Analysis of antibody responses to selected <i>Plasmodium falciparum </i>merozoite surface antigens in mild and cerebral malaria and associations with clinical outcomes

Mbengué, Babacar; Fall, Mansour; Varela, Marie Louise; Loucoubar, Cheikh; Joos, Charlotte; Fall, B.; Niang, Maguette Sylla; Niang, Birahim; Mbow, Moustapha; Dièye, Alioune; Perraut, Ronald

doi:10.1111/cei.13254

Cited by 15 publications

(19 citation statements)

References 55 publications

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“…Mice selectively deficient in IgM experience greater parasitemia and mortality compared with wild-type mice upon infection with Plasmodium chabaudi , a model for uncomplicated Plasmodium falciparum infection ( Couper et al, 2005 ). Anti-parasite IgM antibodies arising from natural exposure can activate complement to inhibit growth of Plasmodium parasites in vitro and are significantly associated with protection from clinical malaria in human cohorts ( Boyle et al, 2019 ; Kurtovic et al, 2018 ; Mbengue et al, 2019 ). Studies of genetically distinct ethnic groups in West Africa, who experience identical parasite exposure but exhibit different susceptibilities to malaria, have found that resistant and susceptible groups display strongly divergent breadth and magnitude of Plasmodium -specific IgM responses, whereas IgG responses are far more similar between groups ( Bolad et al, 2005 ; Arama et al, 2015 ).…”

Section: Introductionmentioning

confidence: 99%

Multimeric antibodies from antigen-specific human IgM+ memory B cells restrict Plasmodium parasites

Thouvenel¹,

Fontana

Netland

et al. 2021

Journal of Experimental Medicine

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Multimeric immunoglobulin-like molecules arose early in vertebrate evolution, yet the unique contributions of multimeric IgM antibodies to infection control are not well understood. This is partially due to the difficulty of distinguishing low-affinity IgM, secreted rapidly by plasmablasts, from high-affinity antibodies derived from later-arising memory cells. We developed a pipeline to express B cell receptors (BCRs) from Plasmodium falciparum–specific IgM+ and IgG+ human memory B cells (MBCs) as both IgM and IgG molecules. BCRs from both subsets were somatically hypermutated and exhibited comparable monomeric affinity. Crystallization of one IgM+ MBC-derived antibody complexed with antigen defined a linear epitope within a conserved Plasmodium protein. In its physiological multimeric state, this antibody displayed exponentially higher antigen binding than a clonally identical IgG monomer, and more effectively inhibited P. falciparum invasion. Forced multimerization of this IgG significantly improved both antigen binding and parasite restriction, underscoring how avidity can alter antibody function. This work demonstrates the potential of high-avidity IgM in both therapeutics and vaccines.

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Section: Introductionmentioning

confidence: 99%

Multimeric antibodies from antigen-specific human IgM+ memory B cells restrict Plasmodium parasites

Thouvenel¹,

Fontana

Netland

et al. 2021

Journal of Experimental Medicine

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“…MSP2 falls into two dimorphic types (Type A and B) represented here by the CH150/9 (type A) and Dd2 (type B) ( 52 ). Despite the level of repetition within the MSP2 proteins studies have used a single allele of MSP2 in combination with other recombinant targets to describe immunity to infection ( 64 ), or have opted for representative sequences from both major dimorphic types as has been done for this study. Lastly, the MSP2-C1 blood stage vaccine is also based on a single representative type from each of the dimorphic classifications (3D7 and Fc27) ( 65 , 66 ).…”

Section: Discussionmentioning

confidence: 99%

Impact of a Rapid Decline in Malaria Transmission on Antimalarial IgG Subclasses and Avidity

et al. 2021

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Understanding how immunity to malaria is affected by declining transmission is important to aid vaccine design and understand disease resurgence. Both IgG subclasses and avidity of antigen-specific responses are important components of an effective immune response. Using a multiplex bead array assay, we measured the total IgG, IgG subclasses, and avidity profiles of responses to 18 P. falciparum blood stage antigens in samples from 160 Ugandans collected at two time points during high malaria transmission and two time points following a dramatic reduction in transmission. Results demonstrated that, for the antigens tested, (i) the rate of decay of total IgG following infection declined with age and was driven consistently by the decrease in IgG3 and occasionally the decrease in IgG1; (ii) the proportion of IgG3 relative to IgG1 in the absence of infection increased with age; (iii) the increase in avidity index (the strength of association between the antibody and antigen) following infection was largely due to a rapid loss of non-avid compared to avid total IgG; and (iv) both avid and non-avid total IgG in the absence of infection increased with age. Further studies are required to understand the functional differences between IgG1 and IgG3 in order to determine their contribution to the longevity of protective immunity to malaria. Measuring changes in antibody avidity may be a better approach of detecting affinity maturation compared to avidity index due to the differential expansion and contraction of high and low avidity total IgG.

