The anti-trypanosome drug fexinidazole shows potential for treating visceral leishmaniasis

Susan Wyllie; Stephen Patterson; Laste Stojanovski; Frederick R C Simeons; Suzanne Norval; Robert Kime; Kevin D Read; Alan H Fairlamb

doi:10.1126/scitranslmed.3003326

The anti-trypanosome drug fexinidazole shows potential for treating visceral leishmaniasis

Sci Transl Med. 2012 Feb 1;4(119):119re1. doi: 10.1126/scitranslmed.3003326.

Authors

Susan Wyllie¹, Stephen Patterson, Laste Stojanovski, Frederick R C Simeons, Suzanne Norval, Robert Kime, Kevin D Read, Alan H Fairlamb

Affiliation

¹ Division of Biological Chemistry and Drug Discovery, Wellcome Trust Biocentre, College of Life Sciences, University of Dundee, Dundee, Scotland, UK.

Abstract

Safer and more effective oral drugs are required to treat visceral leishmaniasis, a parasitic disease that kills 50,000 to 60,000 people each year in parts of Asia, Africa, and Latin America. Here, we report that fexinidazole, a drug currently in phase 1 clinical trials for treating African trypanosomiasis, shows promise for treating visceral leishmaniasis. This 2-substituted 5-nitroimidazole drug is rapidly oxidized in vivo in mice, dogs, and humans to sulfoxide and sulfone metabolites. Both metabolites of fexinidazole were active against Leishmania donovani amastigotes grown in macrophages, whereas the parent compound was inactive. Pharmacokinetic studies with fexinidazole (200 mg/kg) showed that fexinidazole sulfone achieves blood concentrations in mice above the EC(99) (effective concentration inhibiting growth by 99%) value for at least 24 hours after a single oral dose. A once-daily regimen for 5 days at this dose resulted in a 98.4% suppression of infection in a mouse model of visceral leishmaniasis, equivalent to that seen with the drugs miltefosine and Pentostam, which are currently used clinically to treat this tropical disease. In African trypanosomes, the mode of action of nitro drugs involves reductive activation via a NADH (reduced form of nicotinamide adenine dinucleotide)-dependent bacterial-like nitroreductase. Overexpression of the leishmanial homolog of this nitroreductase in L. donovani increased sensitivity to fexinidazole by 19-fold, indicating that a similar mechanism is involved in both parasites. These findings illustrate the potential of fexinidazole as an oral drug therapy for treating visceral leishmaniasis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Administration, Oral
Animals
Biotransformation
Cells, Cultured
Disease Models, Animal
Dose-Response Relationship, Drug
Drug Administration Schedule
Female
Leishmania donovani / drug effects*
Leishmania donovani / enzymology
Leishmania donovani / genetics
Leishmania donovani / growth & development
Leishmaniasis, Visceral / parasitology
Leishmaniasis, Visceral / prevention & control*
Macrophages, Peritoneal / drug effects
Macrophages, Peritoneal / parasitology
Mice
Mice, Inbred BALB C
Nitroimidazoles / administration & dosage
Nitroimidazoles / pharmacokinetics
Nitroimidazoles / pharmacology*
Nitroreductases / antagonists & inhibitors
Nitroreductases / genetics
Nitroreductases / metabolism
Parasitic Sensitivity Tests
Protozoan Proteins / antagonists & inhibitors
Protozoan Proteins / genetics
Protozoan Proteins / metabolism
Sulfones / pharmacology
Sulfoxides / pharmacology
Trypanocidal Agents / administration & dosage
Trypanocidal Agents / pharmacokinetics
Trypanocidal Agents / pharmacology*

Substances

Nitroimidazoles
Protozoan Proteins
Sulfones
Sulfoxides
Trypanocidal Agents
fexinidazole
Nitroreductases

Abstract

Publication types

MeSH terms

Substances

Grants and funding