Genes (Jun 2019)

Identification of <i>Plasmodium falciparum</i> Mitochondrial Malate: Quinone Oxidoreductase Inhibitors from the Pathogen Box

  • Xinying Wang,
  • Yukiko Miyazaki,
  • Daniel Ken Inaoka,
  • Endah Dwi Hartuti,
  • Yoh-Ichi Watanabe,
  • Tomoo Shiba,
  • Shigeharu Harada,
  • Hiroyuki Saimoto,
  • Jeremy Nicholas Burrows,
  • Francisco Javier Gamo Benito,
  • Tomoyoshi Nozaki,
  • Kiyoshi Kita

DOI
https://doi.org/10.3390/genes10060471
Journal volume & issue
Vol. 10, no. 6
p. 471

Abstract

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Malaria is one of the three major global health threats. Drug development for malaria, especially for its most dangerous form caused by Plasmodium falciparum, remains an urgent task due to the emerging drug-resistant parasites. Exploration of novel antimalarial drug targets identified a trifunctional enzyme, malate quinone oxidoreductase (MQO), located in the mitochondrial inner membrane of P. falciparum (PfMQO). PfMQO is involved in the pathways of mitochondrial electron transport chain, tricarboxylic acid cycle, and fumarate cycle. Recent studies have shown that MQO is essential for P. falciparum survival in asexual stage and for the development of experiment cerebral malaria in the murine parasite P. berghei, providing genetic validation of MQO as a drug target. However, chemical validation of MQO, as a target, remains unexplored. In this study, we used active recombinant protein rPfMQO overexpressed in bacterial membrane fractions to screen a total of 400 compounds from the Pathogen Box, released by Medicines for Malaria Venture. The screening identified seven hit compounds targeting rPfMQO with an IC50 of under 5 μM. We tested the activity of hit compounds against the growth of 3D7 wildtype strain of P. falciparum, among which four compounds showed an IC50 from low to sub-micromolar concentrations, suggesting that PfMQO is indeed a potential antimalarial drug target.

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