Meta-analysis and gene set enrichment relative to er status reveal elevated activity of MYC and E2F in the "basal" breast cancer subgroup.

Meta-analysis and gene set enrichment relative to er status reveal elevated activity of MYC and E2F in the "basal" breast cancer subgroup.

BACKGROUND: Breast cancers lacking the estrogen receptor (ER) can be distinguished from other breast cancers on the basis of poor prognosis, high grade, distinctive histopathology and unique molecular signatures. These features further distinguish estrogen receptor negative (ER-) tumor subtypes, but...

Full description

Bibliographic Details
Main Authors: M Chehani Alles, Margaret Gardiner-Garden, David J Nott, Yixin Wang, John A Foekens, Robert L Sutherland, Elizabeth A Musgrove, Christopher J Ormandy
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2009-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2650420?pdf=render
id doaj-afc2d639ce064559bcddd2f7fea1a5ef
record_format Article
spelling doaj-afc2d639ce064559bcddd2f7fea1a5ef2020-11-25T01:57:35ZengPublic Library of Science (PLoS)PLoS ONE1932-62032009-01-0143e471010.1371/journal.pone.0004710Meta-analysis and gene set enrichment relative to er status reveal elevated activity of MYC and E2F in the "basal" breast cancer subgroup.M Chehani AllesMargaret Gardiner-GardenDavid J NottYixin WangJohn A FoekensRobert L SutherlandElizabeth A MusgroveChristopher J OrmandyBACKGROUND: Breast cancers lacking the estrogen receptor (ER) can be distinguished from other breast cancers on the basis of poor prognosis, high grade, distinctive histopathology and unique molecular signatures. These features further distinguish estrogen receptor negative (ER-) tumor subtypes, but targeted therapy is currently limited to tumors over-expressing the ErbB2 receptor. METHODOLOGY/PRINCIPAL FINDINGS: To uncover the pathways against which future therapies could be developed we undertook a meta-analysis of gene expression from five large microarray datasets relative to ER status. A measure of association with ER status was calculated for every Affymetrix HG-U133A probe set and the pathways that distinguished ER- tumors were defined by testing for enrichment of biologically defined gene sets using Gene Set Enrichment Analysis (GSEA). As expected, the expression of the direct transcriptional targets of the ER was muted in ER- tumors, but the expression of genes indirectly regulated by estrogen was enhanced. We also observed enrichment of independent MYC- and E2F-driven transcriptional programs. We used a cell model of estrogen and MYC action to define the interaction between estrogen and MYC transcriptional activity in breast cancer. We found that the basal subgroup of ER- breast cancer showed a strong MYC transcriptional response that reproduced the indirect estrogen response seen in estrogen receptor positive (ER+) breast cancer cells. CONCLUSIONS/SIGNIFICANCE: Increased transcriptional activity of MYC is a characteristic of basal breast cancers where it mimics a large part of an estrogen response in the absence of the ER, suggesting a mechanism by which these cancers achieve estrogen-independence and providing a potential therapeutic target for this poor prognosis sub group of breast cancer.http://europepmc.org/articles/PMC2650420?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author M Chehani Alles
Margaret Gardiner-Garden
David J Nott
Yixin Wang
John A Foekens
Robert L Sutherland
Elizabeth A Musgrove
Christopher J Ormandy
spellingShingle M Chehani Alles
Margaret Gardiner-Garden
David J Nott
Yixin Wang
John A Foekens
Robert L Sutherland
Elizabeth A Musgrove
Christopher J Ormandy
Meta-analysis and gene set enrichment relative to er status reveal elevated activity of MYC and E2F in the "basal" breast cancer subgroup.
PLoS ONE
author_facet M Chehani Alles
Margaret Gardiner-Garden
David J Nott
Yixin Wang
John A Foekens
Robert L Sutherland
Elizabeth A Musgrove
Christopher J Ormandy
author_sort M Chehani Alles
