Re-activation of a dormant tumor suppressor gene maspin by designed transcription factors

Beltran, Adriana S.; Parikh, Shaunak; Liu, Y; Cuevas, Bruce D.; Johnson, Gary L.; Futscher, Bernard W.; Blancafort, Pilar

doi:10.1038/sj.onc.1210072

Cited by 89 publications

(102 citation statements)

References 41 publications

(46 reference statements)

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“…The identified transcription factor binding sites in this region experimentally elucidated by previous studies include the sequences in the negative regulator site HRE and the positive regulator binding sites, ETS, AP1, ATF-126 and ATF-2 sites (Maekawa et al, 2007;Zhang et al, 1997 a and b;Beltran et al, 2007). These sites are 60-83% identical with human suggesting these transcription factors may be active across the different species (Fig 9B).…”

Section: Discussionmentioning

confidence: 74%

Epigenetic silencing of maspin expression occurs early in the conversion of keratocytes to fibroblasts

Horswill

Narayan

Warejcka

et al. 2008

Experimental Eye Research

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Maspin, a 42 kDa non-classical serpin (serine protease inhibitor) that controls cell migration and invasion, is mainly expressed by epithelial-derived cells but is also expressed in corneal stromal keratocytes. Upon culture of stromal keratocytes in the presence of FBS, maspin is down regulated to nearly undetectable levels by passage two. DNA methylation is one of several processes that controls gene expression during cell differentiation, development, genetic imprinting, and carcinogenesis but has not been studied in corneal stromal cells. The purpose of this study was to determine whether DNA methylation of the maspin promoter and histone H3 dimethylation are involved in the mechanism of down regulation of maspin synthesis in human corneal stromal fibroblasts and myofibroblasts. Human donor corneal stroma cells were immediately placed into serum-free defined medium or cultured in the presence of FBS and passed into serum-free medium or medium containing FBS or FGF-2 to induce the fibroblast phenotype or TGF-β1 for the myofibroblast phenotype. These cell types are found in wounded corneas. The cells were used to prepare RNA for semi-quantitative or quantitative RT-PCR or to extract protein for western analysis. In addition, P4 FBS cultured fibroblasts were treated with the DNA demethylating agent, 5-aza-2′-deoxycytidine (5-Aza-dC), and the histone deacetylase inhibitor, trichostatin A (TSA). Cells with and without treatment were harvested and assayed for DNA methylation using sodium bisulfite sequencing. The methylation state of histone H3 associated with the maspin gene in the P4 fibroblast cells was determined using a ChIP assay. Freshly harvested corneal stromal cells expressed maspin but upon phenotypic differentiation, maspin mRNA and protein were dramatically down-regulated. Sodium bisulfite sequencing revealed that the maspin promoter in the freshly isolated stromal keratocytes was hypomethylated while both the P0 stromal cells and the P1 cells cultured in the presence of serum free defined medium, FGF-2 and TGF-β1 were hypermethylated. Down regulation of maspin synthesis was also associated with histone H3 dimethylation at Lysine 9. Both maspin mRNA and protein were reexpressed at low levels with 5-Aza-dC but not TSA treatment. Addition of TSA to 5-Aza-dC treated cells did not increase maspin expression. Treatment with 5-Aza-dC did not significantly alter demethylation of the maspin promoter but did demethylate histone H3. These results show maspin promoter hypermethylation and histone methylation occur with down regulation *Corresponding Author: Sally S. Twining, PhD, Department of Biochemistry, Medical College of Wisconsin, 8701 Watertown Plank Road, Milwaukee, WI 53226, Phone: 414-456-8431, Fax: 414-456-6510, e-mail: stwining@mcw.edu. Publisher's Disclaimer: This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of...

