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Chemical Proteomics and Structural Biology Define EPHA2 Inhibition by Clinical Kinase Drugs.

ACS Chem. Biol.. 2016; 
HeinzlmeirStephanie,KudlinzkiDenis,SreeramuluSridhar,KlaegerSusan,GandeSantosh Lakshmi,LinhardVerena,WilhelmMathias,QiaoHuichao,HelmDominic,RuprechtBenjamin,SaxenaKrishna,MédardGuillaume,SchwalbeHarald,KusterBern
Products/Services Used Details Operation
Gene Synthesis In brief, synthesized EPHA2 gene (residues Asp596–Gly900, GenScript USA Inc) was sub-cloned into pTriEx 1. Get A Quote

摘要

The receptor tyrosine kinase EPHA2 (Ephrin type-A receptor 2) plays important roles in oncogenesis, metastasis, and treatment resistance, yet therapeutic targeting, drug discovery, or investigation of EPHA2 biology is hampered by the lack of appropriate inhibitors and structural information. Here, we used chemical proteomics to survey 235 clinical kinase inhibitors for their kinase selectivity and identified 24 drugs with submicromolar affinities for EPHA2. NMR-based conformational dynamics together with nine new cocrystal structures delineated drug-EPHA2 interactions in full detail. The combination of selectivity profiling, structure determination, and kinome wide sequence alignment allowed the... More

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