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“…Schizonts stage parasites were harvested and lysed in three volumes of sterile distilled water and stored into aliquotes in liquid nitrogen [43]. The MSP3 antigen (clone T9/96) was an E. coli-expressed DG-210 puri ed protein 28 (kind gift from Dr C. Oeuvray) [44].The ELISA assay was performed as previously described [33,44]. The 0703 crude extract was set to 1/3000 dilution by a doseeffect assay using positive control sera.…”

Section: Antigen Preparation and Elisa Assaymentioning

confidence: 99%

“…Results were expressed as optical density (OD) ratio calculated as follow: mean OD sample/mean OD naive serum pool. Sera with an OD ratio > 2 were considered as positive response for prevalence calculations [44] (Mbengue, B et al, 2019). Variations between tests for positive controls should not exceed 20 %.…”

Section: Immunological Parametersmentioning

confidence: 99%

Immune tolerance to asymptomatic submicroscopic Plasmodium falciparum infections in adults living in malaria endemic areas

Diouf

Diop

Dièye

et al. 2020

Preprint

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Background Combined malaria control interventions have reduced mortality rate, number of clinical cases and parasite prevalence across Africa between 2000 and 2015. As a consequence, Plasmodium infections have become mostly asymptomatic and often sub-microscopic in many endemic areas. The present study aims to evaluate the contribution of asymptomatic sub-microscopic P. falciparum carriage on antibody responses against malaria antigens. Methods A total of 353 samples from a cross-sectional sampling conducted in Ndiop (Senegal) in 2016 were tested by qPCR and microscopy to determine parasite prevalence. Plasmodium falciparum positive samples were genotyped using msp-2 marker. The IgG seroprevalence against crude schizont antigen of a local P. falciparum strain, tested by ELISA, was compared to parasite prevalence. An age-matched, under 10 years, 10-15 and over 15 years cohort of 110 positive and negative qPCR samples were used to determine the impact of sub-microscopic carriage on IgG and IgM antibody responses against schizont extract and MSP3 recombinant antigen. Results The microscopic diagnosis was negative for all thick smears defining a study cohort of submicroscopic asymptomatic individuals with an overall parasite prevalence of 22.37% (79/353) by qPCR. Submicroscopic infections were associated with significant lower IgG responses in qPCR positive samples for individuals over 15 years of age, for both crude schizont (p=0.021) and MSP3 recombinant antigen (p=0.035). IgM responses were significantly higher (p=0.034) in children under 10 years, showing their susceptibility to primary infection. Above 15 years of age, a significant difference was found between parasite prevalence of 9.3% (33/353) and IgG seroprevalence of 23.8% (84/353) (p=0.01). The overall genetic diversity detected is characterized by a complexity of infection (COI) and a number of genotypes of 2.4 and 17, respectively.Conclusion Asymptomatic submicroscopic P. falciparum carriage is prevalent in the study area and is associated with immune tolerance to parasites in adults. The difference between parasite prevalence and IgG seroprevalence results from long-lived IgG in adults point out attention for elders in endemic areas as a stable parasite reservoir. In this context, mass molecular detection followed by treatment could be a valuable method for achieving elimination.

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Analysis of antibody responses to selected Plasmodium falciparum merozoite surface antigens in mild and cerebral malaria and associations with clinical outcomes

Cited by 15 publications

References 55 publications

Multimeric antibodies from antigen-specific human IgM+ memory B cells restrict Plasmodium parasites

Multimeric antibodies from antigen-specific human IgM+ memory B cells restrict Plasmodium parasites

Impact of a Rapid Decline in Malaria Transmission on Antimalarial IgG Subclasses and Avidity

Immune tolerance to asymptomatic submicroscopic Plasmodium falciparum infections in adults living in malaria endemic areas

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