Plasmepsin Inhibitory Activity and Structure-Guided Optimization of a Potent Hydroxyethylamine-Based Antimalarial Hit

Plasmepsin Inhibitory Activity and Structure-Guided Optimization of a Potent Hydroxyethylamine-Based Antimalarial Hit

Antimalarial hit 1 SR (TCMDC-134674) identified in a GlaxoSmithKline cell based screening campaign was evaluated for inhibitory activity against the digestive vacuole plasmepsins (Plm I, II, and IV). It was found to be a potent Plm IV inhibitor with no selectivity over Cathepsin D. A cocrystal struc...

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Veröffentlicht in:ACS medicinal chemistry letters 2014-04, Vol.5 (4), p.373-377
Hauptverfasser: Jaudzems, Kristaps, Tars, Kaspars, Maurops, Gundars, Ivdra, Natalija, Otikovs, Martins, Leitans, Janis, Kanepe-Lapsa, Iveta, Domraceva, Ilona, Mutule, Ilze, Trapencieris, Peteris, Blackman, Michael J, Jirgensons, Aigars
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Sprache:eng
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Letter
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Zusammenfassung:Antimalarial hit 1 SR (TCMDC-134674) identified in a GlaxoSmithKline cell based screening campaign was evaluated for inhibitory activity against the digestive vacuole plasmepsins (Plm I, II, and IV). It was found to be a potent Plm IV inhibitor with no selectivity over Cathepsin D. A cocrystal structure of 1 SR bound to Plm II was solved, providing structural insight for the design of more potent and selective analogues. Structure-guided optimization led to the identification of structurally simplified analogues 17 and 18 as low nanomolar inhibitors of both, plasmepsin Plm IV activity and P. falciparum growth in erythrocytes.
ISSN:1948-5875
1948-5875
DOI:10.1021/ml4004952