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Section: Discussionmentioning

confidence: 74%

Epigenetic silencing of maspin expression occurs early in the conversion of keratocytes to fibroblasts

Horswill

Narayan

Warejcka

et al. 2008

Experimental Eye Research

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“…2C). When retrovirally transduced in MDA-MB-231 cells, only the ATF-126 was able to strongly reactivate the promoter (70-fold relative to controls, in the absence of drugs), whereas ATF-97 and ATF-452 alone had a much weaker activity (27).…”

Section: Resultsmentioning

confidence: 96%

“…In a previous report, we have described the construction of three ATFs designed to bind 18-bp sites in the maspin proximal promoter (27). The ATFs were constructed by linkage of six sequence-specific ZF domains with the VP64 transactivator domain (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…Real-time PCR Expression Assays ATF-transduced cells and control cells, drug treated or nontreated, were collected, and the RNA was extracted and 2.5 Ag were used for reverse transcription. Quantification of maspin and VP64 activator domain was obtained by realtime quantitative PCR using fluorescent Taqman assays (Applied Biosystems) as described (27). The primers and probes for the VP64 activator domain were the following: 5 ¶-AAGCGACGCATTGGATGAC-3 ¶ (forward primer), 5 ¶-GGAACGTCGTACGGGTAGTTAATT3 ¶ (reverse primer), and 5 ¶-6FAM-TCGGCTCCGATGCT-MGBNFQ-3 ¶ (probe).…”

Section: Atf Retroviral Transductionmentioning

confidence: 99%

“…Our laboratory has recently applied a new strategy to specifically reactivate tumor suppressor genes silenced by epigenetic mechanisms in aggressive tumors (27). We have targeted the tumor suppressor gene maspin using three rationally designed artificial transcription factors (ATFs).…”

Section: Introductionmentioning

confidence: 99%

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Reprogramming epigenetic silencing: artificial transcription factors synergize with chromatin remodeling drugs to reactivate the tumor suppressor mammary serine protease inhibitor

Beltran

Sun

Lizardi

et al. 2008

Molecular Cancer Therapeutics

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Mammary serine protease inhibitor (maspin) is an important tumor suppressor gene whose expression is associated not only with tumor growth inhibition but also with decreased angiogenesis and metastasis. Maspin expression is down-regulated in metastatic tumors by epigenetic mechanisms, including aberrant promoter hypermethylation. We have constructed artificial transcription factors (ATFs) as novel therapeutic effectors able to bind 18-bp sites in the maspin promoter and reactivate maspin expression in cell lines that harbor an epigenetically silenced promoter. In this article, we have investigated the influence of epigenetic modifications on ATF-mediated regulation of maspin by challenging MDA-MB-231 breast cancer cells, comprising a methylated maspin promoter, with different doses of ATFs and chromatin remodeling drugs: the methyltransferase inhibitor 5-aza-2 ¶-deoxycytidine and the histone deacetylase inhibitor suberoylanilide hydroxamic acid. We found that the ATFs synergized with both inhibitors in reactivating endogenous maspin expression. The strongest synergy was observed with the triple treatment ATF-126 + 5-aza-2 ¶-deoxycytidine + suberoylanilide hydroxamic acid, in which the tumor suppressor was reactivated by 600-fold. Furthermore, this combination inhibited tumor cell proliferation by 95%. Our data suggest that ATFs enhance the efficiency of chromatin remodeling drugs in reactivating silenced tumor suppressors. Our results document the power of a novel therapeutic approach that combines both epigenetic and genetic (sequence-specific ATFs) strategies to reactivate specifically silenced regions of the genome and reprogram cellular phenotypes. [Mol Cancer Ther 2008;7(5):1080 -90]

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Pharmaco-Epigenomics to Improve Cancer Therapies

Claes

Siebens

Lambrechts

2012

Encyclopedia of Molecular Cell Biology and Molecular Medicine

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Re-activation of a dormant tumor suppressor gene maspin by designed transcription factors

Cited by 89 publications

References 41 publications

Epigenetic silencing of maspin expression occurs early in the conversion of keratocytes to fibroblasts

Epigenetic silencing of maspin expression occurs early in the conversion of keratocytes to fibroblasts

Reprogramming epigenetic silencing: artificial transcription factors synergize with chromatin remodeling drugs to reactivate the tumor suppressor mammary serine protease inhibitor

Pharmaco-Epigenomics to Improve Cancer Therapies

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