Primary structure of the 175K Plasmodium falciparum erythrocyte binding antigen and identification of a peptide which elicits antibodies that inhibit malaria merozoite invasion.

Sim, B. Kim Lee; Orlandi, Palmer A.; Haynes, J. David; Klotz, F.; Carter, John M.; Camus, Daniel; Zegans, Michael E.; Chulay, Jeffrey D.

doi:10.1083/jcb.111.5.1877

Cited by 207 publications

(150 citation statements)

References 34 publications

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“…At 72 h after infection, the expression profile of p36 Ϫ and p52 Ϫ single knockouts and p52 Ϫ /p36 Ϫ double knockout resembled the staining profile of WT liver stages, including expression of LSA-1 (Table 3). At 144 h after infection, p36 Ϫ and p52 Ϫ continued to show expression of LSA-1, but we could not detect expression of EBA175 (a late liver-stage/blood-stage marker) (22). Staining of p52 Ϫ /p36 Ϫ liver stages at 144 h after infection could not be evaluated because no parasites were detectable at this time point with any of the tested antibodies ( The p52 Ϫ /p36 Ϫ parasites showed slightly lower gliding activity compared with WT parasites; the effect was not statistically significant at the 95% confidence level (P ϭ 0.11).…”

Section: P52-and P36-deficient P Falciparum Parasites Invade Host Cementioning

confidence: 72%

Preerythrocytic, live-attenuated Plasmodium falciparum vaccine candidates by design

VanBuskirk

O'Neill

Vega

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

153

150

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Falciparum malaria is initiated when Anopheles mosquitoes transmit the Plasmodium sporozoite stage during a blood meal. Irradiated sporozoites confer sterile protection against subsequent malaria infection in animal models and humans. This level of protection is unmatched by current recombinant malaria vaccines. However, the live-attenuated vaccine approach faces formidable obstacles, including development of accurate, reproducible attenuation techniques. We tested whether Plasmodium falciparum could be attenuated at the early liver stage by genetic engineering. The P. falciparum genetically attenuated parasites (GAPs) harbor individual deletions or simultaneous deletions of the sporozoiteexpressed genes P52 and P36. Gene deletions were done by double-cross-over recombination to avoid genetic reversion of the knockout parasites. The gene deletions did not affect parasite replication throughout the erythrocytic cycle, gametocyte production, mosquito infections, and sporozoite production rates. However, the deletions caused parasite developmental arrest during hepatocyte infection. The double-gene deletion line exhibited a more severe intrahepatocytic growth defect compared with the single-gene deletion lines, and it did not persist. This defect was assessed in an in vitro liver-stage growth assay and in a chimeric mouse model harboring human hepatocytes. The strong phenotype of the double knockout GAP justifies its human testing as a whole-organism vaccine candidate using the established sporozoite challenge model. GAPs might provide a safe and reproducible platform to develop an efficacious whole-cell malaria vaccine that prevents infection at the preerythrocytic stage.genetically attenuated parasites ͉ malaria vaccine ͉ P36 ͉ P52 ͉ sporozoite M alaria is a formidable global health problem, affecting 300 million to 500 million people worldwide annually (1). The resulting Ϸ1 million deaths per year are mainly caused by Plasmodium falciparum infections. Eradication of malaria will in large part depend on an effective vaccine that prevents infection by Plasmodium, but such a vaccine has remained elusive. The parasites' preerythrocytic stages, encompassing the mosquito-inoculated sporozoites and liver stages that develop from sporozoites after their invasion of hepatocytes, are attractive targets for antiinfection vaccines, because at this stage the number of infected host cells is low, and further transmission of the parasite is not yet possible. Occurrence of blood-stage infection after sporozoite challenge is completely preventable by immunization with radiation-attenuated sporozoites in mouse models of malaria (2). This was a landmark finding that set the standards for malaria preerythrocytic vaccine development. Radiation-attenuated sporozoites arrest in development during hepatocyte infection, but their safety and efficacy are dependent on a precise irradiation dose. Humans immunized with P. falciparum radiation-attenuated sporozoites have been effectively protected from subsequent challenge with homologous an...

