Meta-Analysis of Human Antibodies Against Plasmodium falciparum Variable Surface and Merozoite Stage Antigens

Eizo Takashima; Bernard N Kanoi; Hikaru Nagaoka; Masayuki Morita; Ifra Hassan; Nirianne M Q Palacpac; Thomas G Egwang; Toshihiro Horii; Jesse Gitaka; Takafumi Tsuboi

doi:10.3389/fimmu.2022.887219

Meta-Analysis of Human Antibodies Against Plasmodium falciparum Variable Surface and Merozoite Stage Antigens

Front Immunol. 2022 Jun 9:13:887219. doi: 10.3389/fimmu.2022.887219. eCollection 2022.

Affiliations

¹ Division of Malaria Research, Proteo-Science Center, Ehime University, Matsuyama, Japan.
² Centre for Research in Infectious Diseases, Directorate of Research and Innovation, Mount Kenya University, Thika, Kenya.
³ Department of Malaria Vaccine Development, Research Institute for Microbial Diseases, Osaka University, Suita, Japan.
⁴ Med Biotech Laboratories, Kampala, Uganda.
⁵ Division of Cell-Free Sciences, Proteo-Science Center, Ehime University, Matsuyama, Japan.

Abstract

Concerted efforts to fight malaria have caused significant reductions in global malaria cases and mortality. Sustaining this will be critical to avoid rebound and outbreaks of seasonal malaria. Identifying predictive attributes that define clinical malaria will be key to guide development of second-generation tools to fight malaria. Broadly reactive antibodies against variable surface antigens that are expressed on the surface of infected erythrocytes and merozoites stage antigens are targets of naturally acquired immunity and prime candidates for anti-malaria therapeutics and vaccines. However, predicting the relationship between the antigen-specific antibodies and protection from clinical malaria remains unresolved. Here, we used new datasets and multiple approaches combined with re-analysis of our previous data to assess the multi-dimensional and complex relationship between antibody responses and clinical malaria outcomes. We observed 22 antigens (17 PfEMP1 domains, 3 RIFIN family members, merozoite surface protein 3 (PF3D7_1035400), and merozoites-associated armadillo repeats protein (PF3D7_1035900) that were selected across three different clinical malaria definitions (1,000/2,500/5,000 parasites/µl plus fever). In addition, Principal Components Analysis (PCA) indicated that the first three components (Dim1, Dim2 and Dim3 with eigenvalues of 306, 48, and 29, respectively) accounted for 66.1% of the total variations seen. Specifically, the Dim1, Dim2 and Dim3 explained 52.8%, 8.2% and 5% of variability, respectively. We further observed a significant relationship between the first component scores and age with antibodies to PfEMP1 domains being the key contributing variables. This is consistent with a recent proposal suggesting that there is an ordered acquisition of antibodies targeting PfEMP1 proteins. Thus, although limited, and further work on the significance of the selected antigens will be required, these approaches may provide insights for identification of drivers of naturally acquired protective immunity as well as guide development of additional tools for malaria elimination and eradication.

Keywords: PCA; PfEMP1; Plasmodium falciparum; RIFIN; malaria immunity; variable surface antigens.

Publication types

Meta-Analysis
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Antibodies / metabolism
Humans
Malaria*
Malaria, Falciparum*
Merozoites
Plasmodium falciparum
Protozoan Proteins

Substances

Antibodies
Protozoan Proteins