Synapse - Crystal structures of the kinase domain of c-Abl in complex with the small molecule inhibitors PD173955 and imatinib (STI-571)

Crystal structures of the kinase domain of c-Abl in complex with the small molecule inhibitors PD173955 and imatinib (STI-571) Journal Article

Authors:	Nagar, B.; Bornmann, W. G.; Pellicena, P.; Schindler, T.; Veach, D. R.; Miller, W. T.; Clarkson, B.; Kuriyan, J.
Article Title:	Crystal structures of the kinase domain of c-Abl in complex with the small molecule inhibitors PD173955 and imatinib (STI-571)
Abstract:	The inadvertent fusion of the bcr gene with the abl gene results in a constitutively active tyrosine kinase (Bcr-Abl) that transforms cells and causes chronic myelogenous leukemia. Small molecule inhibitors of Bcr-Abl that bind to the kinase domain can be used to treat chronic myelogenous leukemia. We report crystal structures of the kinase domain of Abl in complex with two such inhibitors, imatinib (also known as STI-571 and Gleevec) and PD173955 (Parke-Davis). Both compounds bind to the canonical ATP-binding site of the kinase domain, but they do so in different ways. As shown previously in a crystal structure of Abl bound to a smaller variant of STI-571, STI-571 captures a specific inactive conformation of the activation loop of Abl in which the loop mimics bound peptide substrate. In contrast, PD173955 binds to a conformation of AN in which the activation loop resembles that of an active kinase. The structure suggests that PD173955 would be insensitive to whether the conformation of the activation loop corresponds to active kinases or to that seen in the STI-571 complex. lit vitro kinase assays confirm that this is the case and indicate that PD173955 is at least 10-fold more inhibitory than STI-571. The structures suggest that PD173955 achieves its greater potency over STI-571 by being able to target multiple forms of Abl (active or inactive), whereas STI-571 requires a specific inactive conformation of Abl.
Keywords:	autophosphorylation; receptor; tyrosine kinase; bcr-abl; cells; mechanism; growth; dependent protein-kinase; catalytic subunit; hck
Journal Title:	Cancer Research
Volume:	62
Issue:	15
ISSN:	0008-5472
Publisher:	American Association for Cancer Research
Date Published:	2002-08-01
Start Page:	4236
End Page:	4243
Language:	English
ACCESSION:	WOS:000177105600014
PROVIDER:	wos
PUBMED:	12154025
Notes:	Article -- Source: Wos

Citation Impact

What is Dimensions Citation Badge?

MSK Authors

112 Bornmann
97 Veach
220 Clarkson

Related MSK Work

Structural Mechanism For Sti 571 Inhibition Of Abelson Tyrosine Kinase

Science 2000
Inhibition Of Wild Type And Mutant Bcr Abl By Pyrido Pyrimidine Type Small Molecule Kinase Inhibitors

Cancer Research 2003
A Novel Pyridopyrimidine Inhibitor Of Abl Kinase Is A Picomolar Inhibitor Of Bcr Abl Driven K562 Cells And Is Effective Against Sti571 Resistant Bcr Abl Mutants

Clinical Cancer Research 2003
Structural Basis For The Autoinhibition Of C Abl Tyrosine Kinase

Cell 2003
A Novel Mode Of Gleevec Binding Is Revealed By The Structure Of Spleen Tyrosine Kinase

Journal of Biological Chemistry 2004