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Section: P52-and P36-deficient P Falciparum Parasites Invade Host Cementioning

confidence: 72%

Preerythrocytic, live-attenuated Plasmodium falciparum vaccine candidates by design

VanBuskirk

O'Neill

Vega

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

153

150

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“…This will facilitate a more precise understanding of the significance of these antigens as targets of inhibitory antibodies. Antibodies raised in rabbits against EBA175, EBA140, PfRh1, and PfRh2b have been shown to inhibit invasion (13,17,40), further supporting their role as targets of acquired inhibitory antibodies. Antibodies raised in rabbits against PfRh4 did not inhibit invasion (20); lack of inhibitory activity may have resulted from the use of only small regions of the protein to generate antibodies.…”

Section: Figurementioning

confidence: 99%

Variation in use of erythrocyte invasion pathways by Plasmodium falciparum mediates evasion of human inhibitory antibodies

Persson¹,

McCallum²,

Reiling³

et al. 2008

J. Clin. Invest.

168

228

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Antibodies that inhibit Plasmodium falciparum invasion of erythrocytes are believed to be an important component of immunity against malaria. During blood-stage infection, P. falciparum can use different pathways for erythrocyte invasion by varying the expression and/or utilization of members of 2 invasion ligand families: the erythrocyte-binding antigens (EBAs) and reticulocyte-binding homologs (PfRhs). Invasion pathways can be broadly classified into 2 groups based on the use of sialic acid (SA) on the erythrocyte surface by parasite ligands. We found that inhibitory antibodies are acquired by malaria-exposed Kenyan children and adults against ligands of SA-dependent and SA-independent invasion pathways, and the ability of antibodies to inhibit erythrocyte invasion depended on the pathway used by P. falciparum isolates. Differential inhibition of P. falciparum lines that varied in their use of specific EBA and PfRh proteins pointed to these ligand families as major targets of inhibitory antibodies. Antibodies against recombinant EBA and PfRh proteins were acquired in an age-associated manner, and inhibitory antibodies against EBA175 appeared prominent among some individuals. These findings suggest that variation in invasion phenotype might have evolved as a mechanism that facilitates immune evasion by P. falciparum and that a broad inhibitory response against multiple ligands may be required for effective immunity.

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“…falciparum expresses multiple adhesive proteins that localize to the apical invasion organelles of the parasite, most notably members of 2 multigene families: the Erythrocyte Binding Antigen (EBA) family (Sim et al 1990 ;Peterson and Wellems, 2000 ;Thompson et al 2001 ;Gilberger et al 2003), and the P. falciparum Reticulocyte Binding Protein homologue (PfRh) family (Rayner et al 2000(Rayner et al , 2001Triglia et al 2001 ;Kaneko et al 2002 ;Cowman and Crabb, 2006). Differential expression of these proteins, particularly of members of the PfRh family, allows P. falciparum to engage alternative receptors for erythrocyte invasion, termed invasion pathways (Taylor et al 2002 ;Duraisingh et al 2003 a, b;Stubbs et al 2005 ;Triglia et al 2005).…”

Section: Introductionmentioning

confidence: 99%

Erythrocyte invasion profiles are associated with a common invasion ligand polymorphism in Senegalese isolates ofPlasmodium falciparum

et al. 2009

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S U M M A R YPlasmodium falciparum parasites use multiple ligand-receptor interactions to invade human erythrocytes. Variant expression levels of members of the PfRh and PfEBA ligand families are associated with the use of different erythrocyte receptors, defining invasion pathways. Here we analyse a major polymorphism, a large sequence deletion in the PfRh2b ligand, and erythrocyte invasion profiles in uncultured Senegalese isolates. Parasites vary considerably in their use of sialic acid-containing and protease-sensitive erythrocyte receptors for invasion. The erythrocyte selectivity index was not related to invasion pathway usage, while parasite multiplication rate was associated with enhanced use of a trypsin-resistant invasion pathway. PfRh2b protein was expressed in all parasite isolates, although the PfRh2b deletion was present in a subset (y68 %). Parasites with the PfRh2b deletion were found to preferentially utilize protease-resistant pathways for erythrocyte invasion. Sialic acid-independent invasion is reduced in parasites with the PfRh2b deletion, but only in isolates derived from blood group O patients. Our results suggest a significant role for PfRh2b sequence polymorphism in discriminating between alternative erythrocyte receptors for invasion and as a possible determinant of virulence.

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Primary structure of the 175K Plasmodium falciparum erythrocyte binding antigen and identification of a peptide which elicits antibodies that inhibit malaria merozoite invasion.

Cited by 207 publications

References 34 publications

Preerythrocytic, live-attenuated Plasmodium falciparum vaccine candidates by design

Preerythrocytic, live-attenuated Plasmodium falciparum vaccine candidates by design

Variation in use of erythrocyte invasion pathways by Plasmodium falciparum mediates evasion of human inhibitory antibodies

Erythrocyte invasion profiles are associated with a common invasion ligand polymorphism in Senegalese isolates ofPlasmodium falciparum

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