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

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

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

2019

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

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.

Keywords:

Cell potency
Chemistry
cGMP-dependent protein kinase
Novelty
Kinase
Protein kinase A
Biochemistry
Potency
Imidazopyridine
ADME
Plasmodium falciparum

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