Human erythrocyte band 3 is a host receptor for Plasmodium falciparum glutamic acid–rich protein

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Abstract

Malaria remains a major global threat to human health and economic development. Mi-crovascular lesions caused by Plasmodium falciparum–infected human erythrocytes/red blood cells are hallmarks of severe pathogenesis contributing to high mortality, particularly in children from sub-Saharan Africa. In this study, we used a phage display complementary DNA library screening strategy to identify P falciparum glutamic acid–rich protein (PfGARP) as a secreted ligand that recognizes an ectodomain of human erythrocyte anion-exchanger, band 3/AE1, as a host receptor. Domain mapping of PfGARP revealed distinct nonoverlapping repeats encoding the immune response epitopes and core erythrocyte-binding activity. Synthetic peptides derived from the erythrocyte-binding repeats of PfGARP induced erythrocyte aggregation reminiscent of the rosetting phenomenon. Using peptides derived from the immunogenic repeats, a quantitative immunoassay was developed to detect a selective immune response against PfGARP in human plasma samples obtained from patients in rural Mali, suggesting the feasibility of PfGARP as a potential biomarker of disease progression. Collectively, our results suggest that PfGARP may play a functional role in enhancing the adhesive properties of human erythrocytes by engaging band 3 as a host receptor. We propose that immunological and pharmacological inhibition of PfGARP may unveil new therapeutic options for mitigating lesions in cerebral and pregnancy-associated malaria.

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Almukadi, H., Schwake, C., Kaiser, M. M., Ghislaine Mayer, D. C., Schiemer, J., Baldwin, M. R., … Chishti, A. H. (2019). Human erythrocyte band 3 is a host receptor for Plasmodium falciparum glutamic acid–rich protein. Blood, 133(5), 470–480. https://doi.org/10.1182/blood-2018-07-865451

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