DNA methylation inhibits p53-mediated survivin repression

Nabilsi, Nancy H.; Broaddus, Russell R.; Loose, David S.

doi:10.1038/onc.2009.62

Cited by 87 publications

(77 citation statements)

References 29 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In a previous study, we observed p53-dependent repression of NEK2 following treatment with 5aza-dC (8). Here, we report that NEK2 is repressed by wild-type p53 and that loss of p53 results in local accumulation of DNA methylation.…”

supporting

confidence: 51%

“…Additional RT-qPCR primer sequences are listed in supplemental Table 1. The assays were performed at the Quantitative Genomics Core Laboratory (University of TexasHouston Medical School) using a 7700 Sequence Detector (Applied Biosystems) as described previously (8). Transcripts were quantified using the ⌬⌬Ct method, normalizing to 18 S rRNA or ␤-actin mRNA.…”

Section: Methodsmentioning

confidence: 99%

See 1 more Smart Citation

Local Depletion of DNA Methylation Identifies a Repressive p53 Regulatory Region in the NEK2 Promoter

Nabilsi

Ryder

Peraza-Penton

et al. 2013

Journal of Biological Chemistry

View full text Add to dashboard Cite

Background: NEK2 is a mammalian kinase that promotes centrosome separation during the cell cycle. Results: Agents that demethylate the NEK2 promoter or induce DNA damage repress NEK2 expression in a p53-dependent manner. Conclusion: p53 represses NEK2 expression and protects its binding region from accumulating DNA methylation. Significance: Knowledge regarding novel mechanisms of NEK2 regulation may help inform clinical application of NEK2-based anticancer therapeutics.

show abstract

supporting

confidence: 51%

Section: Methodsmentioning

confidence: 99%

Local Depletion of DNA Methylation Identifies a Repressive p53 Regulatory Region in the NEK2 Promoter

Nabilsi

Ryder

Peraza-Penton

et al. 2013

Journal of Biological Chemistry

View full text Add to dashboard Cite

show abstract

“…[22][23][24] Such a mechanism of de-repression as a result of epigenetic regulation by DNA methylation has recently been shown for survivin. 51 In this study, methylation of survivin promoter inhibits the binding of p53, a repressor of its expression. In keeping, earlier studies showed that methylation of the hTERT promoter at the CTCF-binding site inhibited the binding of CTCF, thus derepressing hTERT in some human tumors.…”

Section: Discussionmentioning

confidence: 76%

Epigenetic plasticity of hTERT gene promoter determines retinoid capacity to repress telomerase in maturation-resistant acute promyelocytic leukemia cells

Azouz

Hillion

et al. 2010

Leukemia

View full text Add to dashboard Cite

The expression of hTERT gene, encoding the catalytic subunit of telomerase, is a feature of most cancer cells. Changes in the chromatin environment of its promoter and binding of transcriptional factors have been reported in differentiating cells when its transcription is repressed. However, it is not clear whether these changes are directly involved in this repression or only linked to differentiation. In a maturation-resistant acute promyelocytic leukemia (APL) cell line (NB4-LR1), we have previously identified a new pathway of retinoid-induced hTERT repression independent of differentiation. Using a variant of this cell line (NB4-LR1 SFD ), which resists to this repression, we show that although distinct patterns of histone modifications and transcription factor binding at the proximal domain of hTERT gene promoter could concur to modulate its expression, this region is not sufficient to the on/off switch of hTERT by retinoids. DNA methylation analysis of the hTERT promoter led to the identification of two distinct functional domains, a proximal one, fully unmethylated in both cell lines, and a distal one, significantly methylated in NB4-LR1 SFD cells, whose methylation was further re-enforced by retinoid treatment. Interestingly, we showed that the binding to this distal domain of a known hTERT repressor, WT1, was defective only in NB4-LR1 SFD cells. We propose that epigenetic modifications targeting this distal region could modulate the binding of hTERT repressors and account either for hTERT reactivation and resistance to retinoid-induced hTERT downregulation.

show abstract

“…This in vivo binding preference is supported by a recent study which showed that in endometrial tumor samples, CGI promoter methylation at survivin/BIRC5 prevented p53 from binding. 66 Cancer development is known to be associated with substantial epigenetic changes, DNA hypomethylation on in IMR90, their distributions remain clearly different from the cancer data sets (Fig. S8).…”

Section: Resultsmentioning

confidence: 92%