Identification and Optimization of an Aminoalcohol-Carbazole Series with Antimalarial Properties

Jérôme Molette,Julie Routier,Nada Abla,Dominique Besson,Agnes Bombrun,Reto Brun,Howard Burt,Katrin Georgi,Marcel Kaiser,Solomon Nwaka,Mathilde Muzerelle,Alexander Scheer

Identification and Optimization of an Aminoalcohol-Carbazole Series with Antimalarial Properties

2013

Jérôme Molette
Julie Routier
Nada Abla
Dominique Besson
Agnes Bombrun
Reto Brun
Howard Burt
Katrin Georgi
Marcel Kaiser
Solomon Nwaka
Mathilde Muzerelle
Alexander Scheer

Recent observations on the emergence of artemisinin resistant parasites have highlighted the need for new antimalarial treatments. An HTS campaign led to the identification of the 1-(1-aminopropan-2-ol)carbazole analogues as potent hits against Plasmodium falciparum K1 strain. The SAR study and optimization of early ADME and physicochemical properties direct us to the selection of a late lead compound that shows good efficacy when orally administrated in the in vivo P. berghei mouse model.

Keywords:

Biology
Pharmacology
Lead compound
Carbazole
In vivo
Plasmodium berghei
Plasmodium falciparum
ADME
Artemisinin

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