Plasmodium-infected erythrocytes induce secretion of IGFBP7 to form type II rosettes and escape phagocytosis

In malaria, rosetting is described as a phenomenon where an infected erythrocyte (IRBC) is attached to uninfected erythrocytes (URBC). In some studies, rosetting has been associated with malaria pathogenesis. Here, we have identified a new type of rosetting. Using a step-by-step approach, we identif...

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Veröffentlicht in:eLife 2020-02, Vol.9, Article 51546
Hauptverfasser: Lee, Wenn-Chyau, Russell, Bruce, Sobota, Radoslaw Mikolaj, Ghaffar, Khairunnisa, Howland, Shanshan W., Wong, Zi Xin, Maier, Alexander G., Dorin-Semblat, Dominique, Biswas, Subhra, Gamain, Benoit, Lau, Yee-Ling, Malleret, Benoit, Chu, Cindy, Nosten, Francois, Renia, Laurent
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Sprache:eng
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Zusammenfassung:In malaria, rosetting is described as a phenomenon where an infected erythrocyte (IRBC) is attached to uninfected erythrocytes (URBC). In some studies, rosetting has been associated with malaria pathogenesis. Here, we have identified a new type of rosetting. Using a step-by-step approach, we identified IGFBP7, a protein secreted by monocytes in response to parasite stimulation, as a rosette-stimulator for Plasmodium falciparum- and P. vivax-IRBC. IGFBP7-mediated rosette-stimulation was rapid yet reversible. Unlike type I rosetting that involves direct interaction of rosetting ligands on IRBC and receptors on URBC, the IGFBP7-mediated, type II rosetting requires two additional serum factors, namely von Willebrand factor and thrombospondin-1. These two factors interact with IGFBP7 to mediate rosette formation by the IRBC. Importantly, the IGFBP7-induced type II rosetting hampers phagocytosis of IRBC by host phagocytes.
ISSN:2050-084X
2050-084X
DOI:10.7554/eLife.51546