Clinical Relevance of E2F Family Members in Ovarian Cancer—An Evaluation in a Training Set of 77 Patients

Reimer, Daniel; Sadr, Susann; Wiedemair, Annemarie; Stadlmann, Sylvia; Concin, Nicole; Hofstetter, Gerda; Müller‐Holzner, Elisabeth; Marth, Christian; Zeimet, Alain G.

doi:10.1158/1078-0432.ccr-06-0780

Cited by 97 publications

(90 citation statements)

References 29 publications

(22 reference statements)

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“…In keeping with the results obtained from ovarian cancer cell lines and primary cultured healthy ovarian surface epithelial and mesothelial cells, both E2F3a and E2F3b were found to be overexpressed in ovarian cancers as compared with normal ovarian tissue. These findings are in agreement with earlier data showing both proliferation-promoting and -inhibiting E2F family members to be overexpressed in ovarian cancer specimens (Reimer et al, 2007). Nevertheless, E2F3a expression by far exceeded that of E2F3b in the cancer tissues.…”

Section: Discussionsupporting

confidence: 93%

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Regulation of transcription factor E2F3a and its clinical relevance in ovarian cancer

et al. 2011

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Recently we showed an integral epidermal growth factor receptor (EGFR)-E2F3a signaling path, in which E2F3a was found to be essential in EGFR-mediated proliferation in ovarian cancer cells. The present work evaluates the clinical relevance of this novel axis and of E2F3a itself in a large set of 130 ovarian cancer specimens. For this purpose E2F3a and its counterpart, E2F3b, were measured by RT-PCR and activated EGFR was assessed by immunohistochemistry. When compared with healthy control tissue, both E2F3 isoforms were overexpressed in the cancers, but only E2F3a expression correlated with tumor stage (q ¼ 0.349, P ¼ 0.0001) and residual disease (q ¼ 0.254, P ¼ 0.004). Univariate survival analyses showed E2F3a and activated EGFR to be associated with poor PFS and OS. Furthermore, a strong, positive correlation between activated EGFR and E2F3a expression was shown (P ¼ 0.0001). We further identified two EGFR-independent mechanisms that regulate E2F3a expression, namely one, acting by promoter methylation of miR-34a, which by its physical interaction with E2F3a transcripts causes their degradation, and the second based on 6p22 gene locus amplification. MiRIDIAN-based knockdown and induction of miR-34a evidenced a direct regulatory link between miR-34a and E2F3a, and the tumor-suppressive character of miR-34a was documented by its association with improved survival. Although, 6p22 gene locus amplification was detected in a significant number of ovarian cancer specimens, 6p22 ploidy was not relevant in predicting survival. In Cox regression analysis, E2F3a, but not activated EGFR or miR-34a expression, retained independent prognostic significance (PFS: hazards ratio 3.785 (1.326-9.840), P ¼ 0.013; OS: hazards ratio 4.651 (1.189-15.572), P ¼ 0.013). These clinical findings highlight the relevance of E2F3a in the biology of ovarian cancer. Moreover, identification of EGFR-independent mechanisms in E2F3a control can be helpful in explaining the non-responsiveness of therapeutic EGFR targeting in ovarian cancer.

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Section: Discussionsupporting

confidence: 93%

“…Total RNA extraction and real-time PCR amplification Total RNA extraction from cell lines or patient samples, DNAse treatment and reverse transcription were performed as previously described by Reimer et al (2007). RT-PCRs were performed using an ABI Prism 7900 Detection System as described previously by Reimer et al (2010).…”

Section: Patientsmentioning

confidence: 99%

Regulation of transcription factor E2F3a and its clinical relevance in ovarian cancer

et al. 2011

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“…Interestingly, the genetics of pancreatic cancer suggest that this is a setting where oncogene-induced senescence restricts tumorigenesis, as activating KRAS mutations frequently co-occur with mutations targeting the INK4A/ ARF locus or p53 in later stages of the disease. Underexpression of E2F7 is also associated with platinum resistance and reduced survival in ovarian cancer patients (Reimer et al 2007). Still, somatic mutations in E2F7 have yet to be described, raising the possibility that its activity is not rate-limiting for tumorigenesis.…”

Section: Discussionmentioning

confidence: 99%

The atypical E2F family member E2F7 couples the p53 and RB pathways during cellular senescence

Aksoy

Chicas²,

Zeng³

et al. 2012

Genes Dev.

