Development of kinase inhibitors via metal-catalyzed c–h arylation of 8-alkyl-thiazolo[5,4-f]-quinazolin-9-ones designed by fragment-growing studies

Florence Couly; Marine Harari; Carole Dubouilh-Benard; Laetitia Bailly; Emilie Petit; Julien Diharce; Pascal Bonnet; Laurent Meijer; Corinne Fruit; Thierry Besson

Journal ArticleOPEN ACCESS

Development of kinase inhibitors via metal-catalyzed c–h arylation of 8-alkyl-thiazolo[5,4-f]-quinazolin-9-ones designed by fragment-growing studies

Molecules (2018) 23(9)

DOI: 10.3390/molecules23092181

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Abstract

Efficient metal catalyzed C–H arylation of 8-alkyl-thiazolo[5,4-f]-quinazolin-9-ones was explored for SAR studies. Application of this powerful chemical tool at the last stage of the synthesis of kinase inhibitors allowed the synthesis of arrays of molecules inspired by fragment-growing studies generated by molecular modeling calculations. Among the potentially active compounds designed through this strategy, FC162 (4c) exhibits nanomolar IC50 values against some kinases, and is the best candidate for the development as a DYRK kinase inhibitor.

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Couly, F., Harari, M., Dubouilh-Benard, C., Bailly, L., Petit, E., Diharce, J., … Besson, T. (2018). Development of kinase inhibitors via metal-catalyzed c–h arylation of 8-alkyl-thiazolo[5,4-f]-quinazolin-9-ones designed by fragment-growing studies. Molecules, 23(9). https://doi.org/10.3390/molecules23092181

Development of kinase inhibitors via metal-catalyzed c–h arylation of 8-alkyl-thiazolo[5,4-f]-quinazolin-9-ones designed by fragment-growing studies

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