Nuclear Localization of KLF4 Is Associated with an Aggressive Phenotype in Early-Stage Breast Cancer

Pandya, Ashka Y.; Talley, Lynya; Frost, Andra R.; Fitzgerald, Thomas J.; Trivedi, Vivek; Chakravarthy, Mithun; Chhieng, David C.; Grizzle, William E.; Engler, Jeffrey A.; Krontiras, Helen; Bland, Kirby I.; LoBuglio, Albert F.; Lobo-Ruppert, Susan M.; Ruppert, J. Michael

doi:10.1158/1078-0432.ccr-03-0484

Cited by 185 publications

(189 citation statements)

References 45 publications

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“…Representative results of two independent data sets characterized by large population sizes (Miller et al, 2005;Ivshina et al, 2006;Richardson et al, 2006;Finak et al, 2008) are shown in Figure 1a (KLF4 expression levels in normal versus breast carcinoma; P ¼ 5.4EÀ4, 7.0EÀ3) and 1b (KLF4 expression levels in breast cancers classified by grade; P ¼ 8.0EÀ11, 2.6EÀ10). Earlier reports have shown that 70% of breast carcinomas have elevated KLF4 expression and that increased nuclear staining for KLF4 is associated with a more aggressive phenotype (Foster et al, 2000;Pandya et al, 2004). Inconsistencies between the results obtained from the Oncomine database and earlier reports may be due to the genetic or epigenetic context of breast cancer tissues.…”

Section: Resultsmentioning

confidence: 94%

KLF4 suppresses estrogen-dependent breast cancer growth by inhibiting the transcriptional activity of ERα

et al. 2009

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Kruppel-like factor 4 (KLF4) is a transcription factor that participates in both tumor suppression and oncogenesis. To determine the association of KLF4 with tumorigenesis, we integrated data assembled in the Oncomine database and discovered a decrease in KLF4 gene transcripts in breast cancers. Further analysis of the database also showed a correlation between KLF4 expression and estrogen receptor-a (ERa) positivity. Knockdown of KLF4 in MCF-7 cells elevated the growth rate of these cells in the presence of estrogen. Therefore, we examined the interaction between KLF4 and ERa, and found that KLF4 bound to the DNA-binding region of ERa. KLF4 thus inhibits the binding of ERa to estrogen response elements in promoter regions, resulting in a reduction in ERa target gene transcription. Earlier studies have reported that KLF4 is transcriptionally activated by p53 following DNA damage. We also showed that activation of p53 decreased the transcriptional activity of ERa by elevating KLF4 expression. Our studies discovered a novel molecular network between p53, KLF4 and ERa. As both p53 and ERa are involved in cell growth and apoptosis, these results may explain why KLF4 possesses both tumor suppressive and oncogenic functions in breast cancers.

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Section: Resultsmentioning

confidence: 94%

KLF4 suppresses estrogen-dependent breast cancer growth by inhibiting the transcriptional activity of ERα

et al. 2009

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“…KLF4 overexpression becomes evident at the stage of ductal carcinoma in situ, indicating that, similar to squamous cell carcinoma, this represents an early event in breast cancer progression 59 . Furthermore, nuclear localization of KLF4 was found to be a predictor of poor outcome of breast cancer 60 . In contrast to many other cancer types, TP53 is often not mutated in sporadic breast cancer.…”

Section: Klf4 As An Oncogenementioning

confidence: 98%

KLF4, p21 and context-dependent opposing forces in cancer

2005

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| Krüppel-like factors are transcriptional regulators that influence several cellular functions, including proliferation. Recent studies have shown that one family member, KLF4, can function both as a tumour suppressor and an oncogene. The ability of KLF4 to affect the levels of expression of the cell-cycle regulator p21 seems to be involved, in that this protein might function as a switch that determines the outcome of KLF4 signalling. Is this role of p21 restricted to KLF4, or does p21 represent a nodal point for signals from multiple other factors with opposing functions in cancer?

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“…Current studies in carcinogen-esis have revealed that KLF4 can function as both tumor promoter and tumor suppressor depending on tissue type and cellular context [241]. The oncogenic effect of KLF4 has been reported in breast and squamous cell carcinoma [243][244][245][246][247], while its tumor suppression role was reported in various types of cancers such as colon cancer [248,249]. It was demonstrated that KLF4 is a fast turnover protein, whose turnover-half life is governed by the ubiquitin-proteasome system [250,251].…”

Section: Crosstalk With Tgf-β Signalingmentioning

confidence: 99%

RETRACTED ARTICLE: Regulation of estrogen receptor signaling in breast carcinogenesis and breast cancer therapy

Zhou

Qiao

Shetty

et al. 2013

Cell. Mol. Life Sci.

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Estrogen and estrogen receptors (ERs) are critical regulators of breast epithelial cell proliferation, differentiation, and apoptosis. Compromised signaling vis-à-vis the estrogen receptor is believed © Springer Basel 2013 yow4@pitt.edu. ), which predicts for response to endocrine-based therapy; however, innate or acquired resistance to endocrinebased drugs remains a serious challenge. The complexity of regulation for estrogen signaling coupled with the crosstalk of other oncogenic signaling pathways is a reason for endocrine therapy resistance. Alternative strategies that target novel molecular mechanisms are necessary to overcome this current and urgent gap in therapy. A thorough analysis of estrogen-signaling regulation is critical. In this review article, we will summarize current insights into the regulation of estrogen signaling as related to breast carcinogenesis and breast cancer therapy. NIH Public Access

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Nuclear Localization of KLF4 Is Associated with an Aggressive Phenotype in Early-Stage Breast Cancer

Cited by 185 publications

References 45 publications

KLF4 suppresses estrogen-dependent breast cancer growth by inhibiting the transcriptional activity of ERα

KLF4 suppresses estrogen-dependent breast cancer growth by inhibiting the transcriptional activity of ERα

KLF4, p21 and context-dependent opposing forces in cancer

RETRACTED ARTICLE: Regulation of estrogen receptor signaling in breast carcinogenesis and breast cancer therapy

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