A multi-epitope vaccine designed against blood-stage of malaria: an immunoinformatic and structural approach

Atapour, Amir; Vosough, Parisa; Jafari, Somayeh; Sarab, Gholamreza Anani

doi:10.1038/s41598-022-15956-3

Cited by 13 publications

(9 citation statements)

References 63 publications

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“…In this study, like many other studies, the AAY linker was used to connect CTL epitopes [ 85 , 111 , 112 ], the GGGGS linker to connect HTL epitopes [ 113 , 114 ], the KK linker to connect LBL epitopes [ 115 – 117 ], and the EAAAK linker to connect adjuvant [ 116 , 118 , 119 ]. The AAY linkers help to increase epitope presentation while decreasing the formation of junctional epitopes [ 120 ]. The GGGGS linker, which is made up of small or polar amino acids like Gly and Ser, provides good flexibility and solubility and is an excellent choice for fusion protein domains that require specific movements or interactions [ 121 ].…”

Section: Discussionmentioning

confidence: 99%

“…The KK linker is a target for cathepsin B, a key protease in antigen processing. This linker helps in the reduction of junctional immunogenicity by preventing antibody induction for the peptide sequence formed when the individual epitopes are linearly connected [ 120 ]. The EAAAK linker is a rigid alpha-helix-forming peptide linker that functions as a domain spacer in fusion proteins [ 122 ].…”

Section: Discussionmentioning

confidence: 99%

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In silico design and immunoinformatics analysis of a universal multi-epitope vaccine against monkeypox virus

et al. 2023

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Monkeypox virus (MPXV) outbreaks have been reported in various countries worldwide; however, there is no specific vaccine against MPXV. In this study, therefore, we employed computational approaches to design a multi-epitope vaccine against MPXV. Initially, cytotoxic T lymphocyte (CTL), helper T lymphocyte (HTL), linear B lymphocytes (LBL) epitopes were predicted from the cell surface-binding protein and envelope protein A28 homolog, both of which play essential roles in MPXV pathogenesis. All of the predicted epitopes were evaluated using key parameters. A total of 7 CTL, 4 HTL, and 5 LBL epitopes were chosen and combined with appropriate linkers and adjuvant to construct a multi-epitope vaccine. The CTL and HTL epitopes of the vaccine construct cover 95.57% of the worldwide population. The designed vaccine construct was found to be highly antigenic, non-allergenic, soluble, and to have acceptable physicochemical properties. The 3D structure of the vaccine and its potential interaction with Toll-Like receptor-4 (TLR4) were predicted. Molecular dynamics (MD) simulation confirmed the vaccine’s high stability in complex with TLR4. Finally, codon adaptation and in silico cloning confirmed the high expression rate of the vaccine constructs in strain K12 of Escherichia coli (E. coli). These findings are very encouraging; however, in vitro and animal studies are needed to ensure the potency and safety of this vaccine candidate.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

In silico design and immunoinformatics analysis of a universal multi-epitope vaccine against monkeypox virus

et al. 2023

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“…Both structures fluctuated, indicating their considerable flexibility and validating it as suitable vaccine structures. Similarly, Atapour et al [58] recorded a high degree of fluctuation in the residues at positions 219 and 617 in a P. falciparum multi-epitope vaccine. The results obtained in the form of B-factor and deformability plots indicated that the molecular structures of both of the peptides were stable, and the overall stability of the VT2 constructs was higher compared to the VT1.…”

Section: Discussionmentioning

confidence: 85%

Protective Efficacy of Multiple Epitope-Based Vaccine against Hyalomma anatolicum, Vector of Theileria annulata and Crimean–Congo Hemorrhagic Fever Virus

