Biomarker of Anopheles exposure in Ghanaian children with hemoglobin S and C
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Acta Tropica
Abstract
Heterozygous carriers of hemoglobin S and C (HbAS and HbAC) have a reduced risk of severe malaria but are not
protected from Plasmodium falciparum infection, suggesting that the protection involves acquired immunity.
During a blood meal, female Anopheles mosquitoes inject saliva that can elicit a host antibody response, which
can serve as a proxy for exposure to Plasmodium infection. Previous studies have shown that the peptide gSG6-P1
of An. gambiae saliva is antigenic and highly Anopheles specific. Here, we used plasma samples from 201 Gha naian children with wild-type hemoglobin (HbAA), HbAS, and HbAC to evaluate antibody levels against gSG6-P1
as a serological biomarker of Anopheles exposure and, therefore of P. falciparum infection risk. Malaria antigen
(PfCSP, GLURP, Pfs230, and HB3VAR06)-specific IgG levels, demographic data, and data regarding P. falciparum
infection and malaria control practices were also analyzed. Children with active P. falciparum infection had
higher antibody levels against all antigens, and those with HbAS and HbAC had significantly higher antibody
levels against Pfs230. Pfs230-specific IgG correlated negatively with gSG6-P1-specific IgG in children with HbAC.
Our results highlight the importance of studying the role of hemoglobinopathies in malaria transmission to
improve control interventions.
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Research Article