Influenza viral vectors expressing the Brucella OMP16 or L7/L12 proteins as vaccines against B. abortus infection

BACKGROUND: We generated novel, effective candidate vaccine against Brucella abortus based on recombinant influenza viruses expressing the Brucella ribosomal protein L7/L12 or outer membrane protein (Omp)-16 from the NS1 open reading frame. The main purpose of this work was to evaluate the safety, i...

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Autores principales: Tabynov, Kaissar, Sansyzbay, Abylai, Kydyrbayev, Zhailaubay, Yespembetov, Bolat, Ryskeldinova, Sholpan, Zinina, Nadezhda, Assanzhanova, Nurika, Sultankulova, Kulaisan, Sandybayev, Nurlan, Khairullin, Berik, Kuznetsova, Irina, Ferko, Boris, Egorov, Andrej
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2014
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3997475/
https://www.ncbi.nlm.nih.gov/pubmed/24716528
http://dx.doi.org/10.1186/1743-422X-11-69
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author Tabynov, Kaissar
Sansyzbay, Abylai
Kydyrbayev, Zhailaubay
Yespembetov, Bolat
Ryskeldinova, Sholpan
Zinina, Nadezhda
Assanzhanova, Nurika
Sultankulova, Kulaisan
Sandybayev, Nurlan
Khairullin, Berik
Kuznetsova, Irina
Ferko, Boris
Egorov, Andrej
author_facet Tabynov, Kaissar
Sansyzbay, Abylai
Kydyrbayev, Zhailaubay
Yespembetov, Bolat
Ryskeldinova, Sholpan
Zinina, Nadezhda
Assanzhanova, Nurika
Sultankulova, Kulaisan
Sandybayev, Nurlan
Khairullin, Berik
Kuznetsova, Irina
Ferko, Boris
Egorov, Andrej
author_sort Tabynov, Kaissar
collection PubMed
description BACKGROUND: We generated novel, effective candidate vaccine against Brucella abortus based on recombinant influenza viruses expressing the Brucella ribosomal protein L7/L12 or outer membrane protein (Omp)-16 from the NS1 open reading frame. The main purpose of this work was to evaluate the safety, immunogenicity and protectiveness of vaccine candidate in laboratory animals. METHODS AND RESULTS: Four recombinant influenza A viral constructs of the subtypes Н5N1 or H1N1 expressing the Brucella proteins L7/L12 or Omp16 were obtained by a reverse genetics method: Flu-NS1-124-L7/L12-H5N1, Flu-NS1-124-Omp16-H5N1, Flu-NS1-124-L7/L12-H1N1 and Flu-NS1-124-Omp16-H1N1. Despite of substantial modification of NS1 gene, all constructs replicated well and were retain their Brucella inserts over five passages in embryonated chicken eggs (CE). Administration of the mono- or bivalent vaccine formulation via prime-boost intranasal (i.n.), conjunctival (c.) or subcutaneous (s.c.) immunization was safe in mice; no deaths, body weight loss or pathomorphological changes were observed over 56 days. Moreover, guinea pigs vaccinated i.n. with vaccine vectors did not shed the vaccine viruses through their upper respiratory tract after the prime and booster vaccination. These findings confirmed the replication-deficient phenotype of viral vectors. The highest antibody response to Brucella antigen was obtained with constructs expressing L7/L12 (ELISA, GMT 242.5-735.0); whereas the highest T-cell immune response- with construct expressing Omp16 (ELISPOT, 337 ± 52-651 ± 45 spots/4×10(5)cells), which was comparable (P > 0.05) to the response induced by the commercial vaccine B. abortus 19. Interestingly, c. immunization appeared to be optimal for eliciting T-cell immune response. In guinea pigs, the highest protective efficacy after challenge with B. abortus 544 was achieved with Omp16 expressing constructs in both monovalent or bivalent vaccine formulations; protective efficacy was comparable to those induced by a commercial live B. abortus 19 vaccine. CONCLUSION: Thus, influenza vectors expressing Brucella protective antigens can be developed as novel influenza vectored vaccine against B. abortus infection.
