Global diversity and balancing selection of 23 leading Plasmodium falciparum candidate vaccine antigens

Naung, Myo; Martin, E. A.; Munro, Jacob E.; Mehra, Somya; Guy, Andrew; Laman, Moses; Harrison, G. L. Abby; Tavul, Livingstone; Hetzel, Manuel W; Kwiatkowski, Dominic P.; Müeller, Ivo; Bahlo, Melanie; Barry, Alyssa E.

doi:10.1371/journal.pcbi.1009801

Cited by 22 publications

(22 citation statements)

References 110 publications

(205 reference statements)

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“…Exploration of the Plasmodium gene expression database shows that these genes were preferentially expressed in the asexual blood-stage parasites, which suggests the importance of these correlates in protection against blood-stage malaria. Indeed, the protective role of naturally acquired anti-MSP4 antibodies has been shown previously 32 , 33 . With that said, we also observed an early decrease in the frequencies of IFNγ-producing CD4 + T cells in TBS − subjects, which could indicate migration into lymph nodes and tissues, to facilitate parasite control 34 .…”

Section: Discussionmentioning

confidence: 82%

Immunological profiles associated with distinct parasitemic states in volunteers undergoing malaria challenge in Gabon

Manurung

Jong

Kruize

et al. 2022

Sci Rep

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Controlled human malaria infection (CHMI) using cryopreserved non-attenuated Plasmodium falciparum sporozoites (PfSPZ) offers a unique opportunity to investigate naturally acquired immunity (NAI). By analyzing blood samples from 5 malaria-naïve European and 20 African adults with lifelong exposure to malaria, before, 5, and 11 days after direct venous inoculation (DVI) with SanariaR PfSPZ Challenge, we assessed the immunological patterns associated with control of microscopic and submicroscopic parasitemia. All (5/5) European individuals developed parasitemia as defined by thick blood smear (TBS), but 40% (8/20) of the African individuals controlled their parasitemia, and therefore remained thick blood smear-negative (TBS− Africans). In the TBS− Africans, we observed higher baseline frequencies of CD4+ T cells producing interferon-gamma (IFNγ) that significantly decreased 5 days after PfSPZ DVI. The TBS− Africans, which represent individuals with either very strong and rapid blood-stage immunity or with immunity to liver stages, were stratified into subjects with sub-microscopic parasitemia (TBS-PCR+) or those with possibly sterilizing immunity (TBS−PCR−). Higher frequencies of IFNγ+TNF+CD8+ γδ T cells at baseline, which later decreased within five days after PfSPZ DVI, were associated with those who remained TBS−PCR−. These findings suggest that naturally acquired immunity is characterized by different cell types that show varying strengths of malaria parasite control. While the high frequencies of antigen responsive IFNγ+CD4+ T cells in peripheral blood keep the blood-stage parasites to a sub-microscopic level, it is the IFNγ+TNF+CD8+ γδ T cells that are associated with either immunity to the liver-stage, or rapid elimination of blood-stage parasites.

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Section: Discussionmentioning

confidence: 82%

Immunological profiles associated with distinct parasitemic states in volunteers undergoing malaria challenge in Gabon

Manurung

Jong

Kruize

et al. 2022

Sci Rep

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“…While ongoing studies continue to establish a basis for new directions for malaria vaccine development, they are just the beginning. For example, a recent study assessed the global diversity and population structure of high priority P. falciparum vaccine candidate antigens [ 7 ]. This analysis included data from over 2600 parasite genomes from 15 malaria endemic countries and evaluated and compared the target haplotypes and 3-dimensional structures.…”

Section: Twenty-first Century—turning Point In Malaria Researchmentioning

confidence: 99%

“…Once molecular biological methods took hold in the 1970s, attempts to make a malaria vaccine became the envisioned panacea (reviewed in [ 4 ]). These efforts continue today, with the full recognition that making and introducing an effective malaria vaccine(s) is no small task, especially since the ultimate protection worldwide will require vaccines that have long-lasting immunity and are effective against multiple species of Plasmodium with their ever-changing genetic variation (reviewed in [ 5 – 7 ]). Many factors must be considered to ensure the effectiveness of vaccines in malaria endemic communities [ 8 ].…”

