Your search keyword '"Szyf, Moshe"' showing total 5 results

1. Reversal of the Hypomethylation Status of Urokinase (uPA) Promoter Blocks Breast Cancer Growth and Metastasis.

Author

Pakneshan, Pouya, Szyf, Moshe, Farias-Eisner, Robin, and Rabbani, Shafaat A.

Subjects

*UROKINASE, *BREAST cancer, *METASTASIS, *CANCER invasiveness, *GENES, *CARRIER proteins, *STEROID hormones, *TUMOR growth

Abstract

Metastasis is a leading cause of mortality and morbidity in cancer. Urokinase (uPA), only expressed by the highly invasive cancer cells, has been implicated in invasion, metastases, and angiogenesis of several malignancies including breast cancer. Because uPA expression is strongly correlated with its hypomethylated state, we utilized the uPA gene in the highly invasive MDA-231 human breast cancer cells as a model system to test the hypothesis that pharmacological reversal of the uPA promoter hypomethylation would result in its silencing and inhibition of metastasis. S-Adenosyl-L-methionine (AdoMet) has previously been shown to cause hypermethylation and inhibit demethylation. Treatmerit of MDA-231 cells with AdoMet, but not its unmethylated analogue S-adenosylhomocysteine, significantly inhibits uPA expression and tumor cell invasion in vitro and tumor growth and metastasis in vivo. The effects of AdoMet on uPA expression were reversed by the demethylating agent 5'-azacytidine, supporting the conclusion that AdoMet effects are caused by hypermethylation. Knockdown of the methyl-binding protein 2 also causes a significant inhibition of uPA expression in vitro and tumor growth and metastasis in vivo. These treatments did not have any effects on estrogen receptor expression, suggesting that inhibition of hypomethylation will not affect genes already silenced by hypermethylation. These data are consistent with the hypothesis that hypomethylation of critical genes like uPA plays a causal role in metastasis. Inhibition of hypomethylation can thus be used as a novel therapeutic approach to silence the pro-metastatic gene uPA and block breast cancer progression into the aggressive and metastatic stages of the disease. [ABSTRACT FROM AUTHOR]

Published

2004

2. Valproate Induces Replication-independent Active DNA Demethylation.

Author

Detich, Nancy, Bovenzi, Veronica, and Szyf, Moshe

Subjects

*VALPROIC acid, *DNA, *BIOCHEMISTRY

Abstract

In this report, we demonstrate that valproic acid (VPA), a drug that has been used for decades in the treatment of epilepsy and as a mood stabilizer, triggers replication-independent active demethylation of DNA. Thus, this drug can potentially reverse DNA methylation patterns and erase stable methylation imprints on DNA in non-dividing cells. Recent discoveries support a role for VPA in the regulation of methylated genes; however, the mechanism has been unclear because it is difficult to dissociate active demethylation from the absence of DNA methylation during DNA synthesis. We therefore took advantage of an assay that measures active DNA demethylation independently from other DNA methylation and DNA replication activities in human embryonal kidney 293 cells. We show that VPA induces histone acetylation, DNA demethylation, and expression of an ectopically methylated CMV-GFP plasmid in a dosedependent manner. In contrast, valpromide, an analogue of VPA that does not induce histone acetylation, does not induce demethylation or expression of CMVGFP. Furthermore, we illustrate that methylated DNAbinding protein 2/DNA demethylase (MBD2/dMTase) participates in this reaction since antisense knockdown of MBD2/dMTase attenuates VPA-induced demethylation. Taken together, our data support a new mechanism of action for VPA as enhancing intracellular demethylase activity through its effects on histone acetylation and raises the possibility that DNA methylation is reversible independent of DNA replication by commonly prescribed drugs. [ABSTRACT FROM AUTHOR]

Published

2003

3. DNA Methyltransferase 1 Knock Down Induces Gene Expression by a Mechanism Independent of DNA Methylation and Histone Deacetylation.

Author

Milutinovic, Snezana, Brown, Shelley E., Qianli Zhuang, and Szyf, Moshe

Subjects

*METHYLTRANSFERASES, *METHYLATION, *DNA, *CELL division, *CARCINOGENESIS, *TUMOR suppressor genes, *LUNG cancer, *APOPTOSIS

Abstract

DNA methyltransferase 1 (DNMT1) catalyzes the postreplication methylation of DNA and is responsible for maintaining the DNA methylation pattern during cell division. A long list of data supports a role for DNMT1 in cellular transformation and inhibitors of DNMT1 were shown to have antitumorigenic effects. It was long believed that DNMT1 promoted tumorigenesis by maintaining the hypermethylated and silenced state of tumor suppressor genes. We have previously shown that DNMT1 knock down by either antisense oligonucleotides directed at DNMT1 or expressed antisense activates a number of genes involved in stress response and cell cycle arrest by a DNA methylation-independent mechanism. In this report we demonstrate that antisense knock down of DNMT1 in human lung carcinoma A549 and embryonal kidney HEK293 cells induces gene expression by a mechanism that does not involve either of the known epigenomic mechanisms, DNA methylation, histone acetylation, or histone methylation. The mechanism of activation of the cell cycle inhibitor p21 and apoptosis inducer BIK by DNMT1 inhibition is independent of the mechanism of activation of the same genes by histone deacetylase inhibition. We determine whether DNMT1 knock down activates one of the nodal transcription activation pathways in the cell and demonstrate that DNMT1 activates Sp1 response elements. This activation of Sp1 response does not involve an increase in either Sp1 or Sp3 protein levels in the cell or the occupancy of the Sp1 elements with these proteins. The methylation-independent regulation of Sp1 elements by DNMT1 unravels a novel function for DNMT1 in gene regulation. DNA methylation was believed to be a mechanism for suppression of CG-rich Sp1-bearing promoters. Our data suggest a fundamentally different and surprising role for DNMT1 regulation of CG-rich genes by a mechanism independent of DNA methylation and histone acetylation. The implications of our data on the biological roles of DNMT1 and the therapeutic potential of DNMT1 inhibitors as anticancer agents are discussed. [ABSTRACT FROM AUTHOR]

Published

2004

4. The Methyl Donor S-Adenosylmethionine Inhibits Active Demethylation of DNA.

Author

Detich, Nancy, Hamm, Stefan, Just, George, Knox, J. David, and Szyf, Moshe

Subjects

*ADENOSYLMETHIONINE, *GREEN fluorescent protein

Abstract

Outlines a study conducted by researchers from Canada, which shows that exogenous S-adenosylmethionine (AdoMet) inhibits TSA-stimulated demethylation of ectopically methylated and transiently transfected CMV-green fluorescent protein (GFP) DNA. Effects of increasing doses of AdoMet on the demetylation of methylated CMV-GFP.

Published

2003

5. Epigenomic Stress Response.

Author

Milutinovic, Snezana, Zhuang, Qianli, Niveleau, Alain, and Szyf, Moshe

Subjects

*CELLS, *VERTEBRATES, *METHYLTRANSFERASES, *OLIGONUCLEOTIDES, *ANTISENSE DNA

Abstract

Evaluates the hypothesis that vertebrate cells possess mechanisms that protect them from epigenomic stress similar to DNA damage checkpoints. Effect of DNA methyltransferase knockdown by an oligonucleotide antisense on the intra-S-phase arrest of DNA replication; Implication on the arrest of cells at different positions throughout the S-phase of the cell cycle; Proposition on intra-S-phase arrest of DNA replication.

Published

2003