Novel diaryl ureas with efficacy in a mouse model of malaria.

John W. Anderson,Dimitri Sarantakis,Jacek Terpinski,T. R. Santha Kumar,Han Chun Tsai,Mack Kuo,Arba L. Ager,William R. Jacobs,Guy Alan Schiehser,Sean Ekins,James C. Sacchettini,David P. Jacobus,David A. Fidock,Joel S. Freundlich

Novel diaryl ureas with efficacy in a mouse model of malaria.

2013

John W. Anderson
Dimitri Sarantakis
Jacek Terpinski
T. R. Santha Kumar
Han Chun Tsai
Mack Kuo
Arba L. Ager
William R. Jacobs
Guy Alan Schiehser
Sean Ekins
James C. Sacchettini
David P. Jacobus
David A. Fidock
Joel S. Freundlich

Abstract Exploration of triclosan analogs has led to novel diaryl ureas with significant potency against in vitro cultures of drug-resistant and drug-sensitive strains of the human malaria parasite Plasmodium falciparum . Compound 18 demonstrated EC 50 values of 37 and 55 nM versus in vitro cultured parasite strains and promising in vivo efficacy in a Plasmodium berghei antimalarial mouse model, with >50% survival at day 31 post-treatment when administered subcutaneously at 256 mg/kg. This series of compounds provides a chemical scaffold of novel architecture, as validated by cheminformatics analysis, to pursue antimalarial drug discovery efforts.

Keywords:

Plasmodium falciparum
Plasmodium berghei
Potency
In vivo
Drug discovery
Triclosan
Malaria
Pharmacology
Biology
In vitro

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