Phthalazinone Pyrazoles as Potent, Selective, and Orally Bioavailable Inhibitors of Aurora-A Kinase

Michael Prime,Stephen Martin Courtney,Frederick Arthur Brookfield,Richard W. Marston,Victoria Walker,Justin Warne,Andrew E. Boyd,Norman Kairies,Wolfgang Von Der Dr Rer N Saal,Anja Limberg,Guy Georges,Richard A. Engh,Bernhard Goller,Petra Rueger,Matthias Rueth

Phthalazinone Pyrazoles as Potent, Selective, and Orally Bioavailable Inhibitors of Aurora-A Kinase

2011

Michael Prime
Stephen Martin Courtney
Frederick Arthur Brookfield
Richard W. Marston
Victoria Walker
Justin Warne
Andrew E. Boyd
Norman Kairies
Wolfgang Von Der Dr Rer N Saal
Anja Limberg
Guy Georges
Richard A. Engh
Bernhard Goller
Petra Rueger
Matthias Rueth

The inhibition of Aurora kinases in order to arrest mitosis and subsequently inhibit tumor growth via apoptosis of proliferating cells has generated significant discussion within the literature. We report a novel class of Aurora kinase inhibitors based upon a phthalazinone pyrazole scaffold. The development of the phthalazinone template resulted in a potent Aurora-A selective series of compounds (typically >1000-fold selectivity over Aurora-B) that display good pharmacological profiles with significantly improved oral bioavailability compared to the well studied Aurora inhibitor VX-680.

Keywords:

Pyrazole
Aurora A kinase
Organic chemistry
Aurora kinase
Bioavailability
Apoptosis
Kinase
Mitosis
Aurora inhibitor
Biochemistry
Biology
Chemistry

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