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Series GSE79446 Query DataSets for GSE79446
Status Public on Jun 07, 2016
Title Analysis of Paired Primary-Metastatic Hormone-Receptor Positive Breast Tumors (HRPBC) Uncovers Potential Novel Drivers of Hormonal Resistance
Organism Homo sapiens
Experiment type Genome variation profiling by genome tiling array
Summary We sought to identify genetic variants associated with disease relapse and failure to hormonal treatment in hormone-receptor positive breast cancer (HRPBC). We analyzed a series of HRPBC with distant relapse, by sequencing pairs (n=11) of tumors (primary and metastases) at >800X. Comparative genomic hybridization was performed as well. Top hits, based on the frequency of alteration and severity of the changes, were tested in the TCGA series. Genes determining the most parsimonious prognostic signature were studied for their functional role in vitro, by performing cell growth assays in hormonal-deprivation conditions, a setting that mimics treatment with aromatase inhibitors. Severe alterations were recurrently found in 18 genes in the pairs. However, only MYC, DNAH5, CSFR1, EPHA7, ARID1B, and KMT2C preserved an independent prognosis impact and/or showed a significantly different incidence of alterations between relapsed and non-relapsed cases in the TCGA series. The signature composed of MYC, KMT2C, and EPHA7 best discriminated the clinical course, (overall survival 90,7 vs. 144,5 months; p=0.0001). Having an alteration in any of the genes of the signature implied a hazard ratio of death of 3.25 (p<0.0001), and early relapse during the adjuvant hormonal treatment. The presence of the D348N mutation in KMT2C and/or the T666I mutation in the kinase domain of EPHA7 conferred hormonal resistance in vitro. Novel inactivating mutations in KMT2C and EPHA7, which confer hormonal resistance, are linked to adverse clinical course in HRPBC.
 
Overall design Pairs of tumors (primary and metastases)
 
Contributor(s) Manso L, Mouron S, Tress M, Gómez-López G, Morente M, Ciruelos E, Rubio-Camarillo M, Rodriguez-Peralto JL, Pujana MA, Pisano DG, Quintela-Fandino M
Citation(s) 27195705
Submission date Mar 21, 2016
Last update date Jun 09, 2016
Contact name Silvana Mouron
E-mail(s) smouron@cnio.es
Organization name CNIO
Department Clinical Research
Lab Breast Cancer Lab
Street address Calle Melchor Fdez Almagro
City Madrid
State/province Madrid
ZIP/Postal code 28029
Country Spain
 
Platforms (1)
GPL21613 Agilent-021924 SurePrint G3 Human CGH Microarray 8x60K (Feature number version, hg19:GRCh37:Feb2009)
Samples (16)
GSM2095470 A-7111476 (met)
GSM2095471 A-7111475 (prim)
GSM2095472 C-7111479 (met)
Relations
BioProject PRJNA315859

Download family Format
SOFT formatted family file(s) SOFTHelp
MINiML formatted family file(s) MINiMLHelp
Series Matrix File(s) TXTHelp

Supplementary file Size Download File type/resource
GSE79446_RAW.tar 103.0 Mb (http)(custom) TAR (of TXT)
Processed data included within Sample table
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