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spelling pubmed-39974752014-04-24 Influenza viral vectors expressing the Brucella OMP16 or L7/L12 proteins as vaccines against B. abortus infection Tabynov, Kaissar Sansyzbay, Abylai Kydyrbayev, Zhailaubay Yespembetov, Bolat Ryskeldinova, Sholpan Zinina, Nadezhda Assanzhanova, Nurika Sultankulova, Kulaisan Sandybayev, Nurlan Khairullin, Berik Kuznetsova, Irina Ferko, Boris Egorov, Andrej Virol J Research BACKGROUND: We generated novel, effective candidate vaccine against Brucella abortus based on recombinant influenza viruses expressing the Brucella ribosomal protein L7/L12 or outer membrane protein (Omp)-16 from the NS1 open reading frame. The main purpose of this work was to evaluate the safety, immunogenicity and protectiveness of vaccine candidate in laboratory animals. METHODS AND RESULTS: Four recombinant influenza A viral constructs of the subtypes Н5N1 or H1N1 expressing the Brucella proteins L7/L12 or Omp16 were obtained by a reverse genetics method: Flu-NS1-124-L7/L12-H5N1, Flu-NS1-124-Omp16-H5N1, Flu-NS1-124-L7/L12-H1N1 and Flu-NS1-124-Omp16-H1N1. Despite of substantial modification of NS1 gene, all constructs replicated well and were retain their Brucella inserts over five passages in embryonated chicken eggs (CE). Administration of the mono- or bivalent vaccine formulation via prime-boost intranasal (i.n.), conjunctival (c.) or subcutaneous (s.c.) immunization was safe in mice; no deaths, body weight loss or pathomorphological changes were observed over 56 days. Moreover, guinea pigs vaccinated i.n. with vaccine vectors did not shed the vaccine viruses through their upper respiratory tract after the prime and booster vaccination. These findings confirmed the replication-deficient phenotype of viral vectors. The highest antibody response to Brucella antigen was obtained with constructs expressing L7/L12 (ELISA, GMT 242.5-735.0); whereas the highest T-cell immune response- with construct expressing Omp16 (ELISPOT, 337 ± 52-651 ± 45 spots/4×10(5)cells), which was comparable (P > 0.05) to the response induced by the commercial vaccine B. abortus 19. Interestingly, c. immunization appeared to be optimal for eliciting T-cell immune response. In guinea pigs, the highest protective efficacy after challenge with B. abortus 544 was achieved with Omp16 expressing constructs in both monovalent or bivalent vaccine formulations; protective efficacy was comparable to those induced by a commercial live B. abortus 19 vaccine. CONCLUSION: Thus, influenza vectors expressing Brucella protective antigens can be developed as novel influenza vectored vaccine against B. abortus infection. BioMed Central 2014-04-10 /pmc/articles/PMC3997475/ /pubmed/24716528 http://dx.doi.org/10.1186/1743-422X-11-69 Text en Copyright © 2014 Tabynov et al.; licensee BioMed Central Ltd. 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 credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Tabynov, Kaissar
Sansyzbay, Abylai
Kydyrbayev, Zhailaubay
Yespembetov, Bolat
Ryskeldinova, Sholpan
Zinina, Nadezhda
Assanzhanova, Nurika
Sultankulova, Kulaisan
Sandybayev, Nurlan
Khairullin, Berik
Kuznetsova, Irina
Ferko, Boris
Egorov, Andrej
Influenza viral vectors expressing the Brucella OMP16 or L7/L12 proteins as vaccines against B. abortus infection
title Influenza viral vectors expressing the Brucella OMP16 or L7/L12 proteins as vaccines against B. abortus infection
title_full Influenza viral vectors expressing the Brucella OMP16 or L7/L12 proteins as vaccines against B. abortus infection
title_fullStr Influenza viral vectors expressing the Brucella OMP16 or L7/L12 proteins as vaccines against B. abortus infection
title_full_unstemmed Influenza viral vectors expressing the Brucella OMP16 or L7/L12 proteins as vaccines against B. abortus infection
title_short Influenza viral vectors expressing the Brucella OMP16 or L7/L12 proteins as vaccines against B. abortus infection
title_sort influenza viral vectors expressing the brucella omp16 or l7/l12 proteins as vaccines against b. abortus infection
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3997475/
https://www.ncbi.nlm.nih.gov/pubmed/24716528
http://dx.doi.org/10.1186/1743-422X-11-69
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