Selective inhibitors of the mutant B-raf pathway: discovery of a potent and orally bioavailable aminoisoquinoline.

Adrian L. Smith,Frenel Fils Demorin,Nick A. Paras,Qi Huang,Jeffrey Petkus,Elizabeth M. Doherty,Thomas Nixey,Joseph L. Kim,Douglas A. Whittington,Linda F. Epstein,Matthew R. Lee,Mark Rose,Carol Babij,Manory Fernando,Kristen Hess,Quynh Le,Pedro J. Beltran,Josette Carnahan

Selective inhibitors of the mutant B-raf pathway: discovery of a potent and orally bioavailable aminoisoquinoline.

2009

Adrian L. Smith
Frenel Fils Demorin
Nick A. Paras
Qi Huang
Jeffrey Petkus
Elizabeth M. Doherty
Thomas Nixey
Joseph L. Kim
Douglas A. Whittington
Linda F. Epstein
Matthew R. Lee
Mark Rose
Carol Babij
Manory Fernando
Kristen Hess
Quynh Le
Pedro J. Beltran
Josette Carnahan

The discovery and optimization of a novel series of aminoisoquinolines as potent, selective, and efficacious inhibitors of the mutant B-Raf pathway is presented. The N-linked pyridylpyrimidine benzamide 2 was identified as a potent, modestly selective inhibitor of the B-Raf enzyme. Replacement of the benzamide with an aminoisoquinoline core significantly improved kinase selectivity and imparted favorable pharmacokinetic properties, leading to the identification of 1 as a potent antitumor agent in xenograft models.

Keywords:

Non-specific serine/threonine protein kinase
Enzyme
Benzamide
Signal transduction
Kinase
Mutant
Biochemistry
Bioavailability
Chemistry
Transferase
In vivo
In vitro

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