Literature DB >> 32016547

Protective cellular immune response against hepatitis C virus elicited by chimeric protein formulations in BALB/c mice.

Santa Olivera1, Angel Perez2, Viviana Falcon3, Dioslaida Urquiza4, Dagmara Pichardo4, Gillian Martinez-Donato2.   

Abstract

The eradication of hepatitis C virus (HCV) infection is a public health priority. Despite the efficiency of treatment with direct-acting antivirals, the high cost of the therapy and the lack of accurate data about the HCV-infected population worldwide constitute important factors hampering this task. Hence, an affordable preventive vaccine is still necessary for reducing transmission and the future disease burden globally. In this work, chimeric proteins (EnvCNS3 and NS3EnvCo) encompassing conserved and immunogenic epitopes from the HCV core, E1, E2 and NS3 proteins were produced in Escherichia coli, and their immunogenicity was evaluated in BALB/c mice. The impact of recombinant HCV E2.680 protein and oligodeoxynucleotide 39M (ODN39M) on the immune response to chimeric proteins was also assessed. Immunization with chimeric proteins mixed with E2.680 enhanced the antibody and cellular response against HCV antigens and chimeric proteins. Interestingly, the combination of NS3EnvCo with E2.680 and ODN39M as adjuvant elicited a potent antibody response characterized by an increase in antibodies of the IgG2a subclass against E2.680, NS3 and chimeric proteins, suggesting the induction of a Th1-type response. Moreover, a cytotoxic T lymphocyte response and a broad response of IFN-γ-secreting cells against HCV antigens were induced with this formulation as well. This T cell response was able to protect vaccinated mice against challenge with a surrogate model based on HCV recombinant vaccinia virus. Overall, the vaccine candidate NS3EnvCo/E2.680/ODN39M might constitute an effective immunogen against HCV with potential for reducing the likelihood of viral persistence.

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Year:  2020        PMID: 32016547      PMCID: PMC7224087          DOI: 10.1007/s00705-019-04464-x

Source DB:  PubMed          Journal:  Arch Virol        ISSN: 0304-8608            Impact factor:   2.574


  63 in total

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4.  Neutralizing antibodies and broad, functional T cell immune response following immunization with hepatitis C virus proteins-based vaccine formulation.

Authors:  Gillian Martinez-Donato; Yalena Amador-Cañizares; Liz Alvarez-Lajonchere; Ivis Guerra; Angel Pérez; Jean Dubuisson; Czeslaw Wychowsk; Alexis Musacchio; Daylen Aguilar; Santiago Dueñas-Carrera
Journal:  Vaccine       Date:  2014-01-30       Impact factor: 3.641

5.  Vaccine-induced early control of hepatitis C virus infection in chimpanzees fails to impact on hepatic PD-1 and chronicity.

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Review 6.  CpG DNA as a vaccine adjuvant.

Authors:  Christian Bode; Gan Zhao; Folkert Steinhagen; Takeshi Kinjo; Dennis M Klinman
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8.  The protein DIIIC-2, aggregated with a specific oligodeoxynucleotide and adjuvanted in alum, protects mice and monkeys against DENV-2.

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Journal:  J Hepatol       Date:  2014-07-30       Impact factor: 25.083

10.  Rapid induction of virus-neutralizing antibodies and viral clearance in a single-source outbreak of hepatitis C.

Authors:  Jan M Pestka; Mirjam B Zeisel; Edith Bläser; Peter Schürmann; Birke Bartosch; Francois-Loïc Cosset; Arvind H Patel; Helga Meisel; Jens Baumert; Sergei Viazov; Kay Rispeter; Hubert E Blum; Michael Roggendorf; Thomas F Baumert
Journal:  Proc Natl Acad Sci U S A       Date:  2007-03-28       Impact factor: 11.205

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Review 2.  Structure-Based and Rational Design of a Hepatitis C Virus Vaccine.

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Journal:  Viruses       Date:  2021-05-05       Impact factor: 5.818

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

Authors:  Zamaneh Hajikhezri; Farzin Roohvand; Monireh Maleki; Shohreh Shahmahmoodi; Ali Akbar Amirzargar; Abolfazl Keshavarz; Negar Seyed; Mohammad Farahmand; Katayoun Samimi-Rad
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4.  Development and immunobiological evaluation of nanoparticles containing an immunodominant epitope of herpes simplex virus.

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