In search of antiparasitic agents, we here identify arylmethylamino steroids as potent compounds and characterize more than 60 derivatives. The lead compound 1o is fast acting and highly active against intraerythrocytic stages of chloroquine-sensitive and resistant Plasmodium falciparum parasites (IC50 1–5 nM) as well as against gametocytes. In P. berghei-infected mice, oral administration of 1o drastically reduces parasitaemia and cures the animals. Furthermore, 1o efficiently blocks parasite transmission from mice to mosquitoes. The steroid compounds show low cytotoxicity in mammalian cells and do not induce acute toxicity symptoms in mice. Moreover, 1o has a remarkable activity against the blood-feeding trematode parasite Schistosoma mansoni. The steroid and the hydroxyarylmethylamino moieties are essential for antimalarial activity supporting a chelate-based quinone methide mechanism involving metal or haem bioactivation. This study identifies chemical scaffolds that are rapidly internalized into blood-feeding parasites. Steroid units can facilitate membrane permeation and bioavailability in drugs. Here, using a medicinal chemistry program, Krieget al. identify an arylmethylamino steroid that kills Plasmodium parasites, likely through a chelate-based quinone methide mechanism, and has activity against Schistosoma mansoni.
Arylmethylamino steroids as antiparasitic agents
R. Krieg,E. Jortzik,Alice-Anne Goetz,S. Blandin,S. Wittlin,M. Elhabiri,Mahsa Rahbari,Selbi Nuryyeva,K. Voigt,H. Dahse,A. Brakhage,Svenja Beckmann,T. Quack,C. Grevelding,A. Pinkerton,B. Schönecker,J. Burrows,E. Davioud‐Charvet,S. Rahlfs,K. Becker
Published 2017 in Nature Communications
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- Publication year
2017
- Venue
Nature Communications
- Publication date
2017-02-17
- Fields of study
Biology, Medicine, Chemistry
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Semantic Scholar, PubMed
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