论文信息 - Multiple mechanisms induce transcriptional silencing of a subset of genes, including oestrogen receptor α, in response to deacetylase inhibition by valproic acid and trichostatin A - 字舞流文

Multiple mechanisms induce transcriptional silencing of a subset of genes, including oestrogen receptor α, in response to deacetylase inhibition by valproic acid and trichostatin A

Valproate (VPA) and trichostatin A (TSA), inhibitors of zinc-dependent deacetylase activity, induce reduction in the levels of mRNA encoding oestrogen receptor-α (ERα), resulting in subsequent clearance of ERα protein from breast and ovarian cell lines. Inhibition of oestrogen signalling may account for the endocrine disorders, menstrual abnormalities, osteoporosis and weight gain that occur in a proportion of women treated with VPA for epilepsy or for bipolar mood disorder. Transcriptome profiling revealed that VPA and TSA also modulate the expression of, among others, key regulatory components of the cell cycle. Meta-analysis of genes directly responsive to oestrogen indicates that VPA and TSA have a generally antioestrogenic profile in ERα positive cells. Concomitant treatment with cycloheximide prevented most of these changes in gene expression, including downregulation of ERα mRNA, indicating that a limited number of genes signal a hyperacetylated state within cells. Three members of the NAD-dependent deacetylases, the sirtuins, are upregulated by VPA and by TSA and sirtuin activity contributes to loss of ERα expression. However, prolonged inhibition of the sirtuins by sirtinol also induces loss of ERα from cells. Mechanistically, we show that VPA invokes reversible promoter shutoff of the ERα, pS2 and cyclin D1 promoters, by inducing recruitment of methyl cytosine binding protein 2 (MeCP2) with concomitant exclusion of the maintenance methylase DNMT1. Furthermore, we demonstrate that, in the presence of VPA, local DNA methylation, deacetylation and demethylation of activated histones and recruitment of inhibitory complexes occurs on the pS2 promoter.

Heike Brand | Chin-Yo Lin | Vladimir Benes | George Reid | Frank Gannon | Edison T Liu | V. Beneš | E. Liu | F. Gannon | Chin-Yo Lin | R. Métivier | G. Reid | D. Ibberson | Tomi Ivacevic | Raphaël Métivier | David Ibberson | H. Brand | Stefanie Denger | S. Denger | Tomi Ivacevic

[1] Mike Clarke,et al. Tamoxifen for early breast cancer: an overview of the randomised trials , 1998, The Lancet.

[2] M. Knip,et al. Early hormonal changes during valproate or carbamazepine treatment , 2001, Neurology.

[3] Heike Brand,et al. Estrogen Receptor-α Directs Ordered, Cyclical, and Combinatorial Recruitment of Cofactors on a Natural Target Promoter , 2003, Cell.

[4] J. Slingerland,et al. Down-regulation of p21WAF1/CIP1 or p27Kip1 abrogates antiestrogen-mediated cell cycle arrest in human breast cancer cells. , 2000, Proceedings of the National Academy of Sciences of the United States of America.

[5] Myles Brown,et al. Molecular Determinants for the Tissue Specificity of SERMs , 2002, Science.

[6] G. G. Stokes. "J." , 1890, The New Yale Book of Quotations.

[7] David Botstein,et al. RERG Is a Novel ras-related, Estrogen-regulated and Growth-inhibitory Gene in Breast Cancer* , 2001, The Journal of Biological Chemistry.

[8] S. Schreiber,et al. Identification of a Class of Small Molecule Inhibitors of the Sirtuin Family of NAD-dependent Deacetylases by Phenotypic Screening* , 2001, The Journal of Biological Chemistry.

[9] F. Lallemand,et al. Direct inhibition of the expression of cyclin D1 gene by sodium butyrate. , 1996, Biochemical and biophysical research communications.

