The binding sites for the chromatin insulator protein CTCF map to DNA methylation-free domains genome-wide

All known vertebrate chromatin insulators interact with the highly conserved, multivalent 11-zinc finger nuclear factor CTCF to demarcate expression domains by blocking enhancer or silencer signals in a position-dependent manner. Recent observations document that the properties of CTCF include readi...

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Veröffentlicht in:Genome research 2004-08, Vol.14 (8), p.1594-1602
Hauptverfasser: Mukhopadhyay, Rituparna, Yu, WenQiang, Whitehead, Joanne, Xu, JunWang, Lezcano, Magda, Pack, Svetlana, Kanduri, Chandrasekhar, Kanduri, Meena, Ginjala, Vasudeva, Vostrov, Alexander, Quitschke, Wolfgang, Chernukhin, Igor, Klenova, Elena, Lobanenkov, Victor, Ohlsson, Rolf
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Sprache:eng
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Zusammenfassung:All known vertebrate chromatin insulators interact with the highly conserved, multivalent 11-zinc finger nuclear factor CTCF to demarcate expression domains by blocking enhancer or silencer signals in a position-dependent manner. Recent observations document that the properties of CTCF include reading and propagating the epigenetic state of the differentially methylated H19 imprinting control region. To assess whether these findings may reflect a universal role for CTCF targets, we identified more than 200 new CTCF target sites by generating DNA microarrays of clones derived from chromatin-immunopurified (ChIP) DNA followed by ChIP-on-chip hybridization analysis. Target sites include not only known loci involved in multiple cellular functions, such as metabolism, neurogenesis, growth, apoptosis, and signalling, but potentially also heterochromatic sequences. Using a novel insulator trapping assay, we also show that the majority of these targets manifest insulator functions with a continuous distribution of stringency. As these targets are generally DNA methylation-free as determined by antibodies against 5-methylcytidine and a methyl-binding protein (MBD2), a CTCF-based network correlates with genome-wide epigenetic states.
ISSN:1088-9051
1549-5469
DOI:10.1101/gr.2408304