Discovery of new quinoline ether inhibitors with high affinity and selectivity for PDGFR tyrosine kinases.

Patrick Ple,Frederic Henri Jung,Sue Ashton,Laurent Francois Andre Hennequin,Romuald Laine,Christine Lambert-van der Brempt,Rémy Morgentin,Georges Rene Pasquet,Sian Tomiko Taylor

Discovery of new quinoline ether inhibitors with high affinity and selectivity for PDGFR tyrosine kinases.

2012

Patrick Ple
Frederic Henri Jung
Sue Ashton
Laurent Francois Andre Hennequin
Romuald Laine
Christine Lambert-van der Brempt
Rémy Morgentin
Georges Rene Pasquet
Sian Tomiko Taylor

Abstract A new series of quinoline ether inhibitors, which potently and selectively inhibit PDGFR tyrosine kinases, is described in this Letter. Compounds 23 and 33 are selective, low nanomolar inhibitors of PDGFRα and β, display good pharmacokinetics in rat and dog and are active in vivo at low doses when given orally twice daily. Further evaluation of these compounds is warranted.

Keywords:

Selectivity
Ether
In vivo
PDGFR Inhibitors
Quinoline
Stereochemistry
Biochemistry
Tyrosine kinase
Pharmacokinetics
Chemistry
Platelet-derived growth factor receptor
low doses
Pharmacology

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