| Literature DB >> 33498845 |
Julio López-Abán1, Belén Vicente1, Elías Kabbas-Piñango1, Juan Hernández-Goenaga1, Javier Sánchez-Montejo1, María Aguiriano1, Esther Del Olmo2, Magnolia Vanegas3, Manuel Alfonso Patarroyo3,4, Antonio Muro1.
Abstract
Schistosomiasis is a parasitic disease that affects 143 million people in endemic countries. This work analyzed overexpressed sequences from the cercaria phase to the early schistosomulum phase using bioinformatics tools to predict host interaction and selected proteins for predicting T cell epitopes. The final peptides were chemically synthesized, and their toxicity was evaluated in vitro. Peptides were formulated in the Adjuvant Adaptation (ADAD) vaccination system and injected into BALB/c mice that were challenged with S. mansoni cercariae to assess protection and immunogenicity. A total of 39 highly expressed S.mansoni proteins were identified as being of potential interest. Three T cell peptides predicted to bind MHC mouse and human class II were synthesized and formulated for vaccination. SmGSP and SmIKE reduced the number of eggs trapped in the liver by more than 50% in challenged BALB/c mice. The liver of mice vaccinated with either SmGSP or SmTNP had a significantly reduced affected liver surface. Transcriptome-based T cell peptides elicit partial protection and could be candidates for a multiantigen vaccine.Entities:
Keywords: ADAD vaccination system; Schistosoma mansoni; helminth vaccines; immunomodulator AA0029; synthetic peptide; transcriptome
Year: 2021 PMID: 33498845 PMCID: PMC7865475 DOI: 10.3390/jcm10030445
Source DB: PubMed Journal: J Clin Med ISSN: 2077-0383 Impact factor: 4.241