Associations between Responses to the Rhoptry-Associated Membrane Antigen of
            <i>Plasmodium falciparum</i>
            and Immunity to Malaria Infection

Topolska, Agnieszka Ewa; Richie, Thomas L.; Nhan, Doan Hanh; Coppel, Ross L.

doi:10.1128/iai.72.6.3325-3330.2004

Cited by 32 publications

(25 citation statements)

References 24 publications

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“…In humans, both IgG1 and IgG3 have high affinities for Fc receptors, fix complement, and are preferentially induced during Th1-type responses, but IgG3 appears to be a more efficient mediator of FcR crosslinking and phagocyte activation (8,22). Consistent with this, IgG3 antibodies to various blood-stage antigens are particularly effective mediators of antibody-dependent cellular inhi- (5) and have been repeatedly associated with the acquisition of clinical immunity to malaria (12,14,29,42,45,48). These data make a strong case for trying to engineer antimalarial vaccines to induce high titers of IgG3 antibodies, but this will only be feasible when we have a better understanding of the requirements for induction of IgG3 class switching in human B cells.…”

Section: Discussionmentioning

confidence: 61%

Target Antigen, Age, and Duration of Antigen Exposure Independently Regulate Immunoglobulin G Subclass Switching in Malaria

et al. 2006

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The isotype/subclass of immunoglobulin determines antibody function, but rather little is known about factors that direct class switching in vivo. To evaluate factors that might influence the maturation of the antibody response during infection, we conducted a seroepidemiological study of the immunoglobulin G (IgG) subclass response to four merozoite-associated antigens of Plasmodium falciparum in a mountainous region of northeastern Tanzania, where malaria endemicity declines with increasing altitudes. We found that IgG1/IgG3 class switching is independently affected by the nature of the antigen, cumulative exposure to the antigen, and the maturity of the immune system (i.e., the age of the individual). These observations provide insights into the effects of immune system maturity, the duration and intensity of antigen exposure, and inherent characteristics of individual antigens on the process of class switching in human B cells. Our data also throw light on the consequences of class switch decisions on the gradual acquisition of antimalarial immunity.The isotype/subclass of immunoglobulin determines antibody function (e.g., complement fixation or the activation of phagocytes), and in humans, immunoglobulin G1 (IgG1) and IgG3 are important mediators of pathogen clearance. Specific combinations of cytokines and B-cell activators have been shown to induce class switching to certain isotypes or subclasses in model systems (13), but less is known about factors that direct class switching in vivo during infection. While it has long been suspected that characteristics of antigens themselves influence class switching in B cells (41,43), and while some antigens induce characteristic patterns of Ig class switching, most notably (in humans) encapsulated bacteria (IgG2) (27, 28) and allergens and helminths (IgG4 and IgE) (20), the characteristics of antigens that induce switching to human IgG1 and IgG3 are not well described.Numerous studies have reported that IgG subclass profiles differ among antibodies targeted to different malarial antigens, with the best example being the tendency of merozoite surface protein 2 (MSP-2) to induce very strong IgG3 responses (39,46), in contrast to the tendency of the C terminus of MSP-1, MSP-1 19 , to induce IgG1 or a mixed IgG1/IgG3 response (7,18). Here we demonstrate that characteristics of antigens per se can regulate the IgG1/IgG3 class switch, in that different antigens of Plasmodium falciparum, the causative agent of the virulent form of human malaria, elicit entirely different antibody subclasses even though they are presented to the immune system at the same time and as part of the same single-celled organism (i.e., the malaria merozoite). To evaluate the effects of antigens per se, immune system maturity (age), and cumulative exposure to antigens (which varies according to the intensity of malaria transmission) on the maturation of the IgG response, we conducted a seroepidemiological study in a mountainous region of northeastern Tanzania, where malaria endemicity declines wi...

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Section: Discussionmentioning

confidence: 61%

Target Antigen, Age, and Duration of Antigen Exposure Independently Regulate Immunoglobulin G Subclass Switching in Malaria

et al. 2006

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“…These results suggest that mice were protected. Plasmodium merozoite rhoptry proteins contribute to blood stage immunity and are important targets for a blood stage vaccine (Holder and Freeman 1981;Jakobsen et al 1993Jakobsen et al , 1996Facer and Tanner 1997;Collins et al 2000;Toploska et al 2004;Nixon et al 2005). The Rhop-3 protein, along with other merozoite rhoptry proteins participates in membrane raft formation and parasitophorous vacuole formation during erythrocyte invasion (Hiller et al 2003;Toploska et al 2003).…”

Section: Rhop-3 Transmembrane Domain Conservationmentioning

confidence: 98%

Rhop-3 protein conservation among Plasmodium species and induced protection against lethal P. yoelii and P. berghei challenge

et al. 2006

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In the present study, Rhop-3 polymorphism among Plasmodium falciparum field and laboratory isolates and among rodent Plasmodium species was investigated and identified. The Rhop-3 gene was found in all Plasmodium species so far tested. The overall structure of the Rhop-3 protein was found conserved among P. falciparum, Plasmodium yoelii, and Plasmodium berghei. However, it was more conserved among rodent Plasmodium species than between P. falciparum and Plasmodium vivax. The most conserved regions of Rhop-3 are the second half of exon 6 (amino acid #548 to #665) and the beginning of exon 3 (amino acid #59 to #210). Recombinant C-terminal partial and full-length Rhop-3 proteins of P. yoelii and P. berghei were expressed in Escherichia coli and purified. Immunization-challenge experiments in mice using recombinant Rhop-3 proteins led to a delay in parasite development and protected mice from a homologous lethal challenge infection. In a group of eight outbred Carworth Farm White (CFW) mice immunized with P. yoelii C-terminal recombinant His-Y1412 protein, three mice (37.5%) were protected from a lethal P. yoelii challenge. In BALB/cJ mice one mouse (20%) survived the infection. Immunization of mice with P. berghei recombinant full-length Rhop-3 protein in BALB/cJ mice led to a 40% survival from lethal P. berghei challenge. CFW mice immunized with P. berghei recombinant full-length Rhop-3 protein showed a significant delay in parasite development with a heterologous P. yoelii challenge. The Rhop-3 protein is a promising candidate for an asexual stage malaria vaccine.

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“…Intriguingly, however, no functional equivalent of RAMA has to date been found in other Apicomplexan spp. It should also be noted that because the C-terminus of RAMA is embedded within the lipid bilayer [30], an unidentified TM escorter protein would have to be present in vesicles at the Golgi exit face, interacting with both RAMA and the cytosolic sorting machinery to escort these protein complexes to nascent rhoptries.…”

Section: The Rhoptries and Its Constituentsmentioning

confidence: 99%

Plasmodium rhoptry proteins: why order is important

Counihan

Kalanon

Coppel

et al. 2013

Trends in Parasitology

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101

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Associations between Responses to the Rhoptry-Associated Membrane Antigen of Plasmodium falciparum and Immunity to Malaria Infection

Cited by 32 publications

References 24 publications

Target Antigen, Age, and Duration of Antigen Exposure Independently Regulate Immunoglobulin G Subclass Switching in Malaria

Target Antigen, Age, and Duration of Antigen Exposure Independently Regulate Immunoglobulin G Subclass Switching in Malaria

Rhop-3 protein conservation among Plasmodium species and induced protection against lethal P. yoelii and P. berghei challenge

Plasmodium rhoptry proteins: why order is important

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