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Ordered mesoporous silicas for potential applications in solid vaccine formulations

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Miranda, Matheus C. R. ; Nunes, Carmen M. ; Santos, Luana F. ; da Silva, Leonardo B. ; de Jesus, Vinicius R. ; Andreo Filho, Newton ; Pedro, Jessica A. F. ; Lopes, Jose L. S. ; Oliveira, Cristiano L. P. ; Fantini, Marcia C. A. ; Cardoso, Jessica S. ; Trezena, Aryene G. ; Ribeiro, Orlando G. ; Sant'Anna, Osvaldo A. ; Tino-De-Franco, Milene ; Martins, Tereza S.
Número total de Autores: 16
Tipo de documento: Artigo Científico
Fonte: Vaccine; v. 42, n. 3, p. 12-pg., 2024-02-01.
Resumo

In an effort to develop efficient vaccine formulations, the use of ordered mesoporous silica (SBA -15) as an antigen carrier has been investigated. SBA -15 has required properties such as high surface area and pore volume, including narrow pore size distribution to protect antigens inside its matrix. This study aimed to examine the impact of solvent removal methods, specifically freeze-drying and evaporation on the intrinsic properties of an immunogenic complex. The immunogenic complexes, synthesized and incorporated with BSA, were characterized by various physicochemical techniques. Small Angle X-ray Scattering measurements revealed the characteristic reflections associated to pure SBA -15, indicating the preservation of the silica mesostructured following BSA incorporation and the formation of BSA aggregates within the macropore region. Nitrogen Adsorption Isotherm measurements demonstrated a decrease in surface area and pore volume for all samples, indicating that the BSA was incorporated into the SBA -15 matrix. Fluorescence spectroscopy evidenced that the tryptophan residues in BSA inside SBA -15 or in solution displayed similar spectra, showing the preservation of the aromatic residues' environment. The Circular Dichroism spectra of BSA in both conditions suggest the preservation of its native secondary structure after the encapsulation process. The immunogenic analysis with the detection of antiBSA IgG did not give any significant difference between the non -dried, freeze-dried or evaporated groups. However, all groups containing BSA and SBA -15 showed results almost three times higher than the groups with pure BSA (control group). These facts indicate that none of the BSA incorporation methods interfered with the immunogenicity of the complex. In particular, the freeze-dried process is regularly used in the pharmaceutical industry, therefore its adequacy to produce immunogenic complexes was proved Furthermore, the results showed that SBA -15 increased the immunogenic activity of BSA. (AU)

Processo FAPESP: 19/08582-5 - EMU concedido no processo 17/17844-8:Analisador térmico - TG/DTA modelo sta 2500 TG/DTA TEMP. ambiente a 1100 °c
Beneficiário:Tereza da Silva Martins
Modalidade de apoio: Auxílio à Pesquisa - Programa Equipamentos Multiusuários
Processo FAPESP: 22/08360-5 - Estudo da influência das propriedades morfológicas da SBA-15 na eficácia de moléculas com potencial terapêutico e vacinas
Beneficiário:Matheus Carlos Romeiro Miranda
Modalidade de apoio: Bolsas no Brasil - Pós-Doutorado
Processo FAPESP: 19/19567-7 - Estudos estruturais de proteínas incorporadas em sílica mesoporosas ordenada
Beneficiário:Jéssica Aparecida Ferreira Pedro
Modalidade de apoio: Bolsas no Brasil - Mestrado
Processo FAPESP: 22/01951-8 - Estudo da integridade química e estrutural de partículas semelhantes a vírus e sua incorporação em sílica mesoporosa ordenada
Beneficiário:Jose Luiz de Souza Lopes
Modalidade de apoio: Auxílio à Pesquisa - Projeto Inicial