NicE-seq: high resolution open chromatin profiling

NicE-seq: high resolution open chromatin profiling

Open chromatin profiling integrates information across diverse regulatory elements to reveal the transcriptionally active genome. Tn5 transposase and DNase I sequencing-based methods prefer native or high cell numbers. Here, we describe NicE-seq (nicking enzyme assisted sequencing) for high-resoluti...

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Veröffentlicht in:Genome Biology 2017-06, Vol.18 (1), p.122-122, Article 122
Hauptverfasser: Ponnaluri, V K Chaithanya, Zhang, Guoqiang, Estève, Pierre-Olivier, Spracklin, George, Sian, Stephanie, Xu, Shuang-Yong, Benoukraf, Touati, Pradhan, Sriharsa
Format: Artikel
Sprache:eng
Schlagworte:
5-aza-2'-deoxycytidine
Binding sites
Bioinformatics
Cell cycle
Cell division
Chromatin
Chromatin - genetics
Chromosomes
Colorectal cancer
CpG islands
CpG Islands - genetics
Deoxyribonuclease
Deoxyribonuclease I - genetics
Deoxyribonucleic acid
DNA
DNA methylation
DNA Methylation - genetics
DNA polymerase
DNA sequencing
DNA-directed RNA polymerase
E coli
Enzymes
Epigenetics
Gene expression
Genome, Human - genetics
Genomes
HCT116 Cells
Humans
Labeling
Method
Methods
Molecular weight
NicE-seq
Nicking endonuclease
Open chromatin
Physiological aspects
Proteins
Regulatory Elements, Transcriptional - genetics
Regulatory sequences
RNA Polymerase II - genetics
Stem cells
Transcription factor occupancy
Transcription factors
Transposase
Transposases - genetics
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Zusammenfassung:Open chromatin profiling integrates information across diverse regulatory elements to reveal the transcriptionally active genome. Tn5 transposase and DNase I sequencing-based methods prefer native or high cell numbers. Here, we describe NicE-seq (nicking enzyme assisted sequencing) for high-resolution open chromatin profiling on both native and formaldehyde-fixed cells. NicE-seq captures and reveals open chromatin sites (OCSs) and transcription factor occupancy at single nucleotide resolution, coincident with DNase hypersensitive and ATAC-seq sites at a low sequencing burden. OCSs correlate with RNA polymerase II occupancy and active chromatin marks, while displaying a contrasting pattern to CpG methylation. Decitabine-mediated hypomethylation of HCT116 displays higher numbers of OCSs.
ISSN:1474-760X
1474-7596
1474-760X
DOI:10.1186/s13059-017-1247-6