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Computational design, expression, and characterization of a Plasmodium falciparum multi-epitope, multi-stage vaccine candidate (PfCTMAG)

Heliyon. 2025-01; 
Joan A Chick, Nadege N Abongdia, Robert A Shey, Tobias O Apinjoh
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Bacterial Expression The DNA sequence of PfCTMAG was sent to GenScript (Netherlands) for optimization, synthesis, and cloning into a pET-30a (+) vector. The quality check performed after receiving the candidate from GenScript validated its presence and integrity (Fig. 5B). SDS-PAGE Gels: Gel obtained by GenScript after expression and purification (A). Gel obtained from quality check after receiving the candidate from GenScript (B). Get A Quote

Abstract

Malaria, a tropical disease, claims the lives of thousands of people annually and the development of resistance to insecticides and antimalarial drugs poses a great challenge to current prevention and control strategies. Current malaria vaccines are limited in efficacy, duration of protection, and safety, due to the high antigenic diversity and complex life cycle of the Plasmodium parasite. This study sought to design and assess a more effective multi-stage, multi-epitope vaccine candidate for the control of malaria. A multi-epitope malaria vaccine candidate was designed in silico using multiple antigens from both the pre-erythrocytic and erythrocytic stages, expressed in bacteria, and its sero-reactivity to an... More

Keywords

Immunogenicity; In silico; Multi-epitope; Sero-reactivity; Vaccine candidate.