Potent bicyclic inhibitors of malarial cGMP-dependent protein kinase: approaches to combining improvements in cell potency, selectivity and structural novelty.

Ansell, Keith H; Baker, David A; Birchall, Kristian; Bouloc, Nathalie S; Bowyer, Paul W; Coombs, Peter J; Kettleborough, Catherine A; Large, Jonathan M; Merritt, Andy T; Osborne, Simon A; Smiljanic-Hurley, Ela; Stewart, Lindsay B; Tsagris, Denise J; Whalley, David; Wheldon, Mary C

Potent bicyclic inhibitors of malarial cGMP-dependent protein kinase: approaches to combining improvements in cell potency, selectivity and structural novelty.

Authors: Keith H Ansell
David A Baker
Kristian Birchall
Nathalie S Bouloc
Paul W Bowyer
Peter J Coombs
Catherine A Kettleborough
Jonathan M Large
Andy T Merritt
Simon A Osborne
Ela Smiljanic-Hurley
Lindsay B Stewart
Denise J Tsagris
David Whalley
Mary C Wheldon
Publication date: 9 August 2019
Publisher: 'Elsevier BV'
Doi

Abstract

Focussed studies on imidazopyridine inhibitors of Plasmodium falciparum cyclic GMP-dependent protein kinase (PfPKG) have significantly advanced the series towards desirable in vitro property space. LLE-based approaches towards combining improvements in cell potency, key physicochemical parameters and structural novelty are described, and a structure-based design hypothesis relating to substituent regiochemistry has directed efforts towards key examples with well-balanced potency, ADME and kinase selectivity profiles

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Last time updated on 07/10/2019