Plasmepsin inhibitory activity and structure-guided optimization of a potent hydroxyethylamine-based antimalarial hit

Kristaps Jaudzems; Kaspars Tars; Gundars Maurops; Natalija Ivdra; Martins Otikovs; Janis Leitans; Iveta Kanepe-Lapsa; Ilona Domraceva; Ilze Mutule; Peteris Trapencieris; Michael J Blackman; Aigars Jirgensons

doi:10.1021/ml4004952

Plasmepsin inhibitory activity and structure-guided optimization of a potent hydroxyethylamine-based antimalarial hit

ACS Med Chem Lett. 2014 Jan 13;5(4):373-7. doi: 10.1021/ml4004952. eCollection 2014 Apr 10.

Affiliations

¹ Latvian Institute of Organic Synthesis , Aizkraukles 21, Riga LV-1006, Latvia.
² Biomedical Research and Study Centre , Ratsupites 1, Riga LV-1067, Latvia.
³ Division of Parasitology, MRC National Institute for Medical Research , The Ridgeway, Mill, Hill, London NW7 1AA, U.K.

Abstract

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.

Keywords: Cathepsin D; Malaria; Plasmodium falciparum; hydroxyethylamine; inhibition; plasmepsins; structure-guided optimization.

Grants and funding

MC_U117532063/MRC_/Medical Research Council/United Kingdom