Motif oriented high-resolution analysis of ChIP-seq data reveals the topological order of CTCF and cohesin proteins on DNA.

Gergely NagyErik CzipaLászló SteinerTibor NagySándor PongorLászló NagyEndre Barta

Published in: BMC genomics (2016)

A motif-centered, strand specific analysis of ChIP-seq data improves the accuracy of determining peak positions. If a genome contains a large number of binding sites for a given protein complex, such as transcription factor heterodimers or transcription factor/cofactor complexes, the relative position of the constituent proteins on the DNA can be established with an accuracy that allow one to deduce the local topology of the protein complex. The proposed high resolution mapping approach of ChIP-seq data is applicable for detecting the contact topology of DNA-binding protein complexes.

Keyphrases

high resolution
transcription factor
circulating tumor
binding protein
genome wide
circulating tumor cells
electronic health record
single cell
cell free
high throughput
rna seq
single molecule
big data
mass spectrometry
nucleic acid
data analysis
amino acid
high density
deep learning