Pyrazolobenzodiazepines: Part I. Synthesis and SAR of a potent class of kinase inhibitors

Jin-Jun Liu,Irena Daniewski,Qingjie Ding,Brian Higgins,Grace Ju,Kenneth Kolinsky,Fred Konzelmann,Christine Lukacs,Giacomo Pizzolato,Pamela Loreen Rossman,Amy Swain,Kshitij Chhabilbhai Thakkar,Chung Chen Wei,Dorota Miklowski,Hong Yang,Xuefeng Yin,Peter Michael Wovkulich

Pyrazolobenzodiazepines: Part I. Synthesis and SAR of a potent class of kinase inhibitors

2010

Jin-Jun Liu
Irena Daniewski
Qingjie Ding
Brian Higgins
Grace Ju
Kenneth Kolinsky
Fred Konzelmann
Christine Lukacs
Giacomo Pizzolato
Pamela Loreen Rossman
Amy Swain
Kshitij Chhabilbhai Thakkar
Chung Chen Wei
Dorota Miklowski
Hong Yang
Xuefeng Yin
Peter Michael Wovkulich

Abstract A novel series of pyrazolobenzodiazepines 3 has been identified as potent inhibitors of cyclin-dependent kinase 2 (CDK2). Their synthesis and structure–activity relationships (SAR) are described. Representative compounds from this class reversibly inhibit CDK2 activity in vitro, and block cell cycle progression in human tumor cell lines. Further exploration has revealed that this class of compounds inhibits several kinases that play critical roles in cancer cell growth and division as well as tumor angiogenesis. Together, these properties suggest a compelling basis for their use as antitumor agents.

Keywords:

Cell cycle
Cyclin-dependent kinase
Cell growth
Angiogenesis
Cyclin-dependent kinase 2
Organic chemistry
Biochemistry
Kinase
Structure–activity relationship
Enzyme inhibitor
Chemistry
Cancer cell
In vitro
Cytotoxicity
Cell culture

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations