Development of an immunogen containing CD4+/CD8+ T‐cell epitopes for the prophylaxis of tegumentary leishmaniasis.
Data
2022
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Resumo
Tegumentary leishmaniasis (TL) is a disease of high severity and incidence in Brazil, and Leishmania braziliensis is its main
etiological agent. The inefciency of control measures, such as high toxicity and costs of current treatments and the lack of
efective immunoprophylactic strategies, makes the development of vaccines indispensable and imminent. In this light, the
present work developed a gene encoding multiple T-cell (CD4+/CD8+) epitope, derived from conserved proteins found in
Leishmania species and associated with TL, to generate a chimeric protein (rMEP/TL) and compose a vaccine formulation.
For this, six T-cell epitopes were selected by immunoinformatics approaches from proteins present in the amastigote stage
and associated with host-parasite interactions. The following formulations were then tested in an L. braziliensis murine
infection model: rMEP/TL in saline or associated with MPLA-PHAD®. Our data revealed that, after immunization (three
doses; 14-day intervals) and subsequent challenging, rMEP/TL and rMEP/TL+MPLA-vaccinated mice showed an increased
production of key immunological biomarkers of protection, such as IgG2a, IgG2a/IgG1, NO, CD4+, and CD8+ T-cells with
IFN-γ and TNF-α production, associated with a reduction in CD4+IL-10+ and CD8+IL-10+ T-cells. Vaccines also induced the
development of central (CD44highCD62Lhigh) and efector (CD44highCD62Llow) memory of CD4+ and CD8+ T-cells. These
fndings, associated with the observation of lower rates of parasite burdens in the vaccinated groups, when compared to the
control groups, suggest that immunization with rMEP/TL and, preferably, associated with an adjuvant, may be considered
an efective tool to prevent TL.
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Leishmania braziliensis, Vaccine, Immunoinformatics, T-cell epitope mapping, Chimeric protein
Citação
FERRAZ, I. de A. et al. Development of an immunogen containing CD4+/CD8+ T‐cell epitopes for the prophylaxis of tegumentary leishmaniasis. Applied Microbiology and Biotechnology, v. 106, p. 4627-4641, 2022. Disponível em: <https://link.springer.com/article/10.1007/s00253-022-12033-7>. Acesso em: 01 ago. 2023.