Aminopyrazole Carboxamide Bruton’s Tyrosine Kinase Inhibitors. Irreversible to Reversible Covalent Reactive Group Tuning

Mark E. Schnute,Stephen E. Benoit,Ingrid P. Buchler,Nicole Caspers,Margaret L. Grapperhaus,Seungil Han,Rajeev Hotchandani,Nelson Huang,Robert Hughes,Brian Juba,Kyung-Hee Kim,Erica Liu,Erin McCarthy,Dean Messing,Joy S. Miyashiro,Shashi Mohan,Thomas N. OConnell,Jeffrey F. Ohren,Mihir D. Parikh,Michelle A. Schmidt,Shaun R. Selness,John Robert Springer,Venkataraman Thanabal,John I. Trujillo,Daniel P. Walker,Zhao-Kui Wan,Jane M. Withka,Arthur J. Wittwer,Nancy Wood,Li Xing,Christoph Wolfgang Zapf,John Douhan

Aminopyrazole Carboxamide Bruton’s Tyrosine Kinase Inhibitors. Irreversible to Reversible Covalent Reactive Group Tuning

2019

Potent covalent inhibitors of Bruton’s tyrosine kinase (BTK) based on an aminopyrazole carboxamide scaffold have been identified. Compared to acrylamide-based covalent reactive groups leading to irreversible protein adducts, cyanamide-based reversible-covalent inhibitors provided the highest combined BTK potency and EGFR selectivity. The cyanamide covalent mechanism with BTK was confirmed through enzyme kinetic, NMR, MS, and X-ray crystallographic studies. The lead cyanamide-based inhibitors demonstrated excellent kinome selectivity and rat pharmacokinetic properties.

Keywords:

Biology
Enzyme
Biochemistry
Bruton's tyrosine kinase
Stereochemistry
Kinome
Tyrosine kinase
Transferase
Cyanamide
Carboxamide
Covalent bond

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