| dc.contributor.author |
Early AM, Lievens M, MacInnis BL, Ockenhouse CF, Volkman SK, Adjei S, Agbenyega T, Ansong D, Gondi S, Greenwood B, Hamel M, Odero C, Otieno K, Otieno W, Owusu-Agyei S, Asante KP, Sorgho H, Tina L, Tinto H, Valea I, Wirth DF, Neafsey DE. |
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| dc.description.abstract |
Host immunity exerts strong selective pressure on pathogens. Population-level genetic
analysis can identify signatures of this selection, but these signatures reflect the net
selective effect of all hosts and vectors in a population. In contrast, analysis of pathogen
diversity within hosts provides information on individual, host-specific selection
pressures. Here, we combine these complementary approaches in an analysis of the
malaria parasite Plasmodium falciparum using haplotype sequences from thousands of
natural infections in sub-Saharan Africa. We find that parasite genotypes show
preferential clustering within multi-strain infections in young children, and identify
individual amino acid positions that may contribute to strain-specific immunity. Our
results demonstrate that natural host defenses to P. falciparum act in an allele-specific
manner to block specific parasite haplotypes from establishing blood-stage infections.
This selection partially explains the extreme amino acid diversity of many parasite
antigens and suggests that vaccines targeting such proteins should account for allelespecific immunity. |
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