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Series GSE87418

Query DataSets for GSE87418

Status

Public on Jan 20, 2017

Title

Enhancer Remodeling During Adaptive Bypass to MEK Inhibition Is Attenuated by Pharmacological Targeting of the P-TEFb Complex (ChIP-seq)

Organism

Experiment type

Genome binding/occupancy profiling by high throughput sequencing

Summary

Targeting the dysregulated BRaf-MEK-ERK pathway in cancer has increasingly emerged in clinical trial design. Despite clinical responses in specific cancers using inhibitors targeting BRaf and MEK, resistance develops often involving non-genomic adaptive bypass mechanisms. Inhibition of MEK1/2 by trametinib in triple negative breast cancer (TNBC) patients induced dramatic transcriptional responses, including upregulation of receptor tyrosine kinases (RTKs) comparing tumor samples before and after one week of treatment. In preclinical models MEK inhibition induced genome-wide enhancer formation involving the seeding of BRD4, MED1, H3K27 acetylation and p300 that drives transcriptional adaptation. Inhibition of P-TEFb associated proteins BRD4 and CBP/p300 arrested enhancer seeding and RTK upregulation. BRD4 bromodomain inhibitors overcame trametinib resistance, producing sustained growth inhibition in cells, xenografts and syngeneic mouse TNBC models. Pharmacological targeting of P-TEFb members in conjunction with MEK inhibition by trametinib is an effective strategy to durably inhibit epigenomic remodeling required for adaptive resistance.

Overall design

44 experimental samples analyzed, one chromatin input control sample for each cell line

Contributor(s)

Johnson GL, Zawistowski JS

Citation(s)

Submission date

Sep 28, 2016

Last update date

May 15, 2019

Contact name

Gary L Johnson

E-mail(s)

glj@med.unc.edu

Organization name

University of North Carolina School of Medicine

Department

Pharmacology

Lab

Gary L. Johnson Lab

Street address

4009 Genetic Medicine Building, 120 Mason Farm Road

City

Chapel Hill

State/province

NC

ZIP/Postal code

27599

Country

USA

Platforms (2)

GPL11154	Illumina HiSeq 2000 (Homo sapiens)
GPL18573	Illumina NextSeq 500 (Homo sapiens)

Samples (61)

More...

GSM2330549	SUM159_BRD4_DMSO_24h
GSM2330550	SUM159_BRD4_100nMtrametinib_24h
GSM2330551	SUM159_BRD4_300nMJQ1_24h

