AI Article Synopsis
- SERA5 is a promising candidate antigen for a malaria subunit vaccine, as it plays a key role in the life cycle of the malaria parasite during merozoite release and reinvasion.
- Researchers developed synthetic phosphatidylethanolamine (PE)-peptide conjugates to create a peptide that stimulates strong immune responses, successfully identifying an optimal sequence from SERA5.
- Monoclonal antibodies created against the effective peptide demonstrated the ability to recognize SERA5 in various forms, confirming its presence in sporozoites and making the virosomal formulation a viable candidate for human vaccination.
Article Abstract
Serine repeat antigen-5 (SERA5) is a candidate antigen for inclusion into a malaria subunit vaccine. During merozoite release and reinvasion the 120 kDa SERA5 precursor protein (P120) is processed, and a complex consisting of an N-terminal 47 kDa (P47) and a C-terminal 18kDa (P18) processing product associates with the surface of merozoites. This complex is thought to be involved in merozoite invasion of and/or egress from host erythrocytes. Here we describe the synthesis and immunogenic properties of virosomally formulated synthetic phosphatidylethanolamine (PE)-peptide conjugates, incorporating amino acid sequence stretches from the N-terminus of Plasmodium falciparum SERA5. Choosing an appropriate sequence was crucial for the development of a peptide that elicited high titers of parasite cross-reactive antibodies in mice. Monoclonal antibodies (mAbs) raised against the optimized peptide FB-23 incorporating amino acids 57-94 of SERA5 bound to both P120 and to P47. Western blotting analysis proved for the first time the presence of SERA5 P47 in sporozoites. In immunofluorescence assays, the mAbs stained SERA5 in all its predicted localizations. The virosomal formulation of peptide FB-23 is suitable for use in humans and represents a candidate component for a multi-valent malaria subunit vaccine targeting both sporozoites and blood stage parasites.
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| http://dx.doi.org/10.1016/j.peptides.2007.08.007 | DOI Listing |
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