PNAS 2007-12-18

A systematic interaction map of validated kinase inhibitors with Ser/Thr kinases.

Oleg Fedorov, Brian Marsden, Vanda Pogacic, Peter Rellos, Susanne Müller, Alex N Bullock, Juerg Schwaller, Michael Sundström, Stefan Knapp

Index: Proc. Natl. Acad. Sci. U. S. A. 104 , 20523-8, (2007)

Full Text: HTML

Abstract

Protein kinases play a pivotal role in cell signaling, and dysregulation of many kinases has been linked to disease development. A large number of kinase inhibitors are therefore currently under investigation in clinical trials, and so far seven inhibitors have been approved as anti-cancer drugs. In addition, kinase inhibitors are widely used as specific probes to study cell signaling, but systematic studies describing selectivity of these reagents across a panel of diverse kinases are largely lacking. Here we evaluated the specificity of 156 validated kinase inhibitors, including inhibitors used in clinical trials, against 60 human Ser/Thr kinases using a thermal stability shift assay. Our analysis revealed many unexpected cross-reactivities for inhibitors thought to be specific for certain targets. We also found that certain combinations of active-site residues in the ATP-binding site correlated with the detected ligand promiscuity and that some kinases are highly sensitive to inhibition using diverse chemotypes, suggesting them as preferred intervention points. Our results uncovered also inhibitor cross-reactivities that may lead to alternate clinical applications. For example, LY333'531, a PKCbeta inhibitor currently in phase III clinical trials, efficiently inhibited PIM1 kinase in our screen, a suggested target for treatment of leukemia. We determined the binding mode of this inhibitor by x-ray crystallography and in addition showed that LY333'531 induced cell death and significantly suppressed growth of leukemic cells from acute myeloid leukemia patients.


Related Compounds

Related Articles:

Photosensitizing properties of compounds related to benzophenone.

2013-01-01

[Acta Derm. Venereol. 93(1) , 30-2, (2013)]

Combined experimental and simulation studies suggest a revised mode of action of the anti-Alzheimer disease drug NQ-Trp.

2015-09-01

[Chemistry 21 , 12657-66, (2015)]

Posttranslational Regulation of Human DNA Polymerase ι.

2015-11-06

[J. Biol. Chem. 290 , 27332-44, (2015)]

Genotoxic and inflammatory effects of organic extracts from traffic-related particulate matter in human lung epithelial A549 cells: the role of quinones.

2013-03-01

[Toxicol. In Vitro 27(2) , 922-31, (2013)]

Bioactivities of simplified adociaquinone B and naphthoquinone derivatives against Cdc25B, MKP-1, and MKP-3 phosphatases.

2009-03-15

[Bioorg. Med. Chem. 17 , 2276-81, (2009)]

More Articles...