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Clinical stage EGFR inhibitors irreversibly alkylate Bmx kinase

Authors:	Hur Wooyoung Velentza Anastasia Kim Sungjoon Flatauer Laura Jiang Xinnong Valente David Mason Daniel E Suzuki Melissa Larson Brad Zhang Jianming Zagorska Anna Didonato Michael Nagle Advait Warmuth Markus Balk Steven P Peters Eric C Gray Nathanael S

Institution:	Department of Chemistry, The Scripps Research Institute, La Jolla, CA 92037, USA.

Abstract:	Irreversible HER/erbB inhibitors selectively inhibit HER-family kinases by targeting a unique cysteine residue located within the ATP-binding pocket. Sequence alignment reveals that this rare cysteine is also present in ten other protein kinases including all five Tec-family members. We demonstrate that the Tec-family kinase Bmx is potently inhibited by irreversible modification at Cys496 by clinical stage EGFR inhibitors such as CI-1033. This cross-reactivity may have significant clinical implications.

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