eLife (May 2019)

The Plasmodium liver-specific protein 2 (LISP2) is an early marker of liver stage development

  • Devendra Kumar Gupta,
  • Laurent Dembele,
  • Annemarie Voorberg-van der Wel,
  • Guglielmo Roma,
  • Andy Yip,
  • Vorada Chuenchob,
  • Niwat Kangwanrangsan,
  • Tomoko Ishino,
  • Ashley M Vaughan,
  • Stefan H Kappe,
  • Erika L Flannery,
  • Jetsumon Sattabongkot,
  • Sebastian Mikolajczak,
  • Pablo Bifani,
  • Clemens HM Kocken,
  • Thierry Tidiane Diagana

DOI
https://doi.org/10.7554/eLife.43362
Journal volume & issue
Vol. 8

Abstract

Read online

Plasmodium vivax hypnozoites persist in the liver, cause malaria relapse and represent a major challenge to malaria elimination. Our previous transcriptomic study provided a novel molecular framework to enhance our understanding of the hypnozoite biology (Voorberg-van der Wel A, et al., 2017). In this dataset, we identified and characterized the Liver-Specific Protein 2 (LISP2) protein as an early molecular marker of liver stage development. Immunofluorescence analysis of hepatocytes infected with relapsing malaria parasites, in vitro (P. cynomolgi) and in vivo (P. vivax), reveals that LISP2 expression discriminates between dormant hypnozoites and early developing parasites. We further demonstrate that prophylactic drugs selectively kill all LISP2-positive parasites, while LISP2-negative hypnozoites are only sensitive to anti-relapse drug tafenoquine. Our results provide novel biological insights in the initiation of liver stage schizogony and an early marker suitable for the development of drug discovery assays predictive of anti-relapse activity.

Keywords