4.8 Article

Mapping immune variation and var gene switching in naive hosts infected with Plasmodium falciparum

Journal

ELIFE
Volume 10, Issue -, Pages -

Publisher

ELIFE SCIENCES PUBLICATIONS LTD
DOI: 10.7554/eLife.62800

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Funding

  1. Medical Research Council [G40270, MR/M003906/1]
  2. Wellcome Trust [WT206194, 203783/Z/16/Z, 104111/Z/14/Z, 106917/Z/15/Z, WT084226, 107668/Z/15/Z]
  3. MRC [MR/M003906/1] Funding Source: UKRI
  4. Wellcome Trust [203783/Z/16/Z, 107668/Z/15/Z] Funding Source: Wellcome Trust

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This study found that falciparum malaria displays clinical heterogeneity, with some volunteers triggering inflammatory responses and experiencing hallmark symptoms of malaria. The research also showed that there was no evidence of rapid expansion of parasite variants associated with severe disease in naive hosts, suggesting that the dominant parasite variants in severe malaria do not have an intrinsic growth advantage.
Falciparum malaria is clinically heterogeneous and the relative contribution of parasite and host in shaping disease severity remains unclear. We explored the interaction between inflammation and parasite variant surface antigen (VSA) expression, asking whether this relationship underpins the variation observed in controlled human malaria infection (CHMI). We uncovered marked heterogeneity in the host response to blood challenge; some volunteers remained quiescent, others triggered interferon-stimulated inflammation and some showed transcriptional evidence of myeloid cell suppression. Significantly, only inflammatory volunteers experienced hallmark symptoms of malaria. When we tracked temporal changes in parasite VSA expression to ask whether variants associated with severe disease rapidly expand in naive hosts, we found no transcriptional evidence to support this hypothesis. These data indicate that parasite variants that dominate severe malaria do not have an intrinsic growth or survival advantage; instead, they presumably rely upon infection-induced changes in their within-host environment for selection.

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