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Plasmodium vivax Reticulocyte Binding Proteins Are Key Targets of Naturally Acquired Immunity in Young Papua New Guinean Children

dc.contributor.authorFrança, Camila T.en
dc.contributor.authorHe, Wen Qiangen
dc.contributor.authorGruszczyk, Jakuben
dc.contributor.authorLim, Nicholas T.Y.en
dc.contributor.authorLin, Enmooreen
dc.contributor.authorKiniboro, Bensonen
dc.contributor.authorSiba, Peter M.en
dc.contributor.authorTham, Wai Hongen
dc.contributor.authorMueller, Ivoen
dc.date.accessioned2026-01-01T18:42:15Z
dc.date.available2026-01-01T18:42:15Z
dc.date.issued2016-09-27en
dc.description.abstractBackground: Major gaps in our understanding of Plasmodium vivax biology and the acquisition of immunity to this parasite hinder vaccine development. P. vivax merozoites exclusively invade reticulocytes, making parasite proteins that mediate reticulocyte binding and/or invasion potential key vaccine or drug targets. While protein interactions that mediate invasion are still poorly understood, the P. vivax Reticulocyte-Binding Protein family (PvRBP) is thought to be involved in P. vivax restricted host-cell selectivity.  Methodology/Principal findings: We assessed the binding specificity of five members of the PvRBP family (PvRBP1a, PvRBP1b, PvRBP2a, PvRBP2b, PvRBP2-P2 and a non-binding fragment of PvRBP2c) to normocytes or reticulocytes. PvRBP2b was identified as the only reticulocyte-specific binder (P<0.001), whereas the others preferentially bound to normocytes (PvRBP1a/b P≤0.034), or showed comparable binding to both (PvRBP2a/2-P2, P = 0.38). Furthermore, we measured levels of total and IgG subclasses 1, 2, 3 and 4 to the six PvRBPs in a cohort of young Papua New Guinean children, and assessed their relationship with prospective risk of P. vivax malaria. Children had substantial, highly correlated (rho = 0.49–0.82, P<0.001) antibody levels to all six PvRBPs, with dominant IgG1 and IgG3 subclasses. Both total IgG (Incidence Rate Ratio [IRR] 0.63–0.73, P = 0.008–0.041) and IgG1 (IRR 0.56–0.69, P = 0.001–0.035) to PvRBP2b and PvRBP1a were strongly associated with reduced risk of vivax-malaria, independently of age and exposure.  Conclusion/Significance: These results demonstrate a diversity of erythrocyte-binding phenotypes of PvRBPs, indicating binding to both reticulocyte-specific and normocyte-specific ligands. Our findings provide further insights into the naturally acquired immunity to P. vivax and highlight the importance of PvRBP proteins as targets of naturally acquired humoral immunity. In-depth studies of the role of PvRBPs in P. vivax invasion and functional validation of the role of anti-PvRBP antibodies in clinical immunity against P. vivax are now required to confirm the potential of the reticulocyte-binding PvRBP2b and PvRBP1a as vaccine candidate antigens.en
dc.description.statusPeer-revieweden
dc.format.extent17en
dc.identifier.issn1935-2727en
dc.identifier.otherORCID:/0000-0001-7950-8699/work/218987862en
dc.identifier.scopus84992036704en
dc.identifier.urihttps://hdl.handle.net/1885/733802042
dc.language.isoenen
dc.rightsPublisher Copyright: © 2016 França et al.en
dc.sourcePLoS Neglected Tropical Diseasesen
dc.titlePlasmodium vivax Reticulocyte Binding Proteins Are Key Targets of Naturally Acquired Immunity in Young Papua New Guinean Childrenen
dc.typeJournal articleen
dspace.entity.typePublicationen
local.contributor.affiliationFrança, Camila T.; Walter and Eliza Hall Institute of Medical Researchen
local.contributor.affiliationHe, Wen Qiang; University of Melbourneen
local.contributor.affiliationGruszczyk, Jakub; Walter and Eliza Hall Institute of Medical Researchen
local.contributor.affiliationLim, Nicholas T.Y.; Walter and Eliza Hall Institute of Medical Researchen
local.contributor.affiliationLin, Enmoore; Papua New Guinea Institute of Medical Researchen
local.contributor.affiliationKiniboro, Benson; Papua New Guinea Institute of Medical Researchen
local.contributor.affiliationSiba, Peter M.; Papua New Guinea Institute of Medical Researchen
local.contributor.affiliationTham, Wai Hong; University of Melbourneen
local.contributor.affiliationMueller, Ivo; Walter and Eliza Hall Institute of Medical Researchen
local.identifier.citationvolume10en
local.identifier.doi10.1371/journal.pntd.0005014en
local.identifier.pure80295414-ddad-4b2a-8a65-36c14ab93470en
local.identifier.urlhttps://www.scopus.com/pages/publications/84992036704en
local.type.statusPublisheden

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