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Hit-to-lead optimization and kinase selectivity of imidazo [1, 2-a] quinoxalin-4-amine derived JNK1 inhibitors

Authors

Bei Li, Oana M Cociorva, Tyzoon Nomanbhoy, Helge Weissig, Qiang Li, Kai Nakamura, Marek Liyanage, Melissa C Zhang, Ann Y Shih, Arwin Aban, Yi Hu, Julia Cajica, Lan Pham, John W Kozarich, Kevin R Shreder

Publication date

2013/9/15

Journal

Bioorganic & medicinal chemistry letters

Volume

Issue

Pages

5217-5222

Publisher

Pergamon

Description

As the result of a rhJNK1 HTS, the imidazo[1,2-a]quinoxaline 1 was identified as a 1.6 μM rhJNK1 inhibitor. Optimization of this compound lead to AX13587 (rhJNK1 IC₅₀ = 160 nM) which was co-crystallized with JNK1 to identify key molecular interactions. Kinase profiling against 125+ kinases revealed AX13587 was an inhibitor of JNK, MAST3, and MAST4 whereas its methylene homolog AX14373 (native JNK1 IC₅₀ = 47 nM) was a highly specific JNK inhibitor.

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Cited by 31

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Scholar articles

Hit-to-lead optimization and kinase selectivity of imidazo [1, 2-a] quinoxalin-4-amine derived JNK1 inhibitors

B Li, OM Cociorva, T Nomanbhoy, H Weissig, Q Li… - Bioorganic & medicinal chemistry letters, 2013