A high throughput screen for next-generation leads targeting malaria parasite transmission.

Michael J Delves ORCID logo; Celia Miguel-Blanco; Holly Matthews; Irene Molina; Andrea Ruecker ORCID logo; Sabrina Yahiya; Ursula Straschil; Matthew Abraham; María Luisa León; Oliver J Fischer ORCID logo; +11 more... Ainoa Rueda-Zubiaurre; Jochen R Brandt ORCID logo; Álvaro Cortés; Anna Barnard; Matthew J Fuchter ORCID logo; Félix Calderón; Elizabeth A Winzeler; Robert E Sinden; Esperanza Herreros; Francisco J Gamo; Jake Baum; (2018) A high throughput screen for next-generation leads targeting malaria parasite transmission. NATURE COMMUNICATIONS, 9 (1). 3805-. ISSN 2041-1723 DOI: 10.1038/s41467-018-05777-2
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Spread of parasite resistance to artemisinin threatens current frontline antimalarial therapies, highlighting the need for new drugs with alternative modes of action. Since only 0.2-1% of asexual parasites differentiate into sexual, transmission-competent forms, targeting this natural bottleneck provides a tangible route to interrupt disease transmission and mitigate resistance selection. Here we present a high-throughput screen of gametogenesis against a ~70,000 compound diversity library, identifying seventeen drug-like molecules that target transmission. Hit molecules possess varied activity profiles including male-specific, dual acting male-female and dual-asexual-sexual, with one promising N-((4-hydroxychroman-4-yl)methyl)-sulphonamide scaffold found to have sub-micromolar activity in vitro and in vivo efficacy. Development of leads with modes of action focussed on the sexual stages of malaria parasite development provide a previously unexplored base from which future therapeutics can be developed, capable of preventing parasite transmission through the population.


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