Using the PfEMP1 head structure binding motif to deal a blow at severe malaria

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Abstract

Plasmodium falciparum (Pf) malaria causes 200 million cases worldwide, 8 million being severe and complicated leading to ,1 million deaths and ∼100,000 abortions annually. Plasmodium falciparum erythrocyte membrane protein 1 (Pf EMP1) has been implicated in cytoadherence and infected erythrocyte rosette formation, associated with cerebral malaria; chondroitin sulphate-A attachment and infected erythrocyte sequestration related to pregnancy-associated malaria and other severe forms of disease. An endothelial cell high activity binding peptide is described in several of this ∼300 kDa hypervariable protein's domains displaying a conserved motif (GACxPxRRxxLC); it established H-bonds with other binding peptides to mediate red blood cell group A and chondroitin sulphate attachment. This motif (when properly modified) induced PfEMP1-specific strain-transcending, fully-protective immunity for the first time in experimental challenge in Aotus monkeys, opening the way forward for a long sought-after vaccine against severe malaria. © 2014 Patarroyo et al.

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Patarroyo, M. E., Alba, M. P., Curtidor, H., Vanegas, M., Almonacid, H., & Patarroyo, M. A. (2014). Using the PfEMP1 head structure binding motif to deal a blow at severe malaria. PLoS ONE, 9(2). https://doi.org/10.1371/journal.pone.0088420

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