c-Fos oncogene regulator Elk-1 interacts with BRCA1 splice variants BRCA1a/1b and enhances BRCA1a/1b-mediated growth suppression in breast cancer cells

Chai, Yuli; Chipitsyna, Galina; Cui, Jian; Liao, Bo; S, Liu; Aysola, Kartik; Yezdani, M; Es, Reddy; Vn, Rao

doi:10.1038/sj.onc.1204256

Cited by 55 publications

(41 citation statements)

References 56 publications

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“…Others have found BRCA1 to inhibit the growth of a number of cell lines with an Rb-positive and p53-negative background (Aprelikova et al, 1999;Randrianarison et al, 2001). Our earlier results demonstrate that inhibition of expression of endogenous BRCA1 in mouse fibroblast results in transformation and highlevel expression of BRCA1a in breast cancer cells decreases proliferation (Chai et al, 2001) and induces apoptosis . In an attempt to understand whether BRCA1a can function as a growth suppressor similar to BRCA1, we have transfected BRCA1a (pcDNA3-BRCA1a) into a number of cell lines with known status of tumor suppressor genes, such as p53 and pRb.…”

Section: Resultsmentioning

confidence: 99%

BRCA1a has antitumor activity in TN breast, ovarian and prostate cancers

et al. 2007

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Breast cancer gene 1 (BRCA1) mutations predispose women to breast and ovarian cancers and men to increased risks for prostate cancer. We have previously showed BRCA1 splice variant BRCA1a/p110 to induce apoptosis of human breast cancer cells. In the current study, stable expression of BRCA1a/p110 resulted in inhibition of growth of estrogen receptor (ER)-positive and triplenegative (TN) human breast, ovarian, prostate and colon cancer cells and mouse fibroblast cells. Similar to wildtype BRCA1, only those cells with wild-type Rb were sensitive to BRCA1a-induced growth suppression and the status of p53 did not affect the ability of BRCA1a to suppress growth of tumor cells. BRCA1a also significantly inhibited tumor mass in nude mice bearing human CAL-51 TN breast cancer, ES-2 ovarian cancer and PC-3 prostate cancer xenografts. These results suggest that the majority of exon 11 sequences (residues 263-1365) are not required for the tumor suppressor function of BRCA1 proteins. This is the first report demonstrating antitumor activity of BRCA1a in human ER-positive and TN breast, hormoneindependent ovarian and prostate cancer cells. Currently, there are no effective treatments against TN breast cancers and results from these studies will provide new treatments for one of the biggest needs in breast cancer research.

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Section: Resultsmentioning

confidence: 99%

BRCA1a has antitumor activity in TN breast, ovarian and prostate cancers

et al. 2007

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“…Mut. BRCA1 and Trunc.BRCA1, fail to bind to and repress the activity of any of the three transcription factors suggests that the mutated/deleted region contains elements of the binding site(s) for all three transcription factors (32)(33)(34)60).…”

Section: Discussionmentioning

confidence: 99%

“…High level OPN expression may have adverse prognostic significance (6) and may be associated with up-regulation of ER ␣ , AP-1, or Ets factors in sporadic human breast cancers (30). Because BRCA1 protein may bind ER ␣ (12,32), AP-1 (33), and Ets-transcription factors (34), we now investigate the effects of wild type (WT. ), mutated (Mut.…”

Section: Osteopontin (Opn)mentioning

confidence: 99%

BRCA1 Suppresses Osteopontin-mediated Breast Cancer

El‐Tanani

Campbell

Crowe

et al. 2006

Journal of Biological Chemistry

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BRCA1 is a well described breast cancer susceptibility gene thought to be involved primarily in DNA repair. However, mutation within the BRCA1 transcriptional domain is also implicated in neoplastic transformation of mammary epithelium, but responsible mechanisms are unclear. Here we show in a rat mammary model system that wild type (WT) BRCA1 specifically represses the expression of osteopontin (OPN), a multifunctional estrogen-responsive gene implicated in oncogenic transformation, particularly that of the breast. WT.BRCA1 selectively binds OPN-activating transcription factors estrogen receptor ␣, AP-1, and PEA3, inhibits OPN promoter transactivation, and suppresses OPN mRNA and protein both from an endogenous gene and a relevant model inducible gene. WT.BRCA1 also inhibits OPN-mediated neoplastic transformation characterized by morphology change, anchorage-independent growth, adhesion to fibronectin, and invasion through Matrigel. A mutant BRCA1 allele (Mut.BRCA1) associated with familial breast cancer lacks OPN suppressor effects, binds to WT.BRCA1, and impedes WT.BRCA1 suppression of OPN. Stable transfection of rat breast tumor cell lines with Mut.BRCA1 dramatically up-regulates OPN protein and induces anchorageindependent growth. In human primary breast cancer, BRCA1 mutation is significantly associated with OPN overexpression. Taken together, these data suggest that BRCA1 mutation may confer increased tissue-specific cancer risk, in part by disruption of BRCA1 suppression of OPN gene transcription.

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“…The BRCA1 splice variants BRCA1a and BRCA1b-which suppress the growth of breast cancer cellsinteract with Elk-1, an Ets-domain transcription factor that participates in the induction of immediate early gene expression (Chai et al, 2001). Over-expression of BRCA1a/b inhibited the expression of Elk-1 target genes, such as c-Fos, suggesting a mechanism of growth inhibition.…”

Section: Regulation Of Transcriptionmentioning

confidence: 99%

BRCA1 gene in breast cancer

Rosen

Fan

Pestell

et al. 2003

Journal Cellular Physiology

233

189

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The BRCA1 gene was identified and cloned in 1994 based on its linkage to early onset breast cancer and breast-ovarian cancer syndromes in women. While inherited mutations of BRCA1 are responsible for about 40-45% of hereditary breast cancers, these mutations account for only 2-3% of all breast cancers, since the BRCA1 gene is rarely mutated in sporadic breast cancers. However, BRCA1 expression is frequently reduced or absent in sporadic cancers, suggesting a much wider role in mammary carcinogenesis. Since BRCA1 was cloned in 1994, its molecular function has been the subject of intense investigation. These studies have revealed multiple functions of the BRCA1 that may contribute to its tumor suppressor activity, including roles in: cell cycle progression, several highly specialized DNA repair processes, DNA damage-responsive cell cycle checkpoints, regulation of a set of specific transcriptional pathways, and apoptosis. Many of these functions are linked to protein:protein interactions involving different portions of the 1,863 amino acid (aa) BRCA1 protein. BRCA1 functions in cell cycle progression and the DNA damage response appear to be regulated by distinct and specific phosphorylation events, but the molecular pathways activated by these phosphorylations are only beginning to be unraveled. In addition, the reason that BRCA1 mutation carriers develop specific tumor types (breast and ovarian cancers in women and possibly prostate cancers in men) is not clearly understood. Elucidation of the precise molecular functions of the BRCA1 gene product will greatly enhance our understanding of the pathogenesis of hereditary as well as sporadic mammary carcinogenesis.

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c-Fos oncogene regulator Elk-1 interacts with BRCA1 splice variants BRCA1a/1b and enhances BRCA1a/1b-mediated growth suppression in breast cancer cells

Cited by 55 publications

References 56 publications

BRCA1a has antitumor activity in TN breast, ovarian and prostate cancers

BRCA1a has antitumor activity in TN breast, ovarian and prostate cancers

BRCA1 Suppresses Osteopontin-mediated Breast Cancer

BRCA1 gene in breast cancer

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