<i>Plasmodium falciparum</i>-specific IgM B cells dominate in children, expand with malaria and produce parasite inhibitory IgM

Hopp, Christine S.; Diouf, Ababacar; Miura, Kazutoyo; Boswell, Kristin L.; Sekar, Padmapriya; Skinner, Jeff; Tipton, Christopher; Chambers, Michael; Andrews, Sarah F.; Tan, Joshua; Li, Shanping; Doumbo, Safiatou; Kayentao, Kassoum; Ongoïba, Aïssata; Traoré, Boubacar; Portugal, Sílvia; Long, Carole A.; Koup, Richard A.; Long, Eric O.; McDermott, Adrian B.; Crompton, Peter D.

doi:10.1101/2020.04.12.030049

Cited by 5 publications

(5 citation statements)

References 61 publications

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“…Indeed, Pf-specific IgM levels should be considered confident serological markers of malaria exposure. Although IgM has been associated by other authors with some protection against malaria given its effector role in complement fixation (Kurtovic et al, 2021), opsonic phagocytosis (Hopp et al, 2021), and clonal selection (Murugan et al, 2018), our data do not directly associate population levels of IgM with protection against the disease. However, it cannot be excluded that progressive exposure to the parasite with age and the associated increase in IgM levels in adults may have some degree of immunological functionality, as the lowest levels of parasitemia were the most frequent in the adult population, and precisely those uninfected adults showed the highest Pf-IgM levels of all age groups.…”

Section: Discussioncontrasting

confidence: 86%

“…Regarding IgM, it has been described as a marker of malaria exposure in travelers (Orlandi-Pradines et al, 2006), and Plasmodium-specific IgM memory B cells are recognized as early responders to malaria re-infection providing a strategical protection barrier until IgG is generated (Krishnamurty et al, 2016). Moreover, IgM has been suggested to contribute to human parasite clearance (Boudin et al, 1993;Bolad et al, 2005;Arama et al, 2015;Boyle et al, 2019;Hopp et al, 2021;Kurtovic et al, 2021), which may highlight an underestimated role of IgM in protecting against the frequent malaria reinfections in endemic regions (Krishnamurty et al, 2016). On the other hand, IgA has been shown as an exposure marker in children (Duah et al, 2010) and induced by vaccination with human vaccine RTS,S/AS 01E (Suau et al, 2021).…”

Section: Introductionmentioning

confidence: 99%

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Microscopic and submicroscopic infection by Plasmodium falciparum: Immunoglobulin M and A profiles as markers of intensity and exposure

Abad

Marín-García

Heras

et al. 2022

Front. Cell. Infect. Microbiol.

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Assessment of serological Plasmodium falciparum–specific antibodies in highly endemic areas provides valuable information about malaria status and parasite exposure in the population. Although serological evidence of Plasmodium exposure is commonly determined by Plasmodium-specific immunoglobulin G (IgG) levels; IgM and IgA are likely markers of malaria status that remain relatively unexplored. Previous studies on IgM and IgA responses have been based on their affinity for single antigens with shortage of immune responses analysis against the whole Plasmodium proteome. Here, we provide evidence of how P. falciparum infection triggers the production of specific IgM and IgA in plasma and its relationship with parasite density and changes in hematological parameters. A total of 201 individuals attending a hospital in Breman Asikuma, Ghana, were recruited into this study. Total and P. falciparum–specific IgM, IgA, and IgG were assessed by ELISA and examined in relation to age (0–5, 14–49, and ≥50 age ranges); infection (submicroscopic vs. microscopic malaria); pregnancy and hematological parameters. Well-known IgG response was used as baseline control. P. falciparum–specific IgM and IgA levels increased in the population with the age, similarly to IgG. These data confirm that acquired humoral immunity develops by repeated infections through the years endorsing IgM and IgA as exposure markers in endemic malaria regions. High levels of specific IgA and IgM in children were associated with microscopic malaria and worse prognosis, because most of them showed severe anemia. This new finding shows that IgM and IgA may be used as diagnostic markers in this age group. We also found an extremely high prevalence of submicroscopic malaria (46.27% on average) accompanied by IgM and IgA levels indistinguishable from those of uninfected individuals. These data, together with the observed lack of sensitivity of rapid diagnostic tests (RDTs) compared to PCR, invoke the urgent need to implement diagnostic markers for submicroscopic malaria. Overall, this study opens the potential use of P. falciparum–specific IgM and IgA as new serological markers to predict malaria status in children and parasite exposure in endemic populations. The difficulties in finding markers of submicroscopic malaria are highlighted, emphasizing the need to explore this field in depth.

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Section: Discussioncontrasting

confidence: 86%

Section: Introductionmentioning

confidence: 99%

Microscopic and submicroscopic infection by Plasmodium falciparum: Immunoglobulin M and A profiles as markers of intensity and exposure

Abad

Marín-García

Heras

et al. 2022

Front. Cell. Infect. Microbiol.

