4.1 Article

Molecular Characterization and Designing of a Novel Multiepitope Vaccine Construct Against Pseudomonas aeruginosa

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SPRINGER
DOI: 10.1007/s10989-021-10356-z

关键词

Pseudomonas aeruginosa; Major membrane protein; Immunoinformatics; Multi-peptide vaccine; Epitope

资金

  1. DBT-BUILDER program at KIIT Deemed to Be University, Bhubaneswar [BT/INF/22/SP42155/2021]

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In this study, a computational approach was used to design a vaccine against Pseudomonas aeruginosa infection. The vaccine, containing peptides from B-cells and T-cells, showed good immunogenic and biophysical properties. Through various experiments, the vaccine demonstrated promising efficacy in preventing Pseudomonas aeruginosa infection.
Pseudomonas aeruginosa, an ESKAPE pathogen causes many fatal clinical diseases in humans across the globe. Despite an increase in clinical instances of Pseudomonas infection, there is currently no effective vaccine or treatment available. The major membrane protein candidate of the P. aeruginosa bacterial cell is known to be a critical component for cellular bacterial susceptibility to antimicrobial peptides and survival inside the host organisms. Therefore, the current computational study aims to examine P. aeruginosa's major membrane protein, OprF, and OprI, in order to design linear B-cell, cytotoxic T-cell, and helper T-cell peptide-based vaccine constructs. Utilizing various immune-informatics tools and databases, a total of two B-cells and twelve T-cells peptides were predicted. The final vaccine design was simulated to generate a high-quality three-dimensional structure, which included epitopes, adjuvant, and linkers. The vaccine was shown to be nonallergenic, antigenic, soluble, and had the best biophysical properties. The vaccine and Toll-like receptor 4 have a strong and stable interaction, according to protein-protein docking and molecular dynamics simulations. Additionally, in silico cloning was employed to see how the developed vaccine expressed in the pET28a (+) vector. Ultimately, an immune simulation was performed to see the vaccine efficacy. In conclusion, the newly developed vaccine appears to be a promising option for a vaccine against P. aeruginosa infection. [GRAPHICS] .

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