et al. 2023

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Hyalomma anatolicum is the principal vector for Theileria annulata, T. equi, and T. Lestoquardi in animals and the Crimean–Congo hemorrhagic fever virus in humans. Due to the gradual loss of efficacy of the available acaricides against field tick populations, the development of phytoacaricides and vaccines has been considered the two most critical components of the integrated tick management strategies. In the present study, in order to induce both cellular and humoral immune responses in the host against H. anatolicum, two multi-epitopic peptides (MEPs), i.e., VT1 and VT2, were designed. The immune-stimulating potential of the constructs was determined by in silicoinvestigation on allergenicity (non-allergen, antigenic (0.46 and 1.0046)), physicochemical properties (instability index 27.18 and 35.46), as well as the interaction of constructs with TLRs by docking and molecular dynamics analysis. The immunization efficacy of the MEPs mixed with 8% MontanideTM gel 01 PR against H. anatolicum larvae was determined as 93.3% and 96.9% in VT1- and VT2-immunized rabbits, respectively. Against adults, the efficacy was 89.9% and 86.4% in VT1- and VT2-immunized rabbits, respectively. A significant (p < 0.001) reduction in the anti-inflammatory cytokine (IL-4) and significantly higher IgG response was observed in a VT1-immunized group of rabbits as compared with the response observed in the control group. However, in the case of the VT2-immunized rabbits, an elevated anti-VT2 IgG and pro-inflammatory cytokine (IL-2) (>30 fold) along with a decreased level of anti-inflammatory cytokine IL-4 (0.75 times) was noted. The efficacy of MEP and its potential immune stimulatory responses indicate that it might be useful for tick management.

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“…A multi-epitope vaccine was designed against the blood stage of P. falciparum by selecting multiple epitopes of P. falciparum glutamic acid-rich protein (PfGARP) protein. A total of 10 epitopes (5 B and 5 HTL epitopes) were linked by suitable linkers along with flagellin adjuvant to enhance the immunogenicity of the vaccine construct (169). While in silico immune simulation resulted in an elevated humoral and cellular immune response against malaria, such in silico studies need further in vitro and in vivo evaluations (169).…”

Section: Current Vaccine Approachesmentioning

confidence: 99%

“…A multi-epitope vaccine was designed against the blood stage of P. falciparum by selecting multiple epitopes of P. falciparum glutamic acid-rich protein ( Pf GARP) protein. A total of 10 epitopes (5 B and 5 HTL epitopes) were linked by suitable linkers along with flagellin adjuvant to enhance the immunogenicity of the vaccine construct ( 169 ). While in silico immune simulation resulted in an elevated humoral and cellular immune response against malaria, such in silico studies need further in vitro and in vivo evaluations ( 169 ).…”

Section: Vaccine Candidates Against Plasmodiummentioning

confidence: 99%

Host-parasite interactions during Plasmodium infection: Implications for immunotherapies

et al. 2023

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Malaria is a global infectious disease that remains a leading cause of morbidity and mortality in the developing world. Multiple environmental and host and parasite factors govern the clinical outcomes of malaria. The host immune response against the Plasmodium parasite is heterogenous and stage-specific both in the human host and mosquito vector. The Plasmodium parasite virulence is predominantly associated with its ability to evade the host’s immune response. Despite the availability of drug-based therapies, Plasmodium parasites can acquire drug resistance due to high antigenic variations and allelic polymorphisms. The lack of licensed vaccines against Plasmodium infection necessitates the development of effective, safe and successful therapeutics. To design an effective vaccine, it is important to study the immune evasion strategies and stage-specific Plasmodium proteins, which are targets of the host immune response. This review provides an overview of the host immune defense mechanisms and parasite immune evasion strategies during Plasmodium infection. Furthermore, we also summarize and discuss the current progress in various anti-malarial vaccine approaches, along with antibody-based therapy involving monoclonal antibodies, and research advancements in host-directed therapy, which can together open new avenues for developing novel immunotherapies against malaria infection and transmission.

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A multi-epitope vaccine designed against blood-stage of malaria: an immunoinformatic and structural approach

Cited by 13 publications

References 63 publications

In silico design and immunoinformatics analysis of a universal multi-epitope vaccine against monkeypox virus

In silico design and immunoinformatics analysis of a universal multi-epitope vaccine against monkeypox virus

Protective Efficacy of Multiple Epitope-Based Vaccine against Hyalomma anatolicum, Vector of Theileria annulata and Crimean–Congo Hemorrhagic Fever Virus

Host-parasite interactions during Plasmodium infection: Implications for immunotherapies

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