BRCA1 transcriptionally regulates genes involved in breast tumorigenesis

Welcsh, Piri; Lee, Ming K.; Gonzalez-Hernandez, Rachel M.; Black, Daniel J.; Mahadevappa, M.; Swisher, Elizabeth M.; Warrington, Janet A.; King, Mary Claire

doi:10.1073/pnas.062181799

Cited by 225 publications

(185 citation statements)

References 59 publications

(61 reference statements)

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“…Previous research has shown that BRCA1 protein increases arrest in the cell cycle progression of cells [24]. In addition, BRCA1 protein is reported to indicate the positively regulated expression of CCND1 [25], PCNA [26], NEK2 [27] and MAD2L1 [28]. In the present cell system, cell cycle-related genes, especially those participating in this genetic network (Fig.…”

Section: Discussionsupporting

confidence: 52%

Genetic networks responsive to sodium butyrate in colonic epithelial cells

et al. 2006

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We performed microarray and computational gene network analyses to identify the detailed mechanisms by which sodium butyrate (SB) induces cell growth arrest and the differentiation of mouse colonic epithelial MCE301 cells. Two thousand six hundred four differentially expressed probe sets were identified in the cells treated with 2 mM SB and were classified into four groups. Of these, the gradually increased group and the gradually and remarkably decreased group contained the genetic networks for cellular development and cell cycles or canonical pathways for fatty acid biosynthesis and pyrimidine metabolism, respectively. The present results provide a basis for understanding the detailed molecular mechanisms of action of SB in colonic epithelial cells.

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Section: Discussionsupporting

confidence: 52%

Genetic networks responsive to sodium butyrate in colonic epithelial cells

et al. 2006

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“…32,82,83 BRCA1 gene promoter is methylated in 460% of medullary 95,96 and metaplastic 32 breast cancers of basal-like phenotype. Sporadic invasive ductal carcinomas with basal-like phenotype express ID4, a negative regulator of BRCA1, 97,98 at significantly higher levels than grade-matched controls. 32 This mechanism may account for the low levels of BRCA1 expression in sporadic basal-like carcinomas of ductal morphology.…”

Section: S Badve Et Almentioning

confidence: 94%

Basal-like and triple-negative breast cancers: a critical review with an emphasis on the implications for pathologists and oncologists

et al. 2011

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Breast cancer is a heterogeneous disease encompassing a variety of entities with distinct morphological features and clinical behaviors. Although morphology is often associated with the pattern of molecular aberrations in breast cancers, it is also clear that tumors of the same histological type show remarkably different clinical behavior. This is particularly true for 'basal-like cancer', which is an entity defined using gene expression analysis. The purpose of this article was to review the current state of knowledge of basal-like breast cancers, to discuss the relationship between basal-like and triple-negative breast cancers, and to clarify practical implications of these diagnoses for pathologists and oncologists.

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“…In that study, and in a study by Bouras et al (2002), high levels of STC1 expression were found to be associated with estrogen receptor positivity, which is a marker of good prognosis. Furthermore, the tumor suppressors BRCA1 and p53 have both been reported to upregulate STC1 gene expression (Welcsh et al, 2002;Lai et al, 2007). Continued expression of these genes in cancers is usually associated with good prognosis, and this may be explained in part by STC1 acting as a downstream mediator of apoptosis.…”

Section: Regulation Of Oxidative Stress Response By Stc1mentioning

confidence: 99%

“…A number of studies, mostly correlative, of mammalian STC1 mRNA and protein expression have ascribed roles to STC1 ranging from angiogenesis (Kahn et al, 2000;Bell et al, 2001), bone and muscle development (Jiang et al, 2000;Filvaroff et al, 2002;Varghese et al, 2002;Yoshiko et al, 2003), inflammation (Iyer et al, 1999;Kanellis et al, 2003), cellular metabolism (McCudden et al, 2002;Ellard et al, 2007) and cancer (Fujiwara et al, 2000;Ismail et al, 2000;Okabe et al, 2001;Welcsh et al, 2002). Establishing the functional importance and relevance of these putative functions has proved difficult; moreover, STC1-null mice housed in standard laboratory conditions have no obvious phenotype (Chang et al, 2005).…”

Section: Introductionmentioning

confidence: 99%

“…In an in vitro model of wound healing, STC1 expression was found to be rapidly upregulated following provision of serum to serum-starved human fibroblasts (Iyer et al, 1999). Furthermore, STC1 is regulated by the tumor suppressors BRCA1 (Welcsh et al, 2002) and p53 (Lai et al, 2007), both of which play key roles in orchestrating DNA repair and growth arrest, or apoptosis, in response to various cellular stresses.…”

Section: Introductionmentioning

confidence: 99%

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Stanniocalcin-1 acts in a negative feedback loop in the prosurvival ERK1/2 signaling pathway during oxidative stress

2009

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Mammalian Stanniocalcin-1 (STC1) is a glycoprotein that has been implicated in various biological processes including angiogenesis. Aberrant STC1 expression has been reported in breast, ovarian and prostate cancers, but the significance of this is not well understood. Here, we report that oxidative stress caused a 40-fold increase in STC1 levels in mouse embryo fibroblasts (MEFs). STC1À/À MEFs were resistant to growth inhibition and cell death induced by H 2 O 2 or by 20% O 2 (which is hyperoxic for most mammalian cells); this is the first phenotype reported for STC1-null cells. STC1À/À cells had higher levels of activated MEK and ERK1/2 than their wild-type (WT) counterparts, and these levels were all reduced by stable expression of exogenous STC1 in STC1À/À cells. Furthermore, pharmacological inhibition by PD98059 or UO126 of MEK and therefore of ERK1/2 activation restored sensitivity of STC1À/À cells to oxidative stress. We also found that H 2 O 2 -induced STC1 expression in WT cells was abolished by inhibition of ERK1/2 activation. Thus, the ERK1/2 signaling pathway upregulates STC1 expression, which in turn downregulates the level of activated MEK and consequently ERK1/2 in a novel negative feedback loop. Therefore, STC1 expression downregulates prosurvival ERK1/2 signaling and reduces survival under conditions of oxidative stress.

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BRCA1 transcriptionally regulates genes involved in breast tumorigenesis

Cited by 225 publications

References 59 publications

Genetic networks responsive to sodium butyrate in colonic epithelial cells

Genetic networks responsive to sodium butyrate in colonic epithelial cells

Basal-like and triple-negative breast cancers: a critical review with an emphasis on the implications for pathologists and oncologists

Stanniocalcin-1 acts in a negative feedback loop in the prosurvival ERK1/2 signaling pathway during oxidative stress

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