Comprehensive assay of kinase catalytic activity reveals features of kinase inhibitor selectivity

The promiscuity of most kinase inhibitors can cause drug toxicity and complicate the interpretation of experiments. Rather than assessing kinase-compound binding, Anastassiadis et al . use functional assays to profile the activities of 178 commercially available kinase inhibitors against 300 recombi...

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Veröffentlicht in:Nature biotechnology 2011-11, Vol.29 (11), p.1039-1045
Hauptverfasser: Anastassiadis, Theonie, Deacon, Sean W, Devarajan, Karthik, Ma, Haiching, Peterson, Jeffrey R
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Sprache:eng
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Zusammenfassung:The promiscuity of most kinase inhibitors can cause drug toxicity and complicate the interpretation of experiments. Rather than assessing kinase-compound binding, Anastassiadis et al . use functional assays to profile the activities of 178 commercially available kinase inhibitors against 300 recombinant human protein kinases. Small-molecule protein kinase inhibitors are widely used to elucidate cellular signaling pathways and are promising therapeutic agents. Owing to evolutionary conservation of the ATP-binding site, most kinase inhibitors that target this site promiscuously inhibit multiple kinases. Interpretation of experiments that use these compounds is confounded by a lack of data on the comprehensive kinase selectivity of most inhibitors. Here we used functional assays to profile the activity of 178 commercially available kinase inhibitors against a panel of 300 recombinant protein kinases. Quantitative analysis revealed complex and often unexpected interactions between protein kinases and kinase inhibitors, with a wide spectrum of promiscuity. Many off-target interactions occur with seemingly unrelated kinases, revealing how large-scale profiling can identify multitargeted inhibitors of specific, diverse kinases. The results have implications for drug development and provide a resource for selecting compounds to elucidate kinase function and for interpreting the results of experiments involving kinase inhibitors.
ISSN:1087-0156
1546-1696
DOI:10.1038/nbt.2017