Section: Introductionmentioning

confidence: 99%

Systems biology of malaria explored with nonhuman primates

Galinski

2022

Malar J

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Abstract“The Primate Malarias” book has been a uniquely important resource for multiple generations of scientists, since its debut in 1971, and remains pertinent to the present day. Indeed, nonhuman primates (NHPs) have been instrumental for major breakthroughs in basic and pre-clinical research on malaria for over 50 years. Research involving NHPs have provided critical insights and data that have been essential for malaria research on many parasite species, drugs, vaccines, pathogenesis, and transmission, leading to improved clinical care and advancing research goals for malaria control, elimination, and eradication. Whilst most malaria scientists over the decades have been studying Plasmodium falciparum, with NHP infections, in clinical studies with humans, or using in vitro culture or rodent model systems, others have been dedicated to advancing research on Plasmodium vivax, as well as on phylogenetically related simian species, including Plasmodium cynomolgi, Plasmodium coatneyi, and Plasmodium knowlesi. In-depth study of these four phylogenetically related species over the years has spawned the design of NHP longitudinal infection strategies for gathering information about ongoing infections, which can be related to human infections. These Plasmodium-NHP infection model systems are reviewed here, with emphasis on modern systems biological approaches to studying longitudinal infections, pathogenesis, immunity, and vaccines. Recent discoveries capitalizing on NHP longitudinal infections include an advanced understanding of chronic infections, relapses, anaemia, and immune memory. With quickly emerging new technological advances, more in-depth research and mechanistic discoveries can be anticipated on these and additional critical topics, including hypnozoite biology, antigenic variation, gametocyte transmission, bone marrow dysfunction, and loss of uninfected RBCs. New strategies and insights published by the Malaria Host–Pathogen Interaction Center (MaHPIC) are recapped here along with a vision that stresses the importance of educating future experts well trained in utilizing NHP infection model systems for the pursuit of innovative, effective interventions against malaria.

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“…PfMSP1 has long been considered a vaccine target since antibody responses against this protein have been associated with protection ( 6 , 21 , 23 ), although results from PfMSP1-based vaccine trials have been disappointing ( 24 , 25 ). However, since PfMSP1 has high antigenic heterogeneity across Pf strains ( 26 , 27 ), it is a model antigen well-suited to assess antibody cross-strain reactivity elicited by natural infection. In addition, PfMSP1 is commonly used to study Plasmodium -specific MBCs in both humans ( 15 , 16 , 28 , 29 ) and mice ( 30 – 32 ), and this study therefore adds to a growing body of literature on PfMSP1-specific B cell responses.…”

Section: Introductionmentioning

confidence: 99%

A Molecular Analysis of Memory B Cell and Antibody Responses Against Plasmodium falciparum Merozoite Surface Protein 1 in Children and Adults From Uganda

et al. 2022

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Memory B cells (MBCs) and plasma antibodies against Plasmodium falciparum (Pf) merozoite antigens are important components of the protective immune response against malaria. To gain understanding of how responses against Pf develop in these two arms of the humoral immune system, we evaluated MBC and antibody responses against the most abundant merozoite antigen, full-length Pf merozoite surface protein 1 (PfMSP1FL), in individuals from a region in Uganda with high Pf transmission. Our results showed that PfMSP1FL-specific B cells in adults with immunological protection against malaria were predominantly IgG+ classical MBCs, while children with incomplete protection mainly harbored IgM+ PfMSP1FL-specific classical MBCs. In contrast, anti-PfMSP1FL plasma IgM reactivity was minimal in both children and adults. Instead, both groups showed high plasma IgG reactivity against PfMSP1FL, with broadening of the response against non-3D7 strains in adults. The B cell receptors encoded by PfMSP1FL-specific IgG+ MBCs carried high levels of amino acid substitutions and recognized relatively conserved epitopes on the highly variable PfMSP1 protein. Proteomics analysis of PfMSP119-specific IgG in plasma of an adult revealed a limited repertoire of anti-MSP1 antibodies, most of which were IgG1 or IgG3. Similar to B cell receptors of PfMSP1FL-specific MBCs, anti-PfMSP119 IgGs had high levels of amino acid substitutions and their sequences were predominantly found in classical MBCs, not atypical MBCs. Collectively, these results showed evolution of the PfMSP1-specific humoral immune response with cumulative Pf exposure, with a shift from IgM+ to IgG+ B cell memory, diversification of B cells from germline, and stronger recognition of PfMSP1 variants by the plasma IgG repertoire.

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Global diversity and balancing selection of 23 leading Plasmodium falciparum candidate vaccine antigens

Cited by 22 publications

References 110 publications

Immunological profiles associated with distinct parasitemic states in volunteers undergoing malaria challenge in Gabon

Immunological profiles associated with distinct parasitemic states in volunteers undergoing malaria challenge in Gabon

Systems biology of malaria explored with nonhuman primates

A Molecular Analysis of Memory B Cell and Antibody Responses Against Plasmodium falciparum Merozoite Surface Protein 1 in Children and Adults From Uganda

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