4.8 Article

Declines in prevalence alter the optimal level of sexual investment for the malaria parasite Plasmodium falciparum

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.2122165119

Keywords

malaria; sexual commitment; adaptation; modeling; genomics

Funding

  1. National Institute of Allergy and Infectious Diseases, NIH, Department of Health and Human Services [U19AI110818]
  2. Investissement d'Avenir grant [ANR-10-LABX-25-01]
  3. Sante publique France as National Reference Centre for Malaria
  4. French Ministry for Research
  5. Maximizing Investigators' Research Award for Early-Stage Investigators [R35 GM-124715]
  6. European Commission [REGPOT-CT-2011-285837-430 STRonGer]
  7. NSF [1902214]

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This study investigates the impact of declining infection rates on the investment of Plasmodium falciparum in sexual and asexual growth. Using a mathematical model and analyzing parasite genomes collected over an 18-year period, the study confirms the model's predictions and highlights the wide-ranging selection pressures imposed by public health interventions on basic parasite life history traits.
Successful infectious disease interventions can result in large reductions in parasite prevalence. Such demographic change has fitness implications for individual parasites and may shift the parasite's optimal life history strategy. Here, we explore whether declining infection rates can alter Plasmodium falciparum's investment in sexual versus asexual growth. Using a multiscale mathematical model, we demonstrate how the proportion of polyclonal infections, which decreases as parasite prevalence declines, affects the optimal sexual development strategy: Within-host competition in multiclone infections favors a greater investment in asexual growth whereas single-clone infections benefit from higher conversion to sexual forms. At the same time, drug treatment also imposes selection pressure on sexual development by shortening infection length and reducing within-host competition. We assess these models using 148 P. falciparum parasite genomes sampled in French Guiana over an 18-y period of intensive intervention (1998 to 2015). During this time frame, multiple public health measures, including the introduction of new drugs and expanded rapid diagnostic testing, were implemented, reducing P. falciparum malaria cases by an order ofmagnitude. Consistent with this prevalence decline, we see an increase in the relatedness among parasites, but no single clonal background grew to dominate the population. Analyzing individual allele frequency trajectories, we identify genes that likely experienced selective sweeps. Supporting our model predictions, genes showing the strongest signatures of selection include transcription factors involved in the development of P. falciparum's sexual gametocyte form. These results highlight how public health interventions impose wideranging selection pressures that affect basic parasite life history traits.

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