| Literature DB >> 23891618 |
Hongxing Wang1, Qigui Li2, Sean Reyes2, Jing Zhang2, Qiang Zeng2, Ping Zhang2, Lisa Xie2, Patricia J Lee2, Norma Roncal2, Victor Melendez2, Mark Hickman2, Michael P Kozar2.
Abstract
Decoquinate has potent activity against both Plasmodium hepatic development and red cell replication when tested in vitro. Decoquinate, however, is practically insoluble in water. To achieve its maximal in vivo efficacy, we generated nanoparticle formulations of decoquinate with a mean particle size less than 400 nm. Three separate preparations at doses of decoquinate 0.5-5 mg/kg were examined in mice infected with Plasmodium berghei. Oral administration of nanoparticle decoquinate at a dose of 1.25 mg/kg effectively inhibited the liver-stage parasite growth and provided complete causal prophylactic protection. This efficacy is 15 fold greater than that observed for microparticle decoquinate, which requires minimal dose of 20 mg/kg for the same inhibitory effect. Further in vitro studies utilizing dose-response assays revealed that decoquinate nanoformulation was substantially more potent than decoquinate microsuspension in killing both liver and blood stage malarial parasites, proving its potential for therapeutic development. FROM THE CLINICAL EDITOR: In this study, a nanoparticle formulation of decoquinate is shown to have superior bioavailability and efficacy in a mouse model of malaria, paving the way to the development of novel, potentially less toxic and more effective therapeutics to combat a disease that still has an enormous impact on a global scale despite the available partially effective therapies.Entities:
Keywords: Causal prophylaxis; Malarial life cycle; Parasite growth; Particle size; Real time imaging
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Year: 2013 PMID: 23891618 DOI: 10.1016/j.nano.2013.07.010
Source DB: PubMed Journal: Nanomedicine ISSN: 1549-9634 Impact factor: 5.307