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Series GSE22615

Query DataSets for GSE22615

Status

Public on Mar 16, 2011

Title

Genomic alterations of chromosome 11 induce transcriptomic dysregulation in aggressive and malignant prolactin tumours

Organism

Homo sapiens

Experiment type

Genome variation profiling by SNP array

Summary

Pituitary tumors are generally considered as benign. However, many are invasive (45 to 55%) and some are described as aggressive with a high proliferation rate and short post-operative time to recurrence and 0.2% metastasize. The molecular events associated to the progression of the pituitary tumor toward an aggressive and malignant phenotype is still unresolved. To bring new hypothesis on signaling pathways associated to the tumor progression, we applied a wide genome analysis approach combining transcriptome analysis and CGH analysis on the same 13 prolactin tumours classified as non-invasive (n=5), invasive (n=2) and agressive-invasive tumors (n=6). In 5/6 agressive-invasive tumours a loss of a common region in the p arm of the chromosome 11 was detected. This region extending from position 14.9 to position 46.5 Mb harbours the cytobands 11p15.2, 11p15.1, 11p14.3, 11p14.2, 11p14.1, 11p13, 11p12 and 11p11.2. In 3 of these 5 tumours considered as carcinomas because of the presence of metastasis, an allelic loss is also observed in the 11q arm. The combination of data coming from genome structure exploration and transcriptomic analysis showed that allelic loss impact the expression of genes harbored in the imbalanced region. Data filtering strategy allowed us to highlight among the 139 genes harbored in the 11p region loss, 5 genes (DGKZ, CD44, TSG101, GTF2H1 and HTATIP2) that could be candidate gene for triggering the progression of prolactin tumour toward an aggressive and malignant phenotype. Finally, specific DNA alterations give one molecular argument more to consider agressive-invasive tumour and carcinomas as a distinct step in progression of the pituitary tumours.

Overall design

Copy number analysis of Affymetrix Genome-Wide Human SNP Array 6.0 was performed for 13 prolactin tumors, 6 aggressive-invasive, 2 invasive, 5 non-invasive. The same analysis was performed for one normal pituitary and one genomic DNA called "reference 103" from Affymetrix.

Contributor(s)

WIERINCKX A, ROCHE M, LEGRAS-LACHUER C, NAZARET N, CROZE S, RAVEROT G, REY C, AUGER C, JOUANNEAU E, CHANSON P, TROUILLAS J, LACHUER J

Citation(s)

21251114

Submission date

Jun 29, 2010

Last update date

Jan 08, 2019

Contact name

Joël LACHUER

E-mail(s)

lachuer@univ-lyon1.fr

Phone

04 72 91 34 93

Organization name

INSERM

Department

U842

Street address

16 avenue du Doyen Lépine

City

BRON

ZIP/Postal code

69676

Country

France

Platforms (1)

GPL6801

[GenomeWideSNP_6] Affymetrix Genome-Wide Human SNP 6.0 Array

Samples (15)

More...

GSM560908	agressive-invasive prolactin pituitary tumours 1
GSM560909	agressive-invasive prolactin pituitary tumours 2
GSM560910	agressive-invasive prolactin pituitary tumours 3

This SubSeries is part of SuperSeries:

GSE32191

Genomic alterations of chromosome 11 induce transcriptome dysregulation in aggressive and malignant prolactin tumours

Relations

BioProject

PRJNA153905

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
GSE22615_RAW.tar	635.8 Mb	(http)(custom)	TAR (of CEL, CHP)
Processed data included within Sample table
Processed data provided as supplementary file