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Mapping phospho-catalytic dependencies of therapy-resistant tumours reveals actionable vulnerabilities.

Nat Cell Biol. 2019-06; 
CoppéJean-Philippe,MoriMiki,PanBo,YauChristina,WolfDenise M,Ruiz-SaenzAna,BrunenDiede,PrahalladAnirudh,Cornelissen-SteijgerPaulien,KemperKristel,PoschChristian,WangChangjun,DreyerCourtney A,KrijgsmanOscar,LeePei Rong Evelyn,ChenZhongzhong,PeeperDaniel S,MoasserMark M,BernardsRené,van 't VeerLau
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摘要

Phosphorylation networks intimately regulate mechanisms of response to therapies. Mapping the phospho-catalytic profile of kinases in cells or tissues remains a challenge. Here, we introduce a practical high-throughput system to measure the enzymatic activity of kinases using biological peptide targets as phospho-sensors to reveal kinase dependencies in tumour biopsies and cell lines. A 228-peptide screen was developed to detect the activity of >60?kinases, including ABLs, AKTs, CDKs and MAPKs. Focusing on BRAF tumours, we found mechanisms of intrinsic resistance to BRAF-targeted therapy in colorectal cancer, including targetable parallel activation of PDPK1 and PRKCA. Furthermore, mapping the pho... More

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