Publication | Open Access
DNA methylation presents distinct binding sites for human transcription factors
359
Citations
40
References
2013
Year
Epigenetic ChangeGeneticsDna MethylationMolecular BiologyEpigeneticsTranscriptional RegulationCpg MethylationTranscription FactorsDna Methylation PresentsDna DemethylationGene ExpressionEpigenetic RegulationFunctional GenomicsTranscription RegulationChromatinChromatin RemodelingNatural SciencesEpigenomicsGene RegulationSystems BiologyMedicine
DNA methylation, especially CpG methylation at promoter regions, has been generally considered as a potent epigenetic modification that prohibits transcription factor (TF) recruitment, resulting in transcription suppression. Here, we used a protein microarray-based approach to systematically survey the entire human TF family and found numerous purified TFs with methylated CpG (mCpG)-dependent DNA-binding activities. Interestingly, some TFs exhibit specific binding activity to methylated and unmethylated DNA motifs of distinct sequences. To elucidate the underlying mechanism, we focused on Kruppel-like factor 4 (KLF4), and decoupled its mCpG- and CpG-binding activities via site-directed mutagenesis. Furthermore, KLF4 binds specific methylated or unmethylated motifs in human embryonic stem cells in vivo. Our study suggests that mCpG-dependent TF binding activity is a widespread phenomenon and provides a new framework to understand the role and mechanism of TFs in epigenetic regulation of gene transcription. DOI:http://dx.doi.org/10.7554/eLife.00726.001.
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