TY - JOUR
T1 - Complement receptor 1 availability on red blood cell surface modulates Plasmodium vivax invasion of human reticulocytes
AU - Prajapati, Surendra Kumar
AU - Borlon, Céline
AU - Rovira-Vallbona, Eduard
AU - Gruszczyk, Jakub
AU - Menant, Sebastien
AU - Wai-Hong Tham, null
AU - Kattenberg, Johanna Helena
AU - Villasis, Elizabeth
AU - De Meulenaere, Katlijn
AU - Gamboa, Dionicia
AU - Vinetz, Joseph
AU - Fujita, Ricardo
AU - Xa Nguyen Xuan, null
AU - Ferreira, Marcelo Urbano
AU - Nino, Carlos H.
AU - Patarroyo, Manuel A.
AU - Spanakos, Gregory
AU - Kestens, Luc
AU - Van Den Abbeele, Jan
AU - Rosanas-Urgell, Anna
N1 - FTX; DOAJ; (CC BY 4.0)
PY - 2019
Y1 - 2019
N2 - Plasmodium vivax parasites preferentially invade reticulocyte cells in a multistep process that is still poorly understood. In this study, we used ex vivo invasion assays and population genetic analyses to investigate the involvement of complement receptor 1 (CR1) in P. vivax invasion. First, we observed that P. vivax invasion of reticulocytes was consistently reduced when CR1 surface expression was reduced through enzymatic cleavage, in the presence of naturally low-CR1-expressing cells compared with high-CR1-expressing cells, and with the addition of soluble CR1, a known inhibitor of P. falciparum invasion. Immuno-precipitation experiments with P. vivax Reticulocyte Binding Proteins showed no evidence of complex formation. In addition, analysis of CR1 genetic data for worldwide human populations with different exposure to malaria parasites show significantly higher frequency of CR1 alleles associated with low receptor expression on the surface of RBCs and higher linkage disequilibrium in human populations exposed to P. vivax malaria compared with unexposed populations. These results are consistent with a positive selection of low-CR1-expressing alleles in vivax-endemic areas. Collectively, our findings demonstrate that CR1 availability on the surface of RBCs modulates P. vivax invasion. The identification of new molecular interactions is crucial to guiding the rational development of new therapeutic interventions against vivax malaria.
AB - Plasmodium vivax parasites preferentially invade reticulocyte cells in a multistep process that is still poorly understood. In this study, we used ex vivo invasion assays and population genetic analyses to investigate the involvement of complement receptor 1 (CR1) in P. vivax invasion. First, we observed that P. vivax invasion of reticulocytes was consistently reduced when CR1 surface expression was reduced through enzymatic cleavage, in the presence of naturally low-CR1-expressing cells compared with high-CR1-expressing cells, and with the addition of soluble CR1, a known inhibitor of P. falciparum invasion. Immuno-precipitation experiments with P. vivax Reticulocyte Binding Proteins showed no evidence of complex formation. In addition, analysis of CR1 genetic data for worldwide human populations with different exposure to malaria parasites show significantly higher frequency of CR1 alleles associated with low receptor expression on the surface of RBCs and higher linkage disequilibrium in human populations exposed to P. vivax malaria compared with unexposed populations. These results are consistent with a positive selection of low-CR1-expressing alleles in vivax-endemic areas. Collectively, our findings demonstrate that CR1 availability on the surface of RBCs modulates P. vivax invasion. The identification of new molecular interactions is crucial to guiding the rational development of new therapeutic interventions against vivax malaria.
KW - FRAGMENT-LENGTH-POLYMORPHISM
KW - RICH ANTIGEN PVTRAG38
KW - ERYTHROCYTE RECEPTOR
KW - GENE POLYMORPHISMS
KW - BINDING DOMAIN
KW - FALCIPARUM
KW - CR-1
KW - MALARIA
KW - IDENTIFICATION
KW - EXPRESSION
U2 - 10.1038/s41598-019-45228-6
DO - 10.1038/s41598-019-45228-6
M3 - A1: Web of Science-article
C2 - 31221984
SN - 2045-2322
VL - 9
JO - Scientific Reports
JF - Scientific Reports
IS - 1
M1 - 8943
ER -