The Discovery of Azd5597, a Potent Imidazole Pyrimidine Amide Cdk Inhibitor Suitable for Intravenous Dosing.

Clifford David Jones,David M. Andrews,Andrew John Barker,Kevin Blades,Paula Daunt,Simon J. East,Catherine Geh,Mark A. Graham,Keith M. Johnson,Sarah A. Loddick,Heather M. McFarland,Alexandra McGregor,Louise Moss,David Alan Rudge,Peter B. Simpson,Michael Lingard Swain,Kin Yip Tam,J.A. Tucker,Mike Walker

The Discovery of Azd5597, a Potent Imidazole Pyrimidine Amide Cdk Inhibitor Suitable for Intravenous Dosing.

2008

Clifford David Jones
David M. Andrews
Andrew John Barker
Kevin Blades
Paula Daunt
Simon J. East
Catherine Geh
Mark A. Graham
Keith M. Johnson
Sarah A. Loddick
Heather M. McFarland
Alexandra McGregor
Louise Moss
David Alan Rudge
Peter B. Simpson
Michael Lingard Swain
Kin Yip Tam
J.A. Tucker
Mike Walker

The development of a novel series of imidazole pyrimidine amides as cyclin-dependent kinase (CDK) inhibitors is described. Optimisation of inhibitory potency against multiple CDK’s (1, 2 and 9) resulted in imidazole pyrimidine amides with potent in vitro anti-proliferative effects against a range of cancer cell lines. Excellent physiochemical properties and large margins against inhibition of CYP isoforms and the hERG ion channel were achieved by modification of lipophilicity and amine basicity. A candidate with disease model activity in human cancer cell line xenografts and with suitable physiochemical and pharmacokinetic profiles for intravenous (iv) dosing was selected for further development as AZD5597.

Keywords:

hERG
Potency
CDK inhibitor
Cyclin-dependent kinase
Kinase
Imidazole
Amide
Organic chemistry
Enzyme inhibitor
Biochemistry
Chemistry
Lipophilicity
Biological activity
Pyrimidine

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