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Abstract

A large body of evidence suggests that low parasite carriage in Plasmodium falciparum asymptomatic infection is required for the maintenance of malaria immunity. However, the fact that treating such infections has little to no impact on subsequent clinical malaria is rarely noted. In this paper, we review data and argue that low-density parasite carriage in asymptomatic infection may not support host immune processes and that parasites are virtually under the host's immunological radar. We also discuss factors that may be constraining parasitemia in asymptomatic infections from reaching the threshold required to cause clinical symptoms. A thorough understanding of this infectious reservoir is essential for malaria control and eradication because asymptomatic infections contribute significantly to Plasmodium transmission.

Lay Summary

  1. Persistent asymptomatic Plasmodium falciparum parasite carriage has been recognized as one of the major contributors to malaria transmission that impedes worldwide elimination efforts.

  2. Asymptomatic infection is required for maintaining clinical immunity, hence the controversy regarding its treatment.

  3. Evidence from transcriptional and cellular profiling indicates asymptomatic low parasite carriage may not support host immune processes.

  4. Interventions targeted at persistent asymptomatic infections may be crucial for malaria control.

Plasmodium falciparum, asymptomatic infection, transcriptomics, immunological radar, splenic clearance
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