Immunization of rabbits with synthetic peptides derived from a highly conserved β-sheet epitope region underneath the receptor binding site of influenza A virus

BACKGROUND: There is increasing concern about the speed with which health care providers can administer prophylaxis and treatment in an influenza pandemic. Generally, it takes several months to manufacture an influenza vaccine by propagation of the virus in chicken eggs or cultured cells. Newer, fas...

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Autores principales: Ideno, Shoji, Sakai, Kaoru, Yunoki, Mikihiro, Kubota-Koketsu, Ritsuko, Inoue, Yuji, Nakamura, Shota, Yasunaga, Teruo, Okuno, Yoshinobu, Ikuta, Kazuyoshi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Dove Medical Press 2013
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Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3821756/
https://www.ncbi.nlm.nih.gov/pubmed/24235814
http://dx.doi.org/10.2147/BTT.S50870
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author Ideno, Shoji
Sakai, Kaoru
Yunoki, Mikihiro
Kubota-Koketsu, Ritsuko
Inoue, Yuji
Nakamura, Shota
Yasunaga, Teruo
Okuno, Yoshinobu
Ikuta, Kazuyoshi
author_facet Ideno, Shoji
Sakai, Kaoru
Yunoki, Mikihiro
Kubota-Koketsu, Ritsuko
Inoue, Yuji
Nakamura, Shota
Yasunaga, Teruo
Okuno, Yoshinobu
Ikuta, Kazuyoshi
author_sort Ideno, Shoji
collection PubMed
description BACKGROUND: There is increasing concern about the speed with which health care providers can administer prophylaxis and treatment in an influenza pandemic. Generally, it takes several months to manufacture an influenza vaccine by propagation of the virus in chicken eggs or cultured cells. Newer, faster protocols for the production of vaccines that induce broad-spectrum immunity are therefore highly desirable. We previously developed human monoclonal antibody B-1 that shows broadly neutralizing activity against influenza A virus H3N2. B-1 recognizes an epitope region that includes an antiparallel β-sheet structure underneath the receptor binding site of influenza hemagglutinin (HA). In this study, the efficacy of a synthetic peptide vaccine derived from this epitope region against influenza A was evaluated. MATERIALS AND METHODS: Two peptides were synthesized, the upper and lower peptides. These peptides comprise amino acid residues 167–187 and 225–241, respectively, of the B-1 epitope region of HA, which is involved in forming the β-sheet structure. Both peptides were then coupled to keyhole limpet hemocyanin, and the peptides, alone or in combination, were used to immunize rabbits. The resulting antibody responses were examined by enzyme-linked immunosorbent assay. The upper peptide, but not the lower peptide, elicited antibodies that were reactive to HA. Interestingly, the use of both peptides together could elicit antibodies with a higher reactivity to HA than either peptide alone. The antibodies were found to react to HA at the N-terminus of the upper peptide, which is exposed at the surface of trimeric HA on influenza virions. DISCUSSION: The higher production of HA-reactive antibodies following immunization with both peptides suggests that the upper peptide forms the effective epitope structure in the binding state, and the lower peptide enhances the production of HA antibodies. This study could be the first step towards the development of pandemic viral vaccines that can be produced within short time periods.
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spelling pubmed-38217562013-11-14 Immunization of rabbits with synthetic peptides derived from a highly conserved β-sheet epitope region underneath the receptor binding site of influenza A virus Ideno, Shoji Sakai, Kaoru Yunoki, Mikihiro Kubota-Koketsu, Ritsuko Inoue, Yuji Nakamura, Shota Yasunaga, Teruo Okuno, Yoshinobu Ikuta, Kazuyoshi Biologics Original Research BACKGROUND: There is increasing concern about the speed with which health care providers can administer prophylaxis and treatment in an influenza pandemic. Generally, it takes several months to manufacture an influenza vaccine by propagation of the virus in chicken eggs or cultured cells. Newer, faster protocols for the production of vaccines that induce broad-spectrum immunity are therefore highly desirable. We previously developed human monoclonal antibody B-1 that shows broadly neutralizing activity against influenza A virus H3N2. B-1 recognizes an epitope region that includes an antiparallel β-sheet structure underneath the receptor binding site of influenza hemagglutinin (HA). In this study, the efficacy of a synthetic peptide vaccine derived from this epitope region against influenza A was evaluated. MATERIALS AND METHODS: Two peptides were synthesized, the upper and lower peptides. These peptides comprise amino acid residues 167–187 and 225–241, respectively, of the B-1 epitope region of HA, which is involved in forming the β-sheet structure. Both peptides were then coupled to keyhole limpet hemocyanin, and the peptides, alone or in combination, were used to immunize rabbits. The resulting antibody responses were examined by enzyme-linked immunosorbent assay. The upper peptide, but not the lower peptide, elicited antibodies that were reactive to HA. Interestingly, the use of both peptides together could elicit antibodies with a higher reactivity to HA than either peptide alone. The antibodies were found to react to HA at the N-terminus of the upper peptide, which is exposed at the surface of trimeric HA on influenza virions. DISCUSSION: The higher production of HA-reactive antibodies following immunization with both peptides suggests that the upper peptide forms the effective epitope structure in the binding state, and the lower peptide enhances the production of HA antibodies. This study could be the first step towards the development of pandemic viral vaccines that can be produced within short time periods. Dove Medical Press 2013 2013-11-05 /pmc/articles/PMC3821756/ /pubmed/24235814 http://dx.doi.org/10.2147/BTT.S50870 Text en © 2013 Ideno et al. This work is published by Dove Medical Press Limited, and licensed under Creative Commons Attribution – Non Commercial (unported, v3.0) License The full terms of the License are available at http://creativecommons.org/licenses/by-nc/3.0/. Non-commercial uses of the work are permitted without any further permission from Dove Medical Press Limited, provided the work is properly attributed.
spellingShingle Original Research
Ideno, Shoji
Sakai, Kaoru
Yunoki, Mikihiro
Kubota-Koketsu, Ritsuko
Inoue, Yuji
Nakamura, Shota
Yasunaga, Teruo
Okuno, Yoshinobu
Ikuta, Kazuyoshi
Immunization of rabbits with synthetic peptides derived from a highly conserved β-sheet epitope region underneath the receptor binding site of influenza A virus
title Immunization of rabbits with synthetic peptides derived from a highly conserved β-sheet epitope region underneath the receptor binding site of influenza A virus
title_full Immunization of rabbits with synthetic peptides derived from a highly conserved β-sheet epitope region underneath the receptor binding site of influenza A virus
title_fullStr Immunization of rabbits with synthetic peptides derived from a highly conserved β-sheet epitope region underneath the receptor binding site of influenza A virus
title_full_unstemmed Immunization of rabbits with synthetic peptides derived from a highly conserved β-sheet epitope region underneath the receptor binding site of influenza A virus
title_short Immunization of rabbits with synthetic peptides derived from a highly conserved β-sheet epitope region underneath the receptor binding site of influenza A virus
title_sort immunization of rabbits with synthetic peptides derived from a highly conserved β-sheet epitope region underneath the receptor binding site of influenza a virus
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3821756/
https://www.ncbi.nlm.nih.gov/pubmed/24235814
http://dx.doi.org/10.2147/BTT.S50870
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