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A NOVEL MULTI-EPITOPE PEPTIDE VACCINE CONSTRUCT AGAINST INFLUENZA A VIRUS AND STREPTOCOCCUS PNEUMONIAE CO-INFECTION: AN IN SILICO APPROACH


Article Information

Title: A NOVEL MULTI-EPITOPE PEPTIDE VACCINE CONSTRUCT AGAINST INFLUENZA A VIRUS AND STREPTOCOCCUS PNEUMONIAE CO-INFECTION: AN IN SILICO APPROACH

Authors: Maha Kaiser, Amjad Ali

Journal: NUST Journal of Natural Sciences

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Y 2024-10-01 2025-12-31
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Y 2021-07-01 2022-06-30

Publisher: National University of Sciences & Technology, Rawalpindi/Islamabad (NUST)

Country: Pakistan

Year: 2018

Volume: 4

Issue: 2

Language: en

DOI: 10.53992/njns.v4i2.7

Keywords: Co-infectionStreptococcus pneumoniaeInfluenza A virusMulti-epitope

Categories

Abstract

Viral and bacterial respiratory tract co-infections in the same host often result in severity and heightened pathology of illness compared to single infections. This has proven to be true for combined infections with Influenza A virus and the bacterium Streptococcus pneumoniae. Separate vaccines do exist for each individual infection but they prove to be ineffective and non-specific when the infection has multiplied in case of co-infection. The study utilised in silico approaches and proposed a structural design for multi-epitope peptide vaccine having the ability to target co-infection caused by A/New York/392/2004 (H3N2) and R6 strains of Influenza A virus (NCBI Accession: PRJNA15622) and Streptococcus pneumoniae (NCBI Accession: PRJNA278), respectively. Epitope prediction followed by protein prioritization was performed using the reference sequence of each strain to short list the epitopes that can later be used for constructing multi-epitope structure. The multi-epitope constructs having Cholera Toxin Subunit B as adjuvant and (Gly4Ser)3 as flexible linker were then analyzed for their ability to induce an effective immune response in human body for which Macrophage receptor with collagenous structure, Toll-like receptor 2, 4 and 5 were taken as Pattern Recognition Receptors. The significant immune response generated through each Pattern Recognition Receptor helped to conclude that multi-epitope peptide structures can be used as probable candidates for the design of vaccine. The combination of the epitopes LWSYNAELL and FTGKQLQVG of Influenza A virus and Streptococcus pneumoniae, respectively, induced highly significant immune response in case of each Pattern Recognition Receptor when tested through in-silico predictive tools.


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