International Journal of Molecular Sciences (Feb 2021)

Two 20-Residue-Long Peptides Derived from <i>Plasmodium vivax</i> Merozoite Surface Protein 10 EGF-Like Domains Are Involved in Binding to Human Reticulocytes

  • Laura Alejandra Ricaurte-Contreras,
  • Andrea Lovera,
  • Darwin Andrés Moreno-Pérez,
  • Michel David Bohórquez,
  • Carlos Fernando Suárez,
  • Elizabeth Gutiérrez-Vásquez,
  • Laura Cuy-Chaparro,
  • Diego Garzón-Ospina,
  • Manuel Alfonso Patarroyo

DOI
https://doi.org/10.3390/ijms22041609
Journal volume & issue
Vol. 22, no. 4
p. 1609

Abstract

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Plasmodium parasites’ invasion of their target cells is a complex, multi-step process involving many protein-protein interactions. Little is known about how complex the interaction with target cells is in Plasmodium vivax and few surface molecules related to reticulocytes’ adhesion have been described to date. Natural selection, functional and structural analysis were carried out on the previously described vaccine candidate P. vivax merozoite surface protein 10 (PvMSP10) for evaluating its role during initial contact with target cells. It has been shown here that the recombinant carboxyl terminal region (rPvMSP10-C) bound to adult human reticulocytes but not to normocytes, as validated by two different protein-cell interaction assays. Particularly interesting was the fact that two 20-residue-long regions (388DKEECRCRANYMPDDSVDYF407 and 415KDCSKENGNCDVNAECSIDK434) were able to inhibit rPvMSP10-C binding to reticulocytes and rosette formation using enriched target cells. These peptides were derived from PvMSP10 epidermal growth factor (EGF)-like domains (precisely, from a well-defined electrostatic zone) and consisted of regions having the potential of being B- or T-cell epitopes. These findings provide evidence, for the first time, about the fragments governing PvMSP10 binding to its target cells, thus highlighting the importance of studying them for inclusion in a P. vivax antimalarial vaccine.

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