Enhancer Remodeling during Adaptive Bypass to MEK Inhibition Is Attenuated by Pharmacologic Targeting of the P-TEFb Complex

适应性旁路 MEK 抑制过程中的增强子重塑可通过 P-TEFb 复合物的药理靶向作用减弱

阅读：8

作者：Jon S Zawistowski, Samantha M Bevill, Daniel R Goulet, Timothy J Stuhlmiller, Adriana S Beltran, Jose F Olivares-Quintero, Darshan Singh, Noah Sciaky, Joel S Parker, Naim U Rashid, Xin Chen, James S Duncan, Martin C Whittle, Steven P Angus, Sara Hanna Velarde, Brian T Golitz, Xiaping He, Charlene Sa

期刊：

Cancer Discovery

影响因子：

29.700

时间：

2017

起止号：

2017 Mar;7(3):302-321.

doi：

10.1158/2159-8290.CD-16-0653

种属：

Human

方法学：

IHC、IP、WB

靶点：

MED1

研究方向：

信号转导

Significance

Widespread transcriptional adaptation to pharmacologic MEK inhibition was observed in TNBC patient tumors. In preclinical models, MEK inhibition induces dramatic genome-wide modulation of chromatin, in the form of de novo enhancer formation and enhancer remodeling. Pharmacologic targeting of P-TEFb complex members at enhancers is an effective strategy to durably inhibit such adaptation. Cancer Discov; 7(3); 302-21. ©2017 AACR.This article is highlighted in the In This Issue feature, p. 235.

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