Potent inhibitors of malarial P. Falciparum protein kinase G: Improving the cell activity of a series of imidazopyridines

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

Potent inhibitors of malarial P. Falciparum protein kinase G: Improving the cell activity of a series of imidazopyridines

2019

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

Abstract Development of a class of bicyclic inhibitors of the Plasmodium falciparum cyclic GMP-dependent protein kinase ( Pf PKG), starting from known compounds with activity against a related parasite PKG orthologue, is reported. Examination of key sub-structural elements led to new compounds with good levels of inhibitory activity against the recombinant kinase and in vitro activity against the parasite. Key examples were shown to possess encouraging in vitro ADME properties, and computational analysis provided valuable insight into the origins of the observed activity profiles.

Keywords:

Protein kinase A
Cell
ADME
Biochemistry
Plasmodium falciparum
Recombinant DNA
Bicyclic molecule
Chemistry
Kinase
cGMP-dependent protein kinase
In vitro
Imidazopyridine

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