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A road map to evaluate the proteome-wide selectivity of covalent kinase inhibitors.

Nature chemical biology (2014-07-21)
Bryan R Lanning, Landon R Whitby, Melissa M Dix, John Douhan, Adam M Gilbert, Erik C Hett, Theodore O Johnson, Chris Joslyn, John C Kath, Sherry Niessen, Lee R Roberts, Mark E Schnute, Chu Wang, Jonathan J Hulce, Baoxian Wei, Laurence O Whiteley, Matthew M Hayward, Benjamin F Cravatt
RÉSUMÉ

Kinases are principal components of signal transduction pathways and the focus of intense basic and drug discovery research. Irreversible inhibitors that covalently modify non-catalytic cysteines in kinase active sites have emerged as valuable probes and approved drugs. Many protein classes, however, have functional cysteines, and therefore understanding the proteome-wide selectivity of covalent kinase inhibitors is imperative. Here, we accomplish this objective using activity-based protein profiling coupled with quantitative MS to globally map the targets, both specific and nonspecific, of covalent kinase inhibitors in human cells. Many of the specific off-targets represent nonkinase proteins that, notably, have conserved active site cysteines. We define windows of selectivity for covalent kinase inhibitors and show that, when these windows are exceeded, rampant proteome-wide reactivity and kinase target-independent cell death conjointly occur. Our findings, taken together, provide an experimental road map to illuminate opportunities and surmount challenges for the development of covalent kinase inhibitors.

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PF-06658607, ≥98% (HPLC)