3.9 Article

In silico designing of a multi-epitope vaccine against Burkholderia pseudomallei: reverse vaccinology and immunoinformatics

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DOI: 10.1186/s43141-022-00379-4

关键词

Burkholderia; Epitope; Vaccine; B cell; T cell; Immunoinformatics

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  1. State Key Laboratories of Chemical Resources Engineering, Beijing University of Chemical Technology, Beijing, China

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In this study, an in silico approach was used to design a multi-epitope subunit vaccine peptide for Burkholderia pseudomallei, a drug-resistant infectious agent causing severe melioidosis. The designed vaccine was found to be antigenic, soluble, stable, nonallergenic, and capable of stimulating humoral and cell-mediated immune responses. In silico immune simulations showed promising results, suggesting that this approach could be a breakthrough in designing effective vaccines against B. pseudomallei globally.
Background Burkholderia pseudomallei is an infectious agent causing severe disease melioidosis resulting in pneumonia, fever, and acute septicemia in humans. B. pseudomallei show resistance to drugs. No such FDA-approved vaccine is available against B. pseudomallei, and treatment is limited to therapy. Therefore, the scientific study was designed to develop a vaccine for B. pseudomallei. The protein sequence of B. pseudomallei was retrieved from NCBI. B-cell and T-cell epitopes were identified and further screened for allergenicity, antigenicity docking, and simulation. Results Here, in this study, in silico approach was applied to design a multi-epitope subunit vaccine peptide consisting of linear B-cell and T-cell epitopes of proteins considered to be potential novel vaccine candidates. Peptide epitopes were joined by adjuvant and EAAAK, CPGPG, and AAY linkers. This constructed vaccine was subjected to in silico immune simulations by C-ImmSim. The protein construct was cloned into PET28a (+) vector for expression study in Escherichia coli using SnapGene. Conclusion The designed multi-epitope vaccine was analyzed for its physicochemical, structural, and immunological characteristics, and it was found to be antigenic, soluble, stable, nonallergenic, and have a high affinity to its target receptor. The immune simulation studies were carried out on the C-ImmSim showing increased production of cellular and humoral responses indicating that the constructed vaccine proved effective and able to provoke humoral and cell-mediated response immune responses. In silico study could be a breakthrough in designing effective vaccines to eradicate B. pseudomallei globally.

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