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“…Although we found no evidence of rapid induction of IgM + MBCs into IgM-secreting cells, this does not diminish the potential importance of these cells to the recall response in humans. In particular, Ag-specific IgM + MBCs are identifiable in the blood of individuals from malaria-endemic regions, 37,40,62 and they can produce IgM Abs capable of neutralizing and promoting opsonization. 62 These Ag-specific IgM + MBCs were more abundant than their swIg + counterparts, even after years of repeated Plasmodium infections, 62 Lastly, as markers used to identify MBC populations continue to be defined and their function and biological role on MBCs is deduced, the challenge will be to determine if human MBCs similarly express these markers and if they display a similar functional role.…”

Section: Discussionmentioning

confidence: 99%

“…In particular, Ag-specific IgM + MBCs are identifiable in the blood of individuals from malaria-endemic regions, 37,40,62 and they can produce IgM Abs capable of neutralizing and promoting opsonization. 62 These Ag-specific IgM + MBCs were more abundant than their swIg + counterparts, even after years of repeated Plasmodium infections, 62 suggesting their capacity to play a protective role from severe disease and illustrating the inefficient acquisition of protective IgG responses against Plasmodium. Although, the reduced rate of somatically mutated BCRs in IgM + MBCs may make them better suited to recognize a broader range of variant P. falciparum Ags.…”

Section: Discussionmentioning

confidence: 99%

IgM⁺and IgM^-memory B cells represent heterogeneous populations capable of producing class-switched antibodies and germinal center B cells upon re-challenge withP. yoelii

Brown

et al. 2021

Preprint

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Memory B cells (MBCs) are essential for maintaining long-term humoral immunity to infectious organisms, including Plasmodium. MBCs are a heterogeneous population whose function can be dictated by isotype or expression of particular surface proteins. Here, aided by the use of antigen-specific B cell tetramers, MBC populations were evaluated to discern their phenotype and function in response to infection with a non-lethal strain of P. yoelii. Infection of mice with P. yoelii 17X resulted in the production of three predominant MBC populations: somatically hypermutated isotype-switched (swIg+) and IgM+ MBCs that co-expressed CD73 and CD80, and CD73-CD80- unmutated swIg+ B cells. Re-challenge experiments indicated that IgG-producing cells dominated the recall response with minimal induction of IgM-secreting cells. Furthermore, using fluorescent protein expression as a surrogate for CD73 and CD80 co-expression, ZsGreen1+IgM+ MBCs gave rise to class switched IgG-producing plasmablasts that induced comparable titers of Ag-specific Abs as their swIg+ counterparts after adoptive transfer and P. yoelii infection. Moreover, ZsGreen1+ IgM+ and swIg+ MBCs gave rise to B cells with a germinal center phenotype. Together these data indicated that MBC function is not defined by immunoglobulin isotype, nor does co-expression of key surface markers limit the potential fate of MBCs after recall.

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“…Although the role of IgG and its subclasses is significant in host to symptomatic malaria infection, the role of IgM must not be ignored. Particularly, the protective role of IgM against the blood-stage parasite of P. falciparum has been established [120][121][122].…”

Section: Antibody-mediated Immunitymentioning

confidence: 99%

Plasmodium falciparum Malaria Vaccines and Vaccine Adjuvants

et al. 2021

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Malaria—a parasite vector-borne disease—is a global health problem, and Plasmodium falciparum has proven to be the deadliest among Plasmodium spp., which causes malaria in humans. Symptoms of the disease range from mild fever and shivering to hemolytic anemia and neurological dysfunctions. The spread of drug resistance and the absence of effective vaccines has made malaria disease an ever-emerging problem. Although progress has been made in understanding the host response to the parasite, various aspects of its biology in its mammalian host are still unclear. In this context, there is a pressing demand for the development of effective preventive and therapeutic strategies, including new drugs and novel adjuvanted vaccines that elicit protective immunity. The present article provides an overview of the current knowledge of anti-malarial immunity against P. falciparum and different options of vaccine candidates in development. A special emphasis has been made on the mechanism of action of clinically used vaccine adjuvants.

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Plasmodium falciparum-specific IgM B cells dominate in children, expand with malaria and produce parasite inhibitory IgM

Cited by 5 publications

References 61 publications

Microscopic and submicroscopic infection by Plasmodium falciparum: Immunoglobulin M and A profiles as markers of intensity and exposure

Microscopic and submicroscopic infection by Plasmodium falciparum: Immunoglobulin M and A profiles as markers of intensity and exposure

IgM⁺and IgM^-memory B cells represent heterogeneous populations capable of producing class-switched antibodies and germinal center B cells upon re-challenge withP. yoelii

Plasmodium falciparum Malaria Vaccines and Vaccine Adjuvants

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Plasmodium falciparum-specific IgM B cells dominate in children, expand with malaria and produce parasite inhibitory IgM

Cited by 5 publications

References 61 publications

Microscopic and submicroscopic infection by Plasmodium falciparum: Immunoglobulin M and A profiles as markers of intensity and exposure

Microscopic and submicroscopic infection by Plasmodium falciparum: Immunoglobulin M and A profiles as markers of intensity and exposure

IgM+and IgM-memory B cells represent heterogeneous populations capable of producing class-switched antibodies and germinal center B cells upon re-challenge withP. yoelii

Plasmodium falciparum Malaria Vaccines and Vaccine Adjuvants

Contact Info

Product

Resources

About

IgM⁺and IgM^-memory B cells represent heterogeneous populations capable of producing class-switched antibodies and germinal center B cells upon re-challenge withP. yoelii