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Merck

Conformation-Selective Analogues of Dasatinib Reveal Insight into Kinase Inhibitor Binding and Selectivity.

ACS chemical biology (2016-02-20)
Frank E Kwarcinski, Kristoffer R Brandvold, Sameer Phadke, Omar M Beleh, Taylor K Johnson, Jennifer L Meagher, Markus A Seeliger, Jeanne A Stuckey, Matthew B Soellner
RÉSUMÉ

In the kinase field, there are many widely held tenets about conformation-selective inhibitors that have yet to be validated using controlled experiments. We have designed, synthesized, and characterized a series of kinase inhibitor analogues of dasatinib, an FDA-approved kinase inhibitor that binds the active conformation. This inhibitor series includes two Type II inhibitors that bind the DFG-out inactive conformation and two inhibitors that bind the αC-helix-out inactive conformation. Using this series of compounds, we analyze the impact that conformation-selective inhibitors have on target binding and kinome-wide selectivity.

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UM-164 trifluoroacetate salt, ≥98% (HPLC)