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Development of multi-epitope vaccines against the monkeypox virus based on envelope proteins using immunoinformatics approaches
Development of multi-epitope vaccines against the monkeypox virus based on envelope proteins using immunoinformatics approaches
by Zhu, Fei , Tan, Caixia , Wu, Anhua , Pan, Pinhua , Li, Chunhui
in Accuracy / Adjuvants / Antigens / Bacterial infections / Cytokines / Cytotoxicity / Disease / Drb1 protein / Epitopes / Epitopes, T-Lymphocyte / Histocompatibility antigen HLA / Humans / Immune response / Immunogenicity / immunoinformatics / Immunology / Lymphocytes / Major histocompatibility complex / molecular docking / Molecular Docking Simulation / Molecular dynamics / molecular dynamics (MD) simulation / Monkeypox virus / monkeypox virus (MPXV) / Mpox / Mpox (monkeypox) / multi-epitope vaccine / Peptides / Physicochemical properties / Proteins / Smallpox / TLR2 protein / TLR4 protein / Toll-like receptors / Toxicity / Vaccines / Vaccines, Subunit / Viral envelope proteins / Virions / Viruses / Zoonoses
2023
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Development of multi-epitope vaccines against the monkeypox virus based on envelope proteins using immunoinformatics approaches
by Zhu, Fei , Tan, Caixia , Wu, Anhua , Pan, Pinhua , Li, Chunhui
in Accuracy / Adjuvants / Antigens / Bacterial infections / Cytokines / Cytotoxicity / Disease / Drb1 protein / Epitopes / Epitopes, T-Lymphocyte / Histocompatibility antigen HLA / Humans / Immune response / Immunogenicity / immunoinformatics / Immunology / Lymphocytes / Major histocompatibility complex / molecular docking / Molecular Docking Simulation / Molecular dynamics / molecular dynamics (MD) simulation / Monkeypox virus / monkeypox virus (MPXV) / Mpox / Mpox (monkeypox) / multi-epitope vaccine / Peptides / Physicochemical properties / Proteins / Smallpox / TLR2 protein / TLR4 protein / Toll-like receptors / Toxicity / Vaccines / Vaccines, Subunit / Viral envelope proteins / Virions / Viruses / Zoonoses
2023
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Development of multi-epitope vaccines against the monkeypox virus based on envelope proteins using immunoinformatics approaches
Development of multi-epitope vaccines against the monkeypox virus based on envelope proteins using immunoinformatics approaches
by Zhu, Fei , Tan, Caixia , Wu, Anhua , Pan, Pinhua , Li, Chunhui
in Accuracy / Adjuvants / Antigens / Bacterial infections / Cytokines / Cytotoxicity / Disease / Drb1 protein / Epitopes / Epitopes, T-Lymphocyte / Histocompatibility antigen HLA / Humans / Immune response / Immunogenicity / immunoinformatics / Immunology / Lymphocytes / Major histocompatibility complex / molecular docking / Molecular Docking Simulation / Molecular dynamics / molecular dynamics (MD) simulation / Monkeypox virus / monkeypox virus (MPXV) / Mpox / Mpox (monkeypox) / multi-epitope vaccine / Peptides / Physicochemical properties / Proteins / Smallpox / TLR2 protein / TLR4 protein / Toll-like receptors / Toxicity / Vaccines / Vaccines, Subunit / Viral envelope proteins / Virions / Viruses / Zoonoses
2023

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Development of multi-epitope vaccines against the monkeypox virus based on envelope proteins using immunoinformatics approaches
Development of multi-epitope vaccines against the monkeypox virus based on envelope proteins using immunoinformatics approaches
Journal Article

Development of multi-epitope vaccines against the monkeypox virus based on envelope proteins using immunoinformatics approaches

Zhu, Fei,
Tan, Caixia,
Wu, Anhua,
Pan, Pinhua,
Li, Chunhui
2023
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Overview
Since May 2022, cases of monkeypox, a zoonotic disease caused by the monkeypox virus (MPXV), have been increasingly reported worldwide. There are, however, no proven therapies or vaccines available for monkeypox. In this study, several multi-epitope vaccines were designed against the MPXV using immunoinformatics approaches. Three target proteins, A35R and B6R, enveloped virion (EV) form-derived antigens, and H3L, expressed on the mature virion (MV) form, were selected for epitope identification. The shortlisted epitopes were fused with appropriate adjuvants and linkers to vaccine candidates. The biophysical andbiochemical features of vaccine candidates were evaluated. The Molecular docking and molecular dynamics(MD) simulation were run to understand the binding mode and binding stability between the vaccines and Toll-like receptors (TLRs) and major histocompatibility complexes (MHCs). The immunogenicity of the designed vaccines was evaluated via immune simulation. Five vaccine constructs (MPXV-1-5) were formed. After the evaluation of various immunological and physicochemical parameters, MPXV-2 and MPXV-5 were selected for further analysis. The results of molecular docking showed that the MPXV-2 and MPXV-5 had a stronger affinity to TLRs (TLR2 and TLR4) and MHC (HLA-A*02:01 and HLA-DRB1*02:01) molecules, and the analyses of molecular dynamics (MD) simulation have further confirmed the strong binding stability of MPXV-2 and MPXV-5 with TLRs and MHC molecules. The results of the immune simulation indicated that both MPXV-2 and MPXV-5 could effectively induce robust protective immune responses in the human body. The MPXV-2 and MPXV-5 have good efficacy against the MPXV in theory, but further studies are required to validate their safety and efficacy.
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Publisher
Frontiers Media SA,Frontiers Media S.A
Subject

Accuracy

/ Adjuvants

/ Antigens

/ Bacterial infections

/ Cytokines

/ Cytotoxicity

/ Disease

/ Drb1 protein

/ Epitopes

/ Epitopes, T-Lymphocyte

/ Histocompatibility antigen HLA

/ Humans

/ Immune response

/ Immunogenicity

/ immunoinformatics

/ Immunology

/ Lymphocytes

/ Major histocompatibility complex

/ molecular docking

/ Molecular Docking Simulation

/ Molecular dynamics

/ molecular dynamics (MD) simulation

/ Monkeypox virus

/ monkeypox virus (MPXV)

/ Mpox

/ Mpox (monkeypox)

/ multi-epitope vaccine

/ Peptides

/ Physicochemical properties

/ Proteins

/ Smallpox

/ TLR2 protein

/ TLR4 protein

/ Toll-like receptors

/ Toxicity

/ Vaccines

/ Vaccines, Subunit

/ Viral envelope proteins

/ Virions

/ Viruses

/ Zoonoses

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