110

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Oncogene-induced senescence is an anti-proliferative stress response program that acts as a fail-safe mechanism to limit oncogenic transformation and is regulated by the retinoblastoma protein (RB) and p53 tumor suppressor pathways. We identify the atypical E2F family member E2F7 as the only E2F transcription factor potently upregulated during oncogene-induced senescence, a setting where it acts in response to p53 as a direct transcriptional target. Once induced, E2F7 binds and represses a series of E2F target genes and cooperates with RB to efficiently promote cell cycle arrest and limit oncogenic transformation. Disruption of RB triggers a further increase in E2F7, which induces a second cell cycle checkpoint that prevents unconstrained cell division despite aberrant DNA replication. Mechanistically, E2F7 compensates for the loss of RB in repressing mitotic E2F target genes. Together, our results identify a causal role for E2F7 in cellular senescence and uncover a novel link between the RB and p53 pathways.

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“…Interestingly, gene expression signatures of platinum-resistant advanced stage ovarian cancers revealed activation of E2F3 pathways, and the targeting of E2F pathways with roscovitine could be exploited for improved response to chemotherapy in vitro (Dressman et al, 2007). Additionally, high levels of activating relative to repressing E2Fs have recently been shown to be clinical predictors of poor response to chemotherapy in ovarian cancer patients (Reimer et al, 2007). Future analyses of the relative contribution of FA upregulation to E2F-dependent chemotherapy resistance in cancer patients will be important for an assessment of possible treatment implications.…”

Section: Discussionmentioning

confidence: 99%

Coordinate regulation of Fanconi anemia gene expression occurs through the Rb/E2F pathway

et al. 2008

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Fanconi anemia (FA) is a genome instability syndrome that is characterized by progressive bone marrow failure and a high risk of cancer. FA patients are particularly susceptible to leukemia as well as squamous cell carcinomas (SCCs) of the head and neck, anogenital region and skin. Thirteen complementation groups and the corresponding FA genes have been identified, and their protein products assemble into nuclear core complexes during DNA-damage responses. Much progress has been made in our understanding of post-translational FA protein modifications and physical interactions. By contrast, little is known about the control of protein availability at the level of transcription. We report here that multiple FA proteins were downregulated during the proliferative arrest of primary human keratinocytes and HeLa cells, and that the observed regulation was at a transcriptional level. Proliferative stimuli such as expression of HPV16 E7 as well as E2F1 overexpression in primary cells resulted in coordinate FA upregulation. To define the underlying mechanism, we examined the endogenous FANCD2 promoter, and detected regulated binding of members of the E2F/Rb family in chromatin immunoprecipitation assays. Finally, a 1 kb promoter fragment was sufficient to confer E2F/Rb regulation in reporter assays. Taken together, our data demonstrate FA gene co-regulation in synchrony with the cell cycle and suggest that deregulated expression of individual FA genes-in addition to FA gene mutation-may promote FA-related human cancer.

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Clinical Relevance of E2F Family Members in Ovarian Cancer—An Evaluation in a Training Set of 77 Patients

Cited by 97 publications

References 29 publications

Regulation of transcription factor E2F3a and its clinical relevance in ovarian cancer

Regulation of transcription factor E2F3a and its clinical relevance in ovarian cancer

The atypical E2F family member E2F7 couples the p53 and RB pathways during cellular senescence

Coordinate regulation of Fanconi anemia gene expression occurs through the Rb/E2F pathway

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