Cyclin-dependent kinase 12 is a drug target for visceral leishmaniasis

Authors :: Stephanie Gresham
Stephen Patterson
Laste Stojanovski
Fabio Zuccotto
Susan Wyllie
Matthew Berriman
Timothy J. Miles
Frederick R. C. Simeons
Nadine Homeyer
Lorna MacLean
Paul Connolly
Lalitha Sastry
Manu De Rycker
Rhiannon Lowe
Gerard Drewes
Sabrinia D. Crouch
David W. Gray
Thomas D. Otto
Sebastian Albrecht
Michael G. Thomas
Michael A. J. Ferguson
Sujatha Manthri
Michael D. Urbaniak
Markus Boesche
Hannah Pflaumer
Alan H. Fairlamb
Ian H. Gilbert
Sonja Ghidelli-Disse
Kevin D. Read
Paul G. Wyatt
Jose M. Fiandor
Susan Dixon
Source :: Nature
Publication Year :: 2017
Abstract: Visceral leishmaniasis causes considerable mortality and morbidity in many parts of the world. There is an urgent need for the development of new, effective treatments for this disease. Here we describe the development of an anti-leishmanial drug-like chemical series based on a pyrazolopyrimidine scaffold. The leading compound from this series (7, DDD853651/GSK3186899) is efficacious in a mouse model of visceral leishmaniasis, has suitable physicochemical, pharmacokinetic and toxicological properties for further development, and has been declared a preclinical candidate. Detailed mode-of-action studies indicate that compounds from this series act principally by inhibiting the parasite cdc-2-related kinase 12 (CRK12), thus defining a druggable target for visceral leishmaniasis.

Tools