Selection of a trioxaquine as an antimalarial drug candidate |
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| Authors: | Coslédan Frédéric Fraisse Laurent Pellet Alain Guillou François Mordmüller Benjamin Kremsner Peter G Moreno Alicia Mazier Dominique Maffrand Jean-Pierre Meunier Bernard |
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| Affiliation: | Frédéric Coslédan, Laurent Fraisse, Alain Pellet, François Guillou, Benjamin Mordmüller, Peter G. Kremsner, Alicia Moreno, Dominique Mazier, Jean-Pierre Maffrand, and Bernard Meunier |
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| Abstract: | Trioxaquines are antimalarial agents based on hybrid structures with a dual mode of action. One of these molecules, PA1103/SAR116242, is highly active in vitro on several sensitive and resistant strains of Plasmodium falciparum at nanomolar concentrations (e.g., IC50 value = 10 nM with FcM29, a chloroquine-resistant strain) and also on multidrug-resistant strains obtained from fresh patient isolates in Gabon. This molecule is very efficient by oral route with a complete cure of mice infected with chloroquine-sensitive or chloroquine-resistant strains of Plasmodia at 26–32 mg/kg. This compound is also highly effective in humanized mice infected with P. falciparum. Combined with a good drug profile (preliminary absorption, metabolism, and safety parameters), these data were favorable for the selection of this particular trioxaquine for development as drug candidate among 120 other active hybrid molecules. |
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| Keywords: | curative drug malaria Plasmodium heme alkglation |
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