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Identification of a new chemical class of antimalarials
Authors:Brunner Ralf  Aissaoui Hamed  Boss Christoph  Bozdech Zbynek  Brun Reto  Corminboeuf Olivier  Delahaye Stephane  Fischli Christoph  Heidmann Bibia  Kaiser Marcel  Kamber Jolanda  Meyer Solange  Papastogiannidis Petros  Siegrist Romain  Voss Till  Welford Richard  Wittlin Sergio  Binkert Christoph
Affiliation:Medical Parasitology and Infection Biology, Swiss Tropical and Public Health Institute, Basel CH-4002.
Abstract:The increasing spread of drug-resistant malaria strains underscores the need for new antimalarial agents with novel modes of action (MOAs). Here, we describe a compound representative of a new class of antimalarials. This molecule, ACT-213615, potently inhibits in vitro erythrocytic growth of all tested Plasmodium falciparum strains, irrespective of their drug resistance properties, with half-maximal inhibitory concentration (IC(50)) values in the low single-digit nanomolar range. Like the clinically used artemisinins, the compound equally and very rapidly affects all 3 asexual erythrocytic parasite stages. In contrast, microarray studies suggest that the MOA of ACT-213615 is different from that of the artemisinins and other known antimalarials. ACT-213615 is orally bioavailable in mice, exhibits activity in the murine Plasmodium berghei model and efficacy comparable to that of the reference drug chloroquine in the recently established P. falciparum SCID mouse model. ACT-213615 represents a new class of potent antimalarials that merits further investigation for its clinical potential.
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