The insulator binding protein CTCF positions 20 nucleosomes around its binding sites across the human genome.

Chromatin structure plays an important role in modulating the accessibility of genomic DNA to regulatory proteins in eukaryotic cells. We performed an integrative analysis on dozens of recent datasets generated by deep-sequencing and high-density tiling arrays, and we discovered an array of well-pos...

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Main Authors: Yutao Fu, Manisha Sinha, Craig L Peterson, Zhiping Weng
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2008-07-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC2453330?pdf=render
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spelling doaj-f6da689df485469abf14810579cb36682020-11-24T21:56:53ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042008-07-0147e100013810.1371/journal.pgen.1000138The insulator binding protein CTCF positions 20 nucleosomes around its binding sites across the human genome.Yutao FuManisha SinhaCraig L PetersonZhiping WengChromatin structure plays an important role in modulating the accessibility of genomic DNA to regulatory proteins in eukaryotic cells. We performed an integrative analysis on dozens of recent datasets generated by deep-sequencing and high-density tiling arrays, and we discovered an array of well-positioned nucleosomes flanking sites occupied by the insulator binding protein CTCF across the human genome. These nucleosomes are highly enriched for the histone variant H2A.Z and 11 histone modifications. The distances between the center positions of the neighboring nucleosomes are largely invariant, and we estimate them to be 185 bp on average. Surprisingly, subsets of nucleosomes that are enriched in different histone modifications vary greatly in the lengths of DNA protected from micrococcal nuclease cleavage (106-164 bp). The nucleosomes enriched in those histone modifications previously implicated to be correlated with active transcription tend to contain less protected DNA, indicating that these modifications are correlated with greater DNA accessibility. Another striking result obtained from our analysis is that nucleosomes flanking CTCF sites are much better positioned than those downstream of transcription start sites, the only genomic feature previously known to position nucleosomes genome-wide. This nucleosome-positioning phenomenon is not observed for other transcriptional factors for which we had genome-wide binding data. We suggest that binding of CTCF provides an anchor point for positioning nucleosomes, and chromatin remodeling is an important component of CTCF function.http://europepmc.org/articles/PMC2453330?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Yutao Fu
Manisha Sinha
Craig L Peterson
Zhiping Weng
spellingShingle Yutao Fu
Manisha Sinha
Craig L Peterson
Zhiping Weng
The insulator binding protein CTCF positions 20 nucleosomes around its binding sites across the human genome.
PLoS Genetics
author_facet Yutao Fu
Manisha Sinha
Craig L Peterson
Zhiping Weng
author_sort Yutao Fu
title The insulator binding protein CTCF positions 20 nucleosomes around its binding sites across the human genome.
title_short The insulator binding protein CTCF positions 20 nucleosomes around its binding sites across the human genome.
title_full The insulator binding protein CTCF positions 20 nucleosomes around its binding sites across the human genome.
title_fullStr The insulator binding protein CTCF positions 20 nucleosomes around its binding sites across the human genome.
title_full_unstemmed The insulator binding protein CTCF positions 20 nucleosomes around its binding sites across the human genome.
title_sort insulator binding protein ctcf positions 20 nucleosomes around its binding sites across the human genome.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2008-07-01
description Chromatin structure plays an important role in modulating the accessibility of genomic DNA to regulatory proteins in eukaryotic cells. We performed an integrative analysis on dozens of recent datasets generated by deep-sequencing and high-density tiling arrays, and we discovered an array of well-positioned nucleosomes flanking sites occupied by the insulator binding protein CTCF across the human genome. These nucleosomes are highly enriched for the histone variant H2A.Z and 11 histone modifications. The distances between the center positions of the neighboring nucleosomes are largely invariant, and we estimate them to be 185 bp on average. Surprisingly, subsets of nucleosomes that are enriched in different histone modifications vary greatly in the lengths of DNA protected from micrococcal nuclease cleavage (106-164 bp). The nucleosomes enriched in those histone modifications previously implicated to be correlated with active transcription tend to contain less protected DNA, indicating that these modifications are correlated with greater DNA accessibility. Another striking result obtained from our analysis is that nucleosomes flanking CTCF sites are much better positioned than those downstream of transcription start sites, the only genomic feature previously known to position nucleosomes genome-wide. This nucleosome-positioning phenomenon is not observed for other transcriptional factors for which we had genome-wide binding data. We suggest that binding of CTCF provides an anchor point for positioning nucleosomes, and chromatin remodeling is an important component of CTCF function.
url http://europepmc.org/articles/PMC2453330?pdf=render
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