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Comparative Immunogenicity in Rabbits of the Polypeptides Encoded by the 5′ Terminus of Hepatitis C Virus RNA

Recent studies on the primate protection from HCV infection stressed the importance of immune response against structural viral proteins. Strong immune response against nucleocapsid (core) protein was difficult to achieve, requesting further experimentation in large animals. Here, we analyzed the im...

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Autores principales: Sominskaya, Irina, Jansons, Juris, Dovbenko, Anastasija, Petrakova, Natalia, Lieknina, Ilva, Mihailova, Marija, Latyshev, Oleg, Eliseeva, Olesja, Stahovska, Irina, Akopjana, Inara, Petrovskis, Ivars, Isaguliants, Maria
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi Publishing Corporation 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4644844/
https://www.ncbi.nlm.nih.gov/pubmed/26609538
http://dx.doi.org/10.1155/2015/762426
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author Sominskaya, Irina
Jansons, Juris
Dovbenko, Anastasija
Petrakova, Natalia
Lieknina, Ilva
Mihailova, Marija
Latyshev, Oleg
Eliseeva, Olesja
Stahovska, Irina
Akopjana, Inara
Petrovskis, Ivars
Isaguliants, Maria
author_facet Sominskaya, Irina
Jansons, Juris
Dovbenko, Anastasija
Petrakova, Natalia
Lieknina, Ilva
Mihailova, Marija
Latyshev, Oleg
Eliseeva, Olesja
Stahovska, Irina
Akopjana, Inara
Petrovskis, Ivars
Isaguliants, Maria
author_sort Sominskaya, Irina
collection PubMed
description Recent studies on the primate protection from HCV infection stressed the importance of immune response against structural viral proteins. Strong immune response against nucleocapsid (core) protein was difficult to achieve, requesting further experimentation in large animals. Here, we analyzed the immunogenicity of core aa 1–173, 1–152, and 147–191 and of its main alternative reading frame product F-protein in rabbits. Core aa 147–191 was synthesized; other polypeptides were obtained by expression in E. coli. Rabbits were immunized by polypeptide primes followed by multiple boosts and screened for specific anti-protein and anti-peptide antibodies. Antibody titers to core aa 147–191 reached 10(5); core aa 1–152, 5 × 10(5); core aa 1–173 and F-protein, 10(6). Strong immunogenicity of the last two proteins indicated that they may compete for the induction of immune response. The C-terminally truncated core was also weakly immunogenic on the T-cell level. To enhance core-specific cellular response, we immunized rabbits with the core aa 1–152 gene forbidding F-protein formation. Repeated DNA immunization induced a weak antibody and sustained proliferative response of broad specificity confirming a gain of cellular immunogenicity. Epitopes recognized in rabbits overlapped those in HCV infection. Our data promotes the use of rabbits for the immunogenicity tests of prototype HCV vaccines.
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spelling pubmed-46448442015-11-25 Comparative Immunogenicity in Rabbits of the Polypeptides Encoded by the 5′ Terminus of Hepatitis C Virus RNA Sominskaya, Irina Jansons, Juris Dovbenko, Anastasija Petrakova, Natalia Lieknina, Ilva Mihailova, Marija Latyshev, Oleg Eliseeva, Olesja Stahovska, Irina Akopjana, Inara Petrovskis, Ivars Isaguliants, Maria J Immunol Res Research Article Recent studies on the primate protection from HCV infection stressed the importance of immune response against structural viral proteins. Strong immune response against nucleocapsid (core) protein was difficult to achieve, requesting further experimentation in large animals. Here, we analyzed the immunogenicity of core aa 1–173, 1–152, and 147–191 and of its main alternative reading frame product F-protein in rabbits. Core aa 147–191 was synthesized; other polypeptides were obtained by expression in E. coli. Rabbits were immunized by polypeptide primes followed by multiple boosts and screened for specific anti-protein and anti-peptide antibodies. Antibody titers to core aa 147–191 reached 10(5); core aa 1–152, 5 × 10(5); core aa 1–173 and F-protein, 10(6). Strong immunogenicity of the last two proteins indicated that they may compete for the induction of immune response. The C-terminally truncated core was also weakly immunogenic on the T-cell level. To enhance core-specific cellular response, we immunized rabbits with the core aa 1–152 gene forbidding F-protein formation. Repeated DNA immunization induced a weak antibody and sustained proliferative response of broad specificity confirming a gain of cellular immunogenicity. Epitopes recognized in rabbits overlapped those in HCV infection. Our data promotes the use of rabbits for the immunogenicity tests of prototype HCV vaccines. Hindawi Publishing Corporation 2015 2015-11-02 /pmc/articles/PMC4644844/ /pubmed/26609538 http://dx.doi.org/10.1155/2015/762426 Text en Copyright © 2015 Irina Sominskaya et al. https://creativecommons.org/licenses/by/3.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Sominskaya, Irina
Jansons, Juris
Dovbenko, Anastasija
Petrakova, Natalia
Lieknina, Ilva
Mihailova, Marija
Latyshev, Oleg
Eliseeva, Olesja
Stahovska, Irina
Akopjana, Inara
Petrovskis, Ivars
Isaguliants, Maria
Comparative Immunogenicity in Rabbits of the Polypeptides Encoded by the 5′ Terminus of Hepatitis C Virus RNA
title Comparative Immunogenicity in Rabbits of the Polypeptides Encoded by the 5′ Terminus of Hepatitis C Virus RNA
title_full Comparative Immunogenicity in Rabbits of the Polypeptides Encoded by the 5′ Terminus of Hepatitis C Virus RNA
title_fullStr Comparative Immunogenicity in Rabbits of the Polypeptides Encoded by the 5′ Terminus of Hepatitis C Virus RNA
title_full_unstemmed Comparative Immunogenicity in Rabbits of the Polypeptides Encoded by the 5′ Terminus of Hepatitis C Virus RNA
title_short Comparative Immunogenicity in Rabbits of the Polypeptides Encoded by the 5′ Terminus of Hepatitis C Virus RNA
title_sort comparative immunogenicity in rabbits of the polypeptides encoded by the 5′ terminus of hepatitis c virus rna
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4644844/
https://www.ncbi.nlm.nih.gov/pubmed/26609538
http://dx.doi.org/10.1155/2015/762426
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