GSM2330552	SUM159_BRD4_100nMtrametinib300nMJQ1_24h
GSM2330553	SUM159_MED1_DMSO_24h
GSM2330554	SUM159_MED1_100nMtrametinib_24h
GSM2330555	SUM159_MED1_300nMJQ1_24h
GSM2330556	SUM159_MED1_100nMtrametinib300nMJQ1_24h
GSM2330557	SUM159_p300_DMSO_24h
GSM2330558	SUM159_p300_100nMtrametinib_24h
GSM2330559	SUM159_p300_300nMJQ1_24h
GSM2330560	SUM159_p300_100nMtrametinib300nMJQ1_24h
GSM2330561	SUM159_H3K27ac_DMSO_24h
GSM2330562	SUM159_H3K27ac_100nMtrametinib_24h
GSM2330563	SUM159_H3K27ac_300nMJQ1_24h
GSM2330564	SUM159_H3K27ac_100nMtrametinib300nMJQ1_24h
GSM2330565	SUM159_CEBPB_DMSO_24h
GSM2330566	SUM159_CEBPB_100nMtrametinib_24h
GSM2330567	SUM159_CEBPB_300nMJQ1_24h
GSM2330568	SUM159_CEBPB_100nMtrametinib300nMJQ1_24h
GSM2330569	SUM159_H3K4me1_DMSO_24h
GSM2330570	SUM159_H3K4me1_100nMtrametinib_24h
GSM2330571	SUM159_H3K4me3_DMSO_24h
GSM2330572	SUM159_H3K4me3_500nMtrametinib_24h
GSM2330573	SUM159_input_DMSO_24h
GSM2330574	HCC1806_BRD4_DMSO_24h
GSM2330575	HCC1806_BRD4_100nMtrametinib_24h
GSM2330576	HCC1806_BRD4_300nMJQ1_24h
GSM2330577	HCC1806_BRD4_100nMtrametinib300nMJQ1_24h
GSM2330578	HCC1806_input_DMSO_24h
GSM2330579	Figure7_SUM159_BRD4_DMSO_24h
GSM2330580	Figure7_SUM159_BRD4_100nMtrametinib_24h
GSM2330581	Figure7_SUM159_BRD4_100nMtrametinib1uMSGCCBP30_24h
GSM2330582	Figure7_SUM159_BRD4_100nMtrametinib300nMJIB04_24h
GSM2330583	Figure7_SUM159_p300_DMSO_24h
GSM2330584	Figure7_SUM159_p300_100nMtrametinib_24h
GSM2330585	Figure7_SUM159_p300_100nMtrametinib1uMSGCCBP30_24h
GSM2330586	Figure7_SUM159_p300_100nMtrametinib300nMJIB04_24h
GSM2330587	SUM159_BRD4_DMSO_8h
GSM2330588	SUM159_BRD4_100nMtrametinib_8h
GSM2330589	SUM159_BRD4_30nMbortezomib_8h
GSM2330590	SUM159_BRD4_100nMtrametinib30nMbortezomib_8h
GSM2330591	SUM159_BRD4_DMSO_48h
GSM2330592	SUM159_BRD4_100nMtrametinib_48h
GSM2330593	SUM159_BRD4_dox_48h
GSM2330594	SUM159_input_DMSO_48h
GSM2330595	SUM159shMYC_BRD4_DMSO_48h
GSM2330596	SUM159shMYC_BRD4_100nMtrametinib_48h
GSM2330597	SUM159shMYC_BRD4_dox_48h
GSM2330598	SUM159shMYC_input_DMSO_48h
GSM2330599	timecourse_SUM159_BRD4_DMSO_72h
GSM2330600	timecourse_SUM159_BRD4_100nMtrametinib_1h
GSM2330601	timecourse_SUM159_BRD4_100nMtrametinib_4h
GSM2330602	timecourse_SUM159_BRD4_100nMtrametinib_24h
GSM2330603	timecourse_SUM159_BRD4_100nMtrametinib_72h
GSM2330604	SUM229pos_BRD4_DMSO_24h
GSM2330605	SUM229pos_BRD4_30nMtrametinib_24h
GSM2330606	SUM229pos_input_DMSO_24h
GSM2330607	SUM229neg_BRD4_DMSO_24h
GSM2330608	SUM229neg_BRD4_30nMtrametinib_24h
GSM2330609	SUM229neg_input_DMSO_24h

This SubSeries is part of SuperSeries:

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

Relations

BioProject

SRA

Download family	Format
SOFT formatted family file(s)	SOFT
MINiML formatted family file(s)	MINiML
Series Matrix File(s)	TXT

Supplementary file	Size	Download	File type/resource
GSE87418_Figure7_peakclassification.xlsx	8.6 Mb	(ftp)(http)	XLSX
GSE87418_RAW.tar	93.5 Mb	(http)(custom)	TAR (of BED)
GSE87418_SupplementaryTableS4_peakclassification.xlsx	8.4 Mb	(ftp)(http)	XLSX
GSE87418_SupplementaryTableS5_peakclassification.xlsx	4.2 Mb	(ftp)(http)	XLSX
GSE87418_peakclassification_SUM229neg.xlsx	5.0 Mb	(ftp)(http)	XLSX
GSE87418_peakclassification_SUM229pos.xlsx	5.0 Mb	(ftp)(http)	XLSX
GSE87418_peakclassification_bortezomib.xlsx	7.2 Mb	(ftp)(http)	XLSX
GSE87418_peakclassification_shMYC.xlsx	7.6 Mb	(ftp)(http)	XLSX
GSE87418_peakclassification_trametinib_timecourse.xlsx	7.5 Mb	(ftp)(http)	XLSX
SRA Run Selector
Raw data are available in SRA
Processed data provided as supplementary file
Processed data are available on Series record

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