FOXA1 represses the molecular phenotype of basal breast cancer cells

Bernardo, Gina M.; Bebek, Gürkan; Ginther, Charles; Sizemore, Steven T.; Lozada, Kristen L.; Miedler, John D.; Anderson, Lee; Godwin, Andrew K.; Abdul‐Karim, Fadi W.; Slamon, Dennis J.; Keri, Ruth A.

doi:10.1038/onc.2012.62

Cited by 135 publications

(151 citation statements)

References 54 publications

(102 reference statements)

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“…5C). Although we and others have observed subtype plasticity in breast cancer cell lines following alterations in subtype-specifying genes (29,36), the decrease in the basal-like cytokeratins with GABRP knockdown was not accompanied with an up-regulation of KRT19, a luminal-specific cytokeratin (Fig. 5, B and C).…”

Section: Gabrp Correlates With the Blbc Subtype And Decreasedmentioning

confidence: 99%

“…Migration-Migration assays were performed as described (29). Briefly, 50,000 viable cells, as determined by trypan blue exclusion, were seeded into the top of uncoated 24-well transwell inserts (Corning) in either serum-free RPMI media (HCC70) or RPMI media containing 1% FBS (HCC1187).…”

Section: Methodsmentioning

confidence: 99%

“…Quantitative Real-time PCR-RNA processing, DNase I treatment and reverse transcription was performed as described (29). Applied Biosystems TaqMan Gene Expression Assays included: GAPDH, Hs99999905_m1; GABRP, Hs00959454_m1; KRT5, Hs00361185_m1; KRT6B, Hs00745492_s1; KRT14, Hs00559328_m1; KRT17, Hs00356958_m1; KRT19, Hs00761767_ s1.…”

Section: Methodsmentioning

confidence: 99%

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GABA(A) Receptor Pi (GABRP) Stimulates Basal-like Breast Cancer Cell Migration through Activation of Extracellular-regulated Kinase 1/2 (ERK1/2)

Sizemore

Seachrist

et al. 2014

Journal of Biological Chemistry

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Background: GABRP correlates with the basal-like breast cancer (BLBC)/triple negative subtype, but its function in this disease is poorly understood. Results: Silencing GABRP in BLBC cells decreases migration, BLBC-associated cytokeratins and ERK1/2 activation. Conclusion: A GABRP-ERK1/2-cytokeratin axis maintains BLBC migration. Significance: GABRP is a component of a cell-surface receptor, thus, targeting this signaling axis may have therapeutic potential in BLBC.

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Section: Gabrp Correlates With the Blbc Subtype And Decreasedmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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GABA(A) Receptor Pi (GABRP) Stimulates Basal-like Breast Cancer Cell Migration through Activation of Extracellular-regulated Kinase 1/2 (ERK1/2)

Sizemore

Seachrist

et al. 2014

Journal of Biological Chemistry

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“…Both FOXA1 and FOXA2 are pioneer transcription factors with essential roles in the development of and estrogen signaling in the liver (43). In breast cancer cells, FOXA factors and ESR1 are frequently bound to adjacent cis-regulatory elements in the genome, and recruitment of ESR1 to those binding sites is dependent on FOXA factors (42,44). Of note, the majority of uterine gland-specific genes (Cxcl15, Prss29, Spink3, Ttr, and Wfdc3) studied here are bound by FOXA2 in ChIP sequencing (ChIP-seq) analyses of GD 3.5 mouse uteri (18).…”

