Histone methyltransferase inhibitors are orally bioavailable, fast-acting molecules with activity against different species causing malaria in humans
Date Issued
2015-01-01
Author(s)
Malmquist, Nicholas A
Sundriyal, Sandeep
Caron, Joachim
Chen, Patty
Witkowski, Benoit
Menard, Didier
Suwanarusk, Rossarin
Renia, Laurent
Nosten, Francois
Jiménez-Díaz, María Belén
Angulo-Barturen, Iñigo
Santos Martínez, María
Ferrer, Santiago
Sanz, Laura M
Gamo, Francisco-Javier
Duffy, Sandra
Avery, Vicky M
Ruecker, Andrea
Delves, Michael J
Sinden, Robert E
Fuchter, Matthew J
Scherf, Artur
DOI
10.1128/aac.04419-14
Abstract
Current antimalarials are under continuous threat due to the relentless development of drug resistance by malaria parasites. We previously reported promising in vitro parasite-killing activity with the histone methyltransferase inhibitor BIX-01294 and its analogue TM2-115. Here, we further characterize these diaminoquinazolines for in vitro and in vivo efficacy and pharmacokinetic properties to prioritize and direct compound development. BIX-01294 and TM2-115 displayed potent in vitro activity, with 50% inhibitory concentrations (IC50s) of <50 nM against drug-sensitive laboratory strains and multidrug-resistant field isolates, including artemisinin-refractory Plasmodium falciparum isolates. Activities against ex vivo clinical isolates of both P. falciparum and Plasmodium vivax were similar, with potencies of 300 to 400 nM. Sexual-stage gametocyte inhibition occurs at micromolar levels; however, mature gametocyte progression to gamete formation is inhibited at submicromolar concentrations. Parasite reduction ratio analysis confirms a high asexual-stage rate of killing. Both compounds examined displayed oral efficacy in in vivo mouse models of Plasmodium berghei and P. falciparum infection. The discovery of a rapid and broadly acting antimalarial compound class targeting blood stage infection, including transmission stage parasites, and effective against multiple malaria-causing species reveals the diaminoquinazoline scaffold to be a very promising lead for development into greatly needed novel therapies to control malaria.