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DENV-3 precursor membrane (prM) glycoprotein enhances E protein immunogenicity and confers protection against DENV-2 infections in a murine model.
Dias, Roberto S; Teixeira, Michelle D; Xisto, Mariana F; Prates, John W O; Silva, Jessica D Da; Mello, Iago O; Silva, Cynthia C Da; De Paula, Sérgio O.
Afiliação
  • Dias RS; Laboratory of Molecular Immunovirology, Department of General Biology, Federal University of Viçosa, Viçosa (MG), Brazil.
  • Teixeira MD; Laboratory of Molecular Immunovirology, Department of General Biology, Federal University of Viçosa, Viçosa (MG), Brazil.
  • Xisto MF; Laboratory of Molecular Immunovirology, Department of General Biology, Federal University of Viçosa, Viçosa (MG), Brazil.
  • Prates JWO; Department of Microbiology, Federal University of Viçosa, Viçosa (MG), Brazil.
  • Silva JDD; Laboratory of Molecular Immunovirology, Department of General Biology, Federal University of Viçosa, Viçosa (MG), Brazil.
  • Mello IO; Laboratory of Molecular Immunovirology, Department of General Biology, Federal University of Viçosa, Viçosa (MG), Brazil.
  • Silva CCD; Department of Microbiology, Federal University of Viçosa, Viçosa (MG), Brazil.
  • De Paula SO; Laboratory of Molecular Immunovirology, Department of General Biology, Federal University of Viçosa, Viçosa (MG), Brazil.
Hum Vaccin Immunother ; 17(5): 1271-1277, 2021 05 04.
Article em En | MEDLINE | ID: mdl-33121347
To improve a DNA vaccine containing the truncated dengue virus serotype 2 (DENV-2) envelope (E) protein and evaluate the influence of precursor membrane (prM) glycoprotein polymorphism on E protein immunogenicity, two vaccine candidates have been constructed by upstream insertion of the DENV-2 and DENV-3 prM genes into the DENV-2 E gene, named pCID2EtD2prM and pCID2EtD3prM, respectively. Both constructs were able to induce antibody production, which were neutralizing against DENV-2 in a murine model. Splenocytes of immunized groups, when challenged with virus, demonstrated Th1 cytokine pattern and proliferation, in addition to the increase of specific T cells. Vaccine candidates pCID2EtD2prM and pCID2EtD3prM confer 70% and 90% protection against DENV-2, respectively. The pCID2EtD3prM plasmid conferred only 40% protection in the lethal challenge with DENV-2. The results demonstrate that DENV-3 prM has a greater influence on the immunogenicity of the E protein and, probably due to its role as a chaperone, these results may be related to the correct folding and, consequently, an increase in the presentation efficiency of produced transcripts.
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Dengue / Vírus da Dengue / Vacinas contra Dengue Idioma: En Ano de publicação: 2021 Tipo de documento: Article

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Dengue / Vírus da Dengue / Vacinas contra Dengue Idioma: En Ano de publicação: 2021 Tipo de documento: Article