Literature DB >> 15252835

DNA binding sites for putative methylation boundaries in the unmethylated region of the BRCA1 promoter.

Darci T Butcher1, Debora N Mancini-DiNardo, Trevor K Archer, David I Rodenhiser.   

Abstract

Changes in DNA methylation patterns are frequently observed in human cancers and are associated with a decrease in tumor suppressor gene expression. Hypermethylation of the BRCA1 promoter has been reported in a portion of sporadic breast tumours that correspond to a reduction in BRCA1 transcription and expression. Questions remain concerning the maintenance of methylation free zones in promoter regions of tumor suppressor genes in normal tissues. Sodium bisulfite based analysis of the BRCA1 promoter defines a methylation free zone in normal breast tissue that starts 650 bp upstream of the transcription start site and extends for 1.4 kb through most of the BRCA1 CpG island. We provide data implicating 2 proteins, Sp1 and CTCF, in the maintenance of this methylation-free zone. Both of these proteins have been shown to function as methylation boundaries in other genes. Four Sp1 sites have been identified in the BRCA1 promoter by gel shift assays. In vivo binding of Sp1 has been confirmed at 2 of these sites in the BRCA1 promoter and at 2 CTCF sites that flank the unmethylated region. Our data suggest that these DNA binding sites for Sp1 and CTCF may act as boundary elements that are important in maintaining genomic integrity by delineating the normal methylation free BRCA1 promoter. Inactivation or disruption of these boundaries may facilitate an epigenetic "hit", in this case DNA methylation, leading to BRCA1 downregulation and contributing to tumorigenesis, particularly the genesis of sporadic breast tumours. Copyright 2004 Wiley-Liss, Inc.

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Year:  2004        PMID: 15252835     DOI: 10.1002/ijc.20324

Source DB:  PubMed          Journal:  Int J Cancer        ISSN: 0020-7136            Impact factor:   7.396


  29 in total

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2.  The promoter methylation status and mRNA expression levels of CTCF and SIRT6 in sporadic breast cancer.

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Review 3.  Chromatin insulators: a role in nuclear organization and gene expression.

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4.  Targeted deletion of multiple CTCF-binding elements in the human C-MYC gene reveals a requirement for CTCF in C-MYC expression.

Authors:  Wendy M Gombert; Anton Krumm
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5.  BAT3 and SET1A form a complex with CTCFL/BORIS to modulate H3K4 histone dimethylation and gene expression.

Authors:  Phuongmai Nguyen; Gil Bar-Sela; Lunching Sun; Kheem S Bisht; Hengmi Cui; Elise Kohn; Andrew P Feinberg; David Gius
Journal:  Mol Cell Biol       Date:  2008-09-02       Impact factor: 4.272

6.  Agglomerative epigenetic aberrations are a common event in human breast cancer.

Authors:  Petr Novak; Taylor Jensen; Marc M Oshiro; George S Watts; Christina J Kim; Bernard W Futscher
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7.  Cause and consequences of genetic and epigenetic alterations in human cancer.

Authors:  B Sadikovic; K Al-Romaih; J A Squire; M Zielenska
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8.  Transcriptional dysregulation in NIPBL and cohesin mutant human cells.

Authors:  Jinglan Liu; Zhe Zhang; Masashige Bando; Takehiko Itoh; Matthew A Deardorff; Dinah Clark; Maninder Kaur; Stephany Tandy; Tatsuro Kondoh; Eric Rappaport; Nancy B Spinner; Hugo Vega; Laird G Jackson; Katsuhiko Shirahige; Ian D Krantz
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9.  In vivo expression of MHC class I genes depends on the presence of a downstream barrier element.

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Review 10.  Epigenetic mechanisms in mammals.

Authors:  J K Kim; M Samaranayake; S Pradhan
Journal:  Cell Mol Life Sci       Date:  2009-02       Impact factor: 9.261

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