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Infect. Immun., 04 1996, 1373-1378, Vol 64, No. 4
L Xiao, C Yang, PS Patterson, V Udhayakumar and AA Lal
Sulfated proteoglycans have been shown to be involved in the binding of
sporozoites of malaria parasites to hepatocytes. In this study, we have
evaluated the effect of sulfated glycosaminoglycans on the invasion of
erythrocytes by Plasmodium falciparum merozoites and cytoadherence of
parasitized erythrocytes (PRBC) to endothelial cells. Invasion of
erythrocytes by HB3EC-6 (an HB3 line selected for high binding to
endothelial cells) was inhibited by dextran sulfate 500K, dextran sulfate
5K, sulfatides, fucoidan, and heparin but not by chondroitin sulfate A.
With the exception of sulfatides, the invasion-inhibitory effect was not
mediated by killing of parasites. Cytoadherence of HB3EC- 6 to human
microvascular endothelial cells (HMEC-1) and inhibited by these sulfated
glycoconjugates. The highly sulfated dextran sulfate 500K had the highest
inhibitory effect on both invasion and cytoadherence, whereas the
positively charged protamine sulfate promoted cytoadherence. Because
preincubation of PRBC with sulfated glycosaminoglycans and treatment of
target cells with heparinase had no significant inhibition on
cytoadherence, it is unlikely that sulfated glycoconjugates are used
directly by endothelial cells as cytoadhesion receptors. In an vivo
experiment, we found that the administration of dextran sulfate 500K to
CBA/Ca mice infected with Plasmodium berghei ANKA reduced parasitemia and
delayed the death associated with anemia. These observations suggest that
sulfated polyanions inhibit the invasion of erythrocytes by merozoites and
cytoadherence of PRBC to endothelial cells by increasing negative repulsive
charge and sterically interfering with the ligand-receptor interaction
after binding to target cells.
Copyright © 1996, American Society for Microbiology
Sulfated polyanions inhibit invasion of erythrocytes by plasmodial merozoites and cytoadherence of endothelial cells to parasitized erythrocytes
Division of Parasitic Diseases, Centers for Disease Control and Prevention, Atlanta, Georgia, 30341, USA.
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