| Literature DB >> 25918204 |
Allison M Stickles1, Li-Min Ting1, Joanne M Morrisey1, Yuexin Li1, Michael W Mather1, Erin Meermeier1, April M Pershing1, Isaac P Forquer1, Galen P Miley1, Sovitj Pou1, Rolf W Winter1, David J Hinrichs1, Jane X Kelly1, Kami Kim1, Akhil B Vaidya1, Michael K Riscoe2, Aaron Nilsen2.
Abstract
Single-dose therapies for malaria have been proposed as a way to reduce the cost and increase the effectiveness of antimalarial treatment. However, no compound to date has shown single-dose activity against both the blood-stage Plasmodium parasites that cause disease and the liver-stage parasites that initiate malaria infection. Here, we describe a subset of cytochrome bc1 (cyt bc1) inhibitors, including the novel 4(1H)-quinolone ELQ-400, with single-dose activity against liver, blood, and transmission-stage parasites in mouse models of malaria. Although cyt bc1 inhibitors are generally classified as slow-onset antimalarials, we found that a single dose of ELQ-400 rapidly induced stasis in blood-stage parasites, which was associated with a rapid reduction in parasitemia in vivo. ELQ-400 also exhibited a low propensity for drug resistance and was active against atovaquone-resistant P. falciparum strains with point mutations in cyt bc1. Ultimately, ELQ-400 shows that cyt bc1 inhibitors can function as single-dose, blood-stage antimalarials and is the first compound to provide combined treatment, prophylaxis, and transmission blocking activity for malaria after a single oral administration. This remarkable multi-stage efficacy suggests that metabolic therapies, including cyt bc1 inhibitors, may be valuable additions to the collection of single-dose antimalarials in current development. © The American Society of Tropical Medicine and Hygiene.Entities:
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Year: 2015 PMID: 25918204 PMCID: PMC4458825 DOI: 10.4269/ajtmh.14-0553
Source DB: PubMed Journal: Am J Trop Med Hyg ISSN: 0002-9637 Impact factor: 2.345