Inhibitory and neutral antibodies to Plasmodium falciparum MSP119 form ring structures with their antigen

Abstract Blood-stage malaria vaccine candidates include surface proteins of the merozoite. Antibodies to these proteins may either block essential steps during invasion or render the merozoite susceptible to phagocytosis or complement-mediated degradation. Structural information on merozoite surface proteins complexed to antibodies provides crucial information for knowledge-based vaccine design. The major merozoite surface protein MSP1 is an abundant surface molecule in Plasmodium falciparum . Only a subset of antibodies against MSP1 19 inhibits invasion (inhibitory antibodies), whereas other antibodies binding to MSP1 19 have no effect on invasion (neutral antibodies). Here we report on the complex of MSP1 19 with both inhibitory monoclonal antibody 12.10 and neutral monoclonal antibody 2F10. The complexes were established using both whole IgG’s and Fab fragments, and analysed by dynamic light scattering, electron microscopy and analytical ultra centrifugation. Specific ring structures were formed in the ternary complex with the two antibodies, providing direct evidence of non-overlapping epitopes on MSP1 19 . Mutational studies also indicated that the epitopes of the inhibitory and neutral antibodies are spatially remote.