Section: On Gd 35 Induces the Expression Of Lif In The Glands Of Thementioning

confidence: 99%

Forkhead box a2 (FOXA2) is essential for uterine function and fertility

Kelleher

Wang

Pru

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

126

177

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Establishment of pregnancy is a critical event, and failure of embryo implantation and stromal decidualization in the uterus contribute to significant numbers of pregnancy losses in women. Glands of the uterus are essential for establishment of pregnancy in mice and likely in humans. Forkhead box a2 (FOXA2) is a transcription factor expressed specifically in the glands of the uterus and is a critical regulator of postnatal uterine gland differentiation in mice. In this study, we conditionally deleted FOXA2 in the adult mouse uterus using the lactotransferrin Cre (Ltf-Cre) model and in the neonatal mouse uterus using the progesterone receptor Cre (Pgr-Cre) model. The uteri of adult FOXA2-deleted mice were morphologically normal and contained glands, whereas the uteri of neonatal FOXA2-deleted mice were completely aglandular. Notably, adult FOXA2-deleted mice are completely infertile because of defects in blastocyst implantation and stromal cell decidualization. Leukemia inhibitory factor (LIF), a critical implantation factor of uterine gland origin, was not expressed during early pregnancy in adult FOXA2-deleted mice. Intriguingly, i.p. injections of LIF initiated blastocyst implantation in the uteri of both gland-containing and glandless adult FOXA2-deleted mice. Although pregnancy was rescued by LIF and was maintained to term in uterine gland-containing adult FOXA2-deleted mice, pregnancy failed by day 10 in neonatal FOXA2-deleted mice lacking uterine glands. These studies reveal a previously unrecognized role for FOXA2 in regulation of adult uterine function and fertility and provide original evidence that uterine glands and, by inference, their secretions play important roles in blastocyst implantation and stromal cell decidualization.T he uterus is comprised of two tissue compartments, the endometrium and the myometrium. The endometrium contains three cell types, luminal epithelium (LE), glandular epithelium (GE), and stroma. In mice, the uterus becomes receptive to blastocyst implantation on gestational day (GD) 4 (with the observation of a postcoital vaginal plug designated GD 0.5); it is prereceptive on GD 1-3, and by the afternoon of GD 5 it becomes nonreceptive (refractory) (1-3). Dynamic changes in ovarian estrogen and progesterone production act via the uterus to regulate uterine receptivity, blastocyst implantation, and stromal cell decidualization necessary for the establishment of pregnancy (4-6). The implantation process, which is initiated by the attachment of the blastocyst trophectoderm to the receptive LE, occurs before or right after midnight in the evening of GD 4 and becomes more prominent by the morning of GD 5. By GD 6, the trophectoderm begins to contact directly stromal cells that then begin to differentiate into decidual cells, which are required for successful pregnancy because they regulate placental development and local maternal immune responses (7,8).The infertility observed in leukemia inhibitory factor (Lif)-null mice and uterine gland-knockout (UGKO) mice and sheep established ...

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“…As expected, we identified the estrogen receptor (ESR1), which is the most relevant marker for breast cancer subtyping in histochemistry, as one of the top features. The other top features are FOXA1, which has been identified as a tumor suppressor [19] and MLPH, which is not known to be associated with breast cancer, but has an experimentally verified interaction to RAB27A, which was shown to promote proliferation in human glioma cells [20]. Furthermore, we identified FOXC1 as a top feature, which is of the same family of transcription factors as FOXA1 and which was shown to play a role in NF-κB signaling in basal breast cancer cells [21].…”

Section: Analysis Of Misclassification By the Control Modelmentioning

confidence: 99%

Classification of Breast Cancer Subtypes by combining Gene Expression and DNA Methylation Data

List

Hauschild

Tan

et al. 2014

Journal of Integrative Bioinformatics

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SummarySelecting the most promising treatment strategy for breast cancer crucially depends on determining the correct subtype. In recent years, gene expression profiling has been investigated as an alternative to histochemical methods. Since databases like TCGA provide easy and unrestricted access to gene expression data for hundreds of patients, the challenge is to extract a minimal optimal set of genes with good prognostic properties from a large bulk of genes making a moderate contribution to classification. Several studies have successfully applied machine learning algorithms to solve this so-called gene selection problem. However, more diverse data from other OMICS technologies are available, including methylation. We hypothesize that combining methylation and gene expression data could already lead to a largely improved classification model, since the resulting model will reflect differences not only on the transcriptomic, but also on an epigenetic level. We compared so-called random forest derived classification models based on gene expression and methylation data alone, to a model based on the combined features and to a model based on the gold standard PAM50. We obtained bootstrap errors of 10-20% and classification error of 1-50%, depending on breast cancer subtype and model. The gene expression model was clearly superior to the methylation model, which was also reflected in the combined model, which mainly selected features from gene expression data. However, the methylation model was able to identify unique features not considered as relevant by the gene expression model, which might provide deeper insights into breast cancer subtype differentiation on an epigenetic level.

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FOXA1 represses the molecular phenotype of basal breast cancer cells

Cited by 135 publications

References 54 publications

GABA(A) Receptor Pi (GABRP) Stimulates Basal-like Breast Cancer Cell Migration through Activation of Extracellular-regulated Kinase 1/2 (ERK1/2)

GABA(A) Receptor Pi (GABRP) Stimulates Basal-like Breast Cancer Cell Migration through Activation of Extracellular-regulated Kinase 1/2 (ERK1/2)

Forkhead box a2 (FOXA2) is essential for uterine function and fertility

Classification of Breast Cancer Subtypes by combining Gene Expression and DNA Methylation Data

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