Identification and Characterization of Cell Type–Specific and Ubiquitous Chromatin Regulatory Structures in the Human Genome

Xi, Hualin; Shulha, Hennaed P.; Lin, Jane M.; Vales, Teresa R.; Fu, Yutao; Bodine, David M.; McKay, Ronald D. G.; Chenoweth, Josh G.; Tesar, Paul J.; Furey, Terrence S.; Ren, Bing; Weng, Zhiping; Crawford, Gregory E.

Date Issued

2007-8-17

Publisher Version

10.1371/journal.pgen.0030136

Author(s)

Xi, Hualin

Shulha, Hennaed P.

Lin, Jane M.

Vales, Teresa R.

Fu, Yutao

Bodine, David M.

McKay, Ronald D. G.

Chenoweth, Josh G.

Tesar, Paul J.

Furey, Terrence S.

Ren, Bing

Weng, Zhiping

Crawford, Gregory E.

Export Citation

Download to BibTex

Download to EndNote/RefMan (RIS)

Metadata

Show full item record

Permanent Link

https://hdl.handle.net/2144/3047

Citation (published version)

Xi, Hualin, Hennady P Shulha, Jane M Lin, Teresa R Vales, Yutao Fu, David M Bodine, Ronald D. G McKay, Josh G Chenoweth, Paul J Tesar, Terrence S Furey, Bing Ren, Zhiping Weng, Gregory E Crawford. "Identification and Characterization of Cell Type–Specific and Ubiquitous Chromatin Regulatory Structures in the Human Genome" PLoS Genetics 3(8): e136. (2007)

Abstract

The identification of regulatory elements from different cell types is necessary for understanding the mechanisms controlling cell type–specific and housekeeping gene expression. Mapping DNaseI hypersensitive (HS) sites is an accurate method for identifying the location of functional regulatory elements. We used a high throughput method called DNase-chip to identify 3,904 DNaseI HS sites from six cell types across 1% of the human genome. A significant number (22%) of DNaseI HS sites from each cell type are ubiquitously present among all cell types studied. Surprisingly, nearly all of these ubiquitous DNaseI HS sites correspond to either promoters or insulator elements: 86% of them are located near annotated transcription start sites and 10% are bound by CTCF, a protein with known enhancer-blocking insulator activity. We also identified a large number of DNaseI HS sites that are cell type specific (only present in one cell type); these regions are enriched for enhancer elements and correlate with cell type–specific gene expression as well as cell type–specific histone modifications. Finally, we found that approximately 8% of the genome overlaps a DNaseI HS site in at least one the six cell lines studied, indicating that a significant percentage of the genome is potentially functional. Author Summary. There are many different types of gene regulatory elements that control gene expression. Identifying the location of these regulatory elements in the genome, as well as understanding how exactly they control gene expression in different cell types, has been a major challenge. Here, we use a relatively new strategy to identify all gene regulatory elements within a select 1% of the human genome from six diverse human cell types. We find that only 22% of gene regulatory elements are shared among all cell types studied. Among these, 86% are located near annotated transcription start sites and 10% are bound by CTCF, a protein with known enhancer-blocking insulator activity. The gene regulatory elements that are found to be cell type specific are highly correlated with cell type–specific gene expression as well as cell type–specific chromatin modifications. This indicates that we have made a significant step toward understanding why some genes are expressed in all different cell types within the human body, and why others are only expressed in certain cell types.