Identification of Plasmodium falciparum RhopH3 protein peptides that specifically bind to erythrocytes and inhibit merozoite invasion

doi:10.1110/ps.035923.108

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Published online before print July 1, 2008
Protein Science, DOI: 10.1110/ps.035923.108
Copyright © 2008 The Protein Society
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Identification of Plasmodium falciparum RhopH3 protein peptides that specifically bind to erythrocytes and inhibit merozoite invasion

Carlos G Pinzon¹, Hernando Curtidor², Claudia Reyes¹, David Mendez¹, and Manuel Elkin Patarroyo³^,4

¹ Fundacion Instituto de Inmunologia de Colombia FIDIC;
² Fundacion Instituto de Inmunologia de Colombia FIDIC branch Universidad del Rosario;
³ Fundacion Instituto de Inmunologia de Colombia FIDIC and Universidad Nacional de Colombia

(RECEIVED April 21, 2008; ACCEPTED June 25, 2008)

The identification of sequences involved in binding to erythrocytesis an important step for understanding the molecular basis ofmerozoite-erythrocyte interactions that take place during invasionof the Plasmodium falciparum malaria parasite into host cells.Several molecules located in the apical organelles (micronemes,rhoptry, dense granules) of the invasive-stage parasite areessential for erythrocyte recognition, invasion and establishmentof the nascent parasitophorous vacuole. Particularly, it hasbeen demonstrated that rhoptry proteins play an important rolein binding to erythrocyte surface receptors, amongst which isthe PfRhopH3 protein, which triggers important immune responsesin patients from endemic regions. It has also been reportedthat anti-RhopH3 antibodies inhibit in vitro invasion of erythrocytes,further supporting its direct involvement in erythrocytes invasionprocesses. In this study, PfRhopH3 consecutive peptides weresynthesised and tested in erythrocyte binding assays for identifyingthose regions mediating binding to erythrocytes. Fourteen PfRhopH3peptides presenting high specific binding activity were found,whose binding were saturable and presented nanomolar dissociationconstants. These high activity binding peptides (HABPs) werecharacterised by having ${alpha}$ -helical structural elements as determinedby CD; and receptors of possible sialic acid-dependent and/orglycoprotein-dependent nature, as evidenced in enzyme-treatederythrocyte binding assays and further corroborated by cross-linkingassay results. Furthermore, these HABPs inhibited merozoitein vitro invasion of normal erythrocytes at 200 µM byup to 60% and 90%, suggesting that some RhopH3 protein regionsare involved in the P. falciparum erythrocyte invasion.

Keywords: High activity binding peptides; Malaria; Plasmodium falciparum; RhopH3 protein

⁴ E-mail: mepatarr{at}mail.com

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