title Meta-analysis and gene set enrichment relative to er status reveal elevated activity of MYC and E2F in the "basal" breast cancer subgroup.
title_short Meta-analysis and gene set enrichment relative to er status reveal elevated activity of MYC and E2F in the "basal" breast cancer subgroup.
title_full Meta-analysis and gene set enrichment relative to er status reveal elevated activity of MYC and E2F in the "basal" breast cancer subgroup.
title_fullStr Meta-analysis and gene set enrichment relative to er status reveal elevated activity of MYC and E2F in the "basal" breast cancer subgroup.
title_full_unstemmed Meta-analysis and gene set enrichment relative to er status reveal elevated activity of MYC and E2F in the "basal" breast cancer subgroup.
title_sort meta-analysis and gene set enrichment relative to er status reveal elevated activity of myc and e2f in the "basal" breast cancer subgroup.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2009-01-01
description BACKGROUND: Breast cancers lacking the estrogen receptor (ER) can be distinguished from other breast cancers on the basis of poor prognosis, high grade, distinctive histopathology and unique molecular signatures. These features further distinguish estrogen receptor negative (ER-) tumor subtypes, but targeted therapy is currently limited to tumors over-expressing the ErbB2 receptor. METHODOLOGY/PRINCIPAL FINDINGS: To uncover the pathways against which future therapies could be developed we undertook a meta-analysis of gene expression from five large microarray datasets relative to ER status. A measure of association with ER status was calculated for every Affymetrix HG-U133A probe set and the pathways that distinguished ER- tumors were defined by testing for enrichment of biologically defined gene sets using Gene Set Enrichment Analysis (GSEA). As expected, the expression of the direct transcriptional targets of the ER was muted in ER- tumors, but the expression of genes indirectly regulated by estrogen was enhanced. We also observed enrichment of independent MYC- and E2F-driven transcriptional programs. We used a cell model of estrogen and MYC action to define the interaction between estrogen and MYC transcriptional activity in breast cancer. We found that the basal subgroup of ER- breast cancer showed a strong MYC transcriptional response that reproduced the indirect estrogen response seen in estrogen receptor positive (ER+) breast cancer cells. CONCLUSIONS/SIGNIFICANCE: Increased transcriptional activity of MYC is a characteristic of basal breast cancers where it mimics a large part of an estrogen response in the absence of the ER, suggesting a mechanism by which these cancers achieve estrogen-independence and providing a potential therapeutic target for this poor prognosis sub group of breast cancer.
url http://europepmc.org/articles/PMC2650420?pdf=render
work_keys_str_mv AT mchehanialles metaanalysisandgenesetenrichmentrelativetoerstatusrevealelevatedactivityofmycande2finthebasalbreastcancersubgroup
AT margaretgardinergarden metaanalysisandgenesetenrichmentrelativetoerstatusrevealelevatedactivityofmycande2finthebasalbreastcancersubgroup
AT davidjnott metaanalysisandgenesetenrichmentrelativetoerstatusrevealelevatedactivityofmycande2finthebasalbreastcancersubgroup
AT yixinwang metaanalysisandgenesetenrichmentrelativetoerstatusrevealelevatedactivityofmycande2finthebasalbreastcancersubgroup
AT johnafoekens metaanalysisandgenesetenrichmentrelativetoerstatusrevealelevatedactivityofmycande2finthebasalbreastcancersubgroup
AT robertlsutherland metaanalysisandgenesetenrichmentrelativetoerstatusrevealelevatedactivityofmycande2finthebasalbreastcancersubgroup
AT elizabethamusgrove metaanalysisandgenesetenrichmentrelativetoerstatusrevealelevatedactivityofmycande2finthebasalbreastcancersubgroup
AT christopherjormandy metaanalysisandgenesetenrichmentrelativetoerstatusrevealelevatedactivityofmycande2finthebasalbreastcancersubgroup
_version_ 1724974066948898816

Similar Items