In vitro and in vivo anti-malarial activity of novel harmine-analog heat shock protein 90 inhibitors: a possible partner for artemisinin

Malar J. 2016 Dec 1;15(1):579. doi: 10.1186/s12936-016-1625-7.

Abstract

Background: The emergence of artemisinin-resistant Plasmodium falciparum strains poses a serious challenge to the control of malaria. This necessitates the development of new anti-malarial drugs. Previous studies have shown that the natural beta-carboline alkaloid harmine is a promising anti-malarial agent targeting the P. falciparum heat-shock protein 90 (PfHsp90). The aim of this study was to test the anti-malarial activity of harmine analogues.

Methods: Forty-two harmine analogues were synthesized and the binding of these analogues to P. falciparum heat shock protein 90 was investigated. The in vitro anti-malarial activity of two of the analogues, 17A and 21A, was evaluated using a 72-h growth inhibition assay. The in vivo anti-malarial activity was tested in Plasmodium berghei infection of BALB/c mice. The potential of 21A for a combination treatment with artemisinin was evaluated using in vivo combination study with dihydro-artemisinin in BALB/c mice. Cytotoxicity of the harmine analogues was tested in vitro using HepG2 and HeLa cell lines.

Results: 17A and 21A bound to PfHsp90 with average IC50 values of 12.2 ± 2.3 and 23.1 ± 8.8 µM, respectively. They also inhibited the P. falciparum W2 strain with average IC50 values of 4.2 ± 1.3 and 5.7 ± 1.7 µM, respectively. In vivo, three daily injections of P. berghei-infected BALB/c mice with 100 mg/kg of either 17A or 21A showed significant reduction in parasitaemia with a 51.5 and 56.1% reduction, respectively. Mice treated with 17A and 21A showed a median survival time of 11 and 14 days, respectively, while the vehicle control mice survived a median of only 8.5 days. A dose-ranging experiment with 21A showed that the compound has a dose-dependent anti-malarial effect. Furthermore, treatment of infected mice with a combination of 21A and dihydroartemisinin (DHA) showed a dramatic reduction in parasitaemia compared to treatment with DHA alone.

Conclusion: A novel and non-toxic harmine analogue has been synthesized which binds to PfHsp90 protein, inhibits P. falciparum in vitro at micromolar concentration, reduces parasitaemia and prolongs survival of P. berghei-infected mice with an additive anti-malarial effect when combined with DHA.

Keywords: Anti-malarial drugs; Heat-shock protein 90; Malaria; Plasmodium falciparum.

MeSH terms

  • Animals
  • Antimalarials / administration & dosage
  • Antimalarials / chemical synthesis
  • Antimalarials / chemistry
  • Antimalarials / pharmacology*
  • Artemisinins / administration & dosage
  • Artemisinins / pharmacology*
  • Cell Line
  • Cell Survival / drug effects
  • Disease Models, Animal
  • Drug Synergism*
  • Female
  • HSP90 Heat-Shock Proteins / antagonists & inhibitors*
  • Harmine / administration & dosage
  • Harmine / chemical synthesis
  • Harmine / chemistry
  • Harmine / pharmacology*
  • Humans
  • Inhibitory Concentration 50
  • Malaria / drug therapy
  • Mice, Inbred BALB C
  • Plasmodium berghei / drug effects*
  • Plasmodium falciparum / drug effects*
  • Plasmodium falciparum / growth & development
  • Protein Binding
  • Protozoan Proteins / antagonists & inhibitors
  • Treatment Outcome

Substances

  • Antimalarials
  • Artemisinins
  • HSP90 Heat-Shock Proteins
  • Protozoan Proteins
  • Harmine
  • artemisinin