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Genome-wide ChIP-seq analysis of human TOP2B occupancy in MCF7 breast cancer epithelial cells

Authors :
Graham Jackson
Zbyslaw Sondka
Simon Cockell
Kay Padget
Caroline A. Austin
Holly Ashlene Rance
Catriona Manville
Kayleigh A. Smith
Ka Cheong Lee
Nicholas J. Morris
Ian G. Cowell
Source :
Biology Open, Vol 4, Iss 11, Pp 1436-1447 (2015), Biology Open
Publication Year :
2015
Publisher :
The Company of Biologists, 2015.

Abstract

We report the whole genome ChIP seq for human TOP2B from MCF7 cells. Using three different peak calling methods, regions of binding were identified in the presence or absence of the nuclear hormone estradiol, as TOP2B has been reported to play a role in ligand-induced transcription. TOP2B peaks were found across the whole genome, 50% of the peaks fell either within a gene or within 5 kb of a transcription start site. TOP2B peaks coincident with gene promoters were less frequently associated with epigenetic features marking active promoters in estradiol treated than in untreated cells. Significantly enriched transcription factor motifs within the DNA sequences underlying the peaks were identified. These included SP1, KLF4, TFAP2A, MYF, REST, CTCF, ESR1 and ESR2. Gene ontology analysis of genes associated with TOP2B peaks found neuronal development terms including axonogenesis and axon guidance were significantly enriched. In the absence of functional TOP2B there are errors in axon guidance in the zebrafish eye. Specific heparin sulphate structures are involved in retinal axon targeting. The glycosaminoglycan biosynthesis–heparin sulphate/heparin pathway is significantly enriched in the TOP2B gene ontology analysis, suggesting changes in this pathway in the absence of TOP2B may cause the axon guidance faults.<br />Summary: Gene ontology enrichment analysis of genes associated with human TOP2B peaks, identified by whole genome ChIP seq used to identify regions of binding, highlighted a number of processes in neuronal development including axonogenesis and axon guidance.

Details

Language :
English
ISSN :
20466390
Volume :
4
Issue :
11
Database :
OpenAIRE
Journal :
Biology Open
Accession number :
edsair.doi.dedup.....439070e5fc3cec5ed444e93fc575e278