[10] S. Kyrylenko,et al. Differential regulation of the Sir2 histone deacetylase gene family by inhibitors of class I and II histone deacetylases , 2003, Cellular and Molecular Life Sciences CMLS.

[11] M. Guenther,et al. Histone Deacetylase Is a Direct Target of Valproic Acid, a Potent Anticonvulsant, Mood Stabilizer, and Teratogen* , 2001, The Journal of Biological Chemistry.

[12] A. Pakarinen,et al. Polycystic Ovaries and Hyperandrogenism in Women Taking Valproate for Epilepsy , 1993 .

[13] M Baum,et al. First results from the International Breast Cancer Intervention Study (IBIS-I): a randomised prevention trial , 2002, The Lancet.

[14] A. Bird,et al. MeCP2 Is a Transcriptional Repressor with Abundant Binding Sites in Genomic Chromatin , 1997, Cell.

[15] J. Kurebayashi,et al. Endocrine-resistant breast cancer: Underlying mechanisms and strategies for overcoming resistance , 2003, Breast cancer.

[16] Myles Brown,et al. Cofactor Dynamics and Sufficiency in Estrogen Receptor–Regulated Transcription , 2000, Cell.

[17] J. Simpkins,et al. Estrogens and Estrogen‐Like Non‐Feminizing Compounds: Their Role in the Prevention and Treatment of Alzheimer's Disease , 2000, Annals of the New York Academy of Sciences.

[18] F. Denizot,et al. Rapid colorimetric assay for cell growth and survival. Modifications to the tetrazolium dye procedure giving improved sensitivity and reliability. , 1986, Journal of immunological methods.

[19] Ulla Hansen,et al. Nucleosome Positioning and Transcription-associated Chromatin Alterations on the Human Estrogen-responsive pS2 Promoter* , 1997, The Journal of Biological Chemistry.

[20] Tony Kouzarides,et al. The Methyl-CpG-binding Protein MeCP2 Links DNA Methylation to Histone Methylation* , 2003, The Journal of Biological Chemistry.

[21] V. Kusumakar,et al. Menstrual abnormalities and polycystic ovary syndrome in women taking valproate for bipolar mood disorder. , 2002, The Journal of clinical psychiatry.

[22] E. Trinka,et al. Increase in postprandial serum insulin levels in epileptic patients with valproic acid therapy. , 2002, Metabolism: clinical and experimental.

[23] J. Carroll,et al. A Pure Estrogen Antagonist Inhibits Cyclin E-Cdk2 Activity in MCF-7 Breast Cancer Cells and Induces Accumulation of p130-E2F4 Complexes Characteristic of Quiescence* , 2000, The Journal of Biological Chemistry.

[24] Allen Chong,et al. Discovery of estrogen receptor α target genes and response elements in breast tumor cells , 2004, Genome Biology.

[25] E. Hughes,et al. Randomised comparative monotherapy trial of phenobarbitone, phenytoin, carbamazepine, or sodium valproate for newly diagnosed childhood epilepsy , 1996, The Lancet.

[26] Ericka Stricklin-Parker,et al. Ann , 2005 .

[27] A. Colao,et al. Estrogens and health in males , 2001, Molecular and Cellular Endocrinology.

[28] K. Satoh,et al. Decreased bone mass and increased bone turnover with valproate therapy in adults with epilepsy [RETRACTED] , 2001, Neurology.

[29] Zbigniew Dauter,et al. Molecular basis of agonism and antagonism in the oestrogen receptor , 1997, Nature.

[30] M. Moore,et al. Associated effects of sodium butyrate on histone acetylation and estrogen receptor in the human breast cancer cell line MCF-7. , 1984, Biochemical and biophysical research communications.

[31] S. Duncan. Polycystic Ovarian Syndrome in Women with Epilepsy: A Review , 2001, Epilepsia.

[32] B. Macmahon,et al. Etiology of human breast cancer: a review. , 1973, Journal of the National Cancer Institute.