Author:
Huang Chun-Hao,Lujambio Amaia,Zuber Johannes,Tschaharganeh Darjus F.,Doran Michael G.,Evans Michael J.,Kitzing Thomas,Zhu Nan,de Stanchina Elisa,Sawyers Charles L.,Armstrong Scott A.,Lewis Jason S.,Sherr Charles J.,Lowe Scott W.
Abstract
One-year survival rates for newly diagnosed hepatocellular carcinoma (HCC) are <50%, and unresectable HCC carries a dismal prognosis owing to its aggressiveness and the undruggable nature of its main genetic drivers. By screening a custom library of shRNAs directed toward known drug targets in a genetically defined Myc-driven HCC model, we identified cyclin-dependent kinase 9 (Cdk9) as required for disease maintenance. Pharmacological or shRNA-mediated CDK9 inhibition led to robust anti-tumor effects that correlated with MYC expression levels and depended on the role that both CDK9 and MYC exert in transcription elongation. Our results establish CDK9 inhibition as a therapeutic strategy for MYC-overexpressing liver tumors and highlight the relevance of transcription elongation in the addiction of cancer cells to MYC.
Publisher
Cold Spring Harbor Laboratory
Subject
Developmental Biology,Genetics
Cited by
164 articles.
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