HCV Core/NS3 Protein Immunization with “N-Terminal Heat Shock gp96 Protein (rNT (gp96))” Induced Strong and Sustained Th1-Type Cytokines in Immunized Mice

Feeble cellular responses induced by T cell-based vaccines are a major challenge for the development of an effective vaccine against Hepatitis C virus (HCV) infection. To address this challenge, the potential of N-terminal fragment of gp96 heat shock protein (rNT (gp96) as an adjuvant was evaluated...

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Autores principales: Hajikhezri, Zamaneh, Roohvand, Farzin, Maleki, Monireh, Shahmahmoodi, Shohreh, Amirzargar, Ali Akbar, Keshavarz, Abolfazl, Seyed, Negar, Farahmand, Mohammad, Samimi-Rad, Katayoun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7999198/
https://www.ncbi.nlm.nih.gov/pubmed/33802466
http://dx.doi.org/10.3390/vaccines9030215
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author Hajikhezri, Zamaneh
Roohvand, Farzin
Maleki, Monireh
Shahmahmoodi, Shohreh
Amirzargar, Ali Akbar
Keshavarz, Abolfazl
Seyed, Negar
Farahmand, Mohammad
Samimi-Rad, Katayoun
author_facet Hajikhezri, Zamaneh
Roohvand, Farzin
Maleki, Monireh
Shahmahmoodi, Shohreh
Amirzargar, Ali Akbar
Keshavarz, Abolfazl
Seyed, Negar
Farahmand, Mohammad
Samimi-Rad, Katayoun
author_sort Hajikhezri, Zamaneh
collection PubMed
description Feeble cellular responses induced by T cell-based vaccines are a major challenge for the development of an effective vaccine against Hepatitis C virus (HCV) infection. To address this challenge, the potential of N-terminal fragment of gp96 heat shock protein (rNT (gp96) as an adjuvant was evaluated and compared to that of the CpG (as a recognized Th1-type adjuvant) in the formulation of HCV core/NS3 antigens in three immunization strategies of protein/protein, DNA/DNA, and DNA/protein. Immunized mice were evaluated for elicited immune responses in week 3 (W3) and 11 post-immunizations. Our results demonstrated that the protein (subunit) vaccine formulated with rNT (gp96) in protein/protein strategy (core/NS3 + gp96) was significantly more efficient than CpG oligodeoxynucleotides (CpG ODN) formulation and all other immunization strategies in the induction of Th1-type cytokines. This group of mice (core/NS3 + gp96) also elicited a high level of anti-Core-NS3 total immunoglobulin G (IgG) with dominant IgG2a isotype at W3. Thus, the co-administration of recombinant NT (gp96) protein with rHCV proteins might be a promising approach in the formulation of HCV subunit vaccine candidates for induction of high levels of Th1 cytokines and humoral responses.
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spelling pubmed-79991982021-03-28 HCV Core/NS3 Protein Immunization with “N-Terminal Heat Shock gp96 Protein (rNT (gp96))” Induced Strong and Sustained Th1-Type Cytokines in Immunized Mice Hajikhezri, Zamaneh Roohvand, Farzin Maleki, Monireh Shahmahmoodi, Shohreh Amirzargar, Ali Akbar Keshavarz, Abolfazl Seyed, Negar Farahmand, Mohammad Samimi-Rad, Katayoun Vaccines (Basel) Article Feeble cellular responses induced by T cell-based vaccines are a major challenge for the development of an effective vaccine against Hepatitis C virus (HCV) infection. To address this challenge, the potential of N-terminal fragment of gp96 heat shock protein (rNT (gp96) as an adjuvant was evaluated and compared to that of the CpG (as a recognized Th1-type adjuvant) in the formulation of HCV core/NS3 antigens in three immunization strategies of protein/protein, DNA/DNA, and DNA/protein. Immunized mice were evaluated for elicited immune responses in week 3 (W3) and 11 post-immunizations. Our results demonstrated that the protein (subunit) vaccine formulated with rNT (gp96) in protein/protein strategy (core/NS3 + gp96) was significantly more efficient than CpG oligodeoxynucleotides (CpG ODN) formulation and all other immunization strategies in the induction of Th1-type cytokines. This group of mice (core/NS3 + gp96) also elicited a high level of anti-Core-NS3 total immunoglobulin G (IgG) with dominant IgG2a isotype at W3. Thus, the co-administration of recombinant NT (gp96) protein with rHCV proteins might be a promising approach in the formulation of HCV subunit vaccine candidates for induction of high levels of Th1 cytokines and humoral responses. MDPI 2021-03-03 /pmc/articles/PMC7999198/ /pubmed/33802466 http://dx.doi.org/10.3390/vaccines9030215 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) ).
spellingShingle Article
Hajikhezri, Zamaneh
Roohvand, Farzin
Maleki, Monireh
Shahmahmoodi, Shohreh
Amirzargar, Ali Akbar
Keshavarz, Abolfazl
Seyed, Negar
Farahmand, Mohammad
Samimi-Rad, Katayoun
HCV Core/NS3 Protein Immunization with “N-Terminal Heat Shock gp96 Protein (rNT (gp96))” Induced Strong and Sustained Th1-Type Cytokines in Immunized Mice
title HCV Core/NS3 Protein Immunization with “N-Terminal Heat Shock gp96 Protein (rNT (gp96))” Induced Strong and Sustained Th1-Type Cytokines in Immunized Mice
title_full HCV Core/NS3 Protein Immunization with “N-Terminal Heat Shock gp96 Protein (rNT (gp96))” Induced Strong and Sustained Th1-Type Cytokines in Immunized Mice
title_fullStr HCV Core/NS3 Protein Immunization with “N-Terminal Heat Shock gp96 Protein (rNT (gp96))” Induced Strong and Sustained Th1-Type Cytokines in Immunized Mice
title_full_unstemmed HCV Core/NS3 Protein Immunization with “N-Terminal Heat Shock gp96 Protein (rNT (gp96))” Induced Strong and Sustained Th1-Type Cytokines in Immunized Mice
title_short HCV Core/NS3 Protein Immunization with “N-Terminal Heat Shock gp96 Protein (rNT (gp96))” Induced Strong and Sustained Th1-Type Cytokines in Immunized Mice
title_sort hcv core/ns3 protein immunization with “n-terminal heat shock gp96 protein (rnt (gp96))” induced strong and sustained th1-type cytokines in immunized mice
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7999198/
https://www.ncbi.nlm.nih.gov/pubmed/33802466
http://dx.doi.org/10.3390/vaccines9030215
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