Differences in PfEMP1s recognized by antibodies from patients with uncomplicated or severe malaria

Research output: Contribution to journalJournal articlepeer-review

  • Michael F Duffy
  • Rintis Noviyanti
  • Takafumi Tsuboi
  • Zhi-Ping Feng
  • Leily Trianty
  • Boni F Sebayang
  • Eizo Takashima
  • Fransisca Sumardy
  • Daniel A Lampah
  • Turner, Louise
  • Lavstsen, Thomas
  • Freya J I Fowkes
  • Peter Siba
  • Stephen J Rogerson
  • Theander, Thor Grundtvig
  • Jutta Marfurt
  • Ric N Price
  • Nicholas M Anstey
  • Graham V Brown
  • Anthony T Papenfuss

BACKGROUND: Plasmodium falciparum erythrocyte membrane protein 1 (PfEMP1) variants are encoded by var genes and mediate pathogenic cytoadhesion and antigenic variation in malaria. PfEMP1s can be broadly divided into three principal groups (A, B and C) and they contain conserved arrangements of functional domains called domain cassettes. Despite their tremendous diversity there is compelling evidence that a restricted subset of PfEMP1s is expressed in severe disease. In this study antibodies from patients with severe and uncomplicated malaria were compared for differences in reactivity with a range of PfEMP1s to determine whether antibodies to particular PfEMP1 domains were associated with severe or uncomplicated malaria.

METHODS: Parts of expressed var genes in a severe malaria patient were identified by RNAseq and several of these partial PfEMP1 domains were expressed together with others from laboratory isolates. Antibodies from Papuan patients to these parts of multiple PfEMP1 proteins were measured.

RESULTS: Patients with uncomplicated malaria were more likely to have antibodies that recognized PfEMP1 of Group C type and recognized a broader repertoire of group A and B PfEMP1s than patients with severe malaria.

CONCLUSION: These data suggest that exposure to a broad range of group A and B PfEMP1s is associated with protection from severe disease in Papua, Indonesia.

Original languageEnglish
Article number258
JournalMalaria Journal
Volume15
Number of pages12
ISSN1475-2875
DOIs
Publication statusPublished - 2016

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