Synthesis and evaluation of indenopyrazoles as cyclin-dependent kinase inhibitors. Part 4: Heterocycles at C3

Eddy W. Yue,Susan V. Dimeo,C.Anne Higley,Jay A. Markwalder,Catherine R. Burton,Pamela A. Benfield,Robert H. Grafstrom,Sarah Cox,Jodi K. Muckelbauer,Angela Smallwood,Haiying Chen,Chong-Hwan Chang,George L. Trainor,Steven P. Seitz

Synthesis and evaluation of indenopyrazoles as cyclin-dependent kinase inhibitors. Part 4: Heterocycles at C3

2004

Eddy W. Yue
Susan V. Dimeo
C.Anne Higley
Jay A. Markwalder
Catherine R. Burton
Pamela A. Benfield
Robert H. Grafstrom
Sarah Cox
Jodi K. Muckelbauer
Angela Smallwood
Haiying Chen
Chong-Hwan Chang
George L. Trainor
Steven P. Seitz

New indeno[1,2-c]pyrazol-4-one cyclin dependent kinase inhibitors have been disclosed. The most promising compounds are nanomolar enzyme inhibitors with excellent activity against tumor cells. The most advanced compound retains cell culture activity even in the presence of human serum proteins. The most advanced compound did not kill the normal fibroblast line AG1523.

Keywords:

Blood proteins
Enzyme
Protein kinase A
Cyclin-dependent kinase
Biochemistry
Fibroblast
Organic chemistry
In vitro
Chemistry
Enzyme inhibitor
Cell culture

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