecca J.
Chu, Karen K. Y.
Musson, Julie A.
Moore, Stephen J.
Gallagher, Theresa
Baillie, Les
Williamson, Ethel D.
Robinson, John H.
Maillere, Bernard
Boyton, Rosemary J.
Altmann, Daniel M.
CD4+ T Cells Targeting Dominant and Cryptic Epitopes from Bacillus anthracis Lethal Factor
title CD4+ T Cells Targeting Dominant and Cryptic Epitopes from Bacillus anthracis Lethal Factor
title_full CD4+ T Cells Targeting Dominant and Cryptic Epitopes from Bacillus anthracis Lethal Factor
title_fullStr CD4+ T Cells Targeting Dominant and Cryptic Epitopes from Bacillus anthracis Lethal Factor
title_full_unstemmed CD4+ T Cells Targeting Dominant and Cryptic Epitopes from Bacillus anthracis Lethal Factor
title_short CD4+ T Cells Targeting Dominant and Cryptic Epitopes from Bacillus anthracis Lethal Factor
title_sort cd4+ t cells targeting dominant and cryptic epitopes from bacillus anthracis lethal factor
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4700811/
https://www.ncbi.nlm.nih.gov/pubmed/26779161
http://dx.doi.org/10.3389/fmicb.2015.01506
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