CTCF-binding sites within the H19 ICR differentially regulate local chromatin structures and cis-acting functions

Sylvain Guibert; Zhihu Zhao; Mikael Sjölinder; Anita Göndör; Alejandro Fernandez; Vinod Pant; Rolf Ohlsson

doi:10.4161/epi.19487

CTCF-binding sites within the H19 ICR differentially regulate local chromatin structures and cis-acting functions

Sylvain Guibert, Zhihu Zhao, Mikael Sjölinder, Anita Göndör, Alejandro Fernandez, Vinod Pant, Rolf Ohlsson

Genetics

Research output: Contribution to journal › Article › peer-review

17 Scopus citations

Abstract

It is generally assumed that CTCF-binding sites are synonymous with the demarcation of expression domains by promoting the formation of chromatin loops. We have proposed earlier, however, that such features may be contextdependent. In support of this notion, we show here that chromatin loop structures, impinging on CTCF-binding sites 1/2 and 3/4 at the 5' and 3'-ends, respectively, within the maternal allele of the H19 imprinting control region (ICR), differ significantly. Although abrogation of CTCF binding to the maternal H19 ICR allele results in loss of chromatin loops in the 3'-region, there is a dramatic gain of long-range chromatin loops impinging on the 5'-region. As the degree of occupancy of its four CTCF-binding sites discriminates between the chromatin insulator and replication timing functions, we submit that the CTCF-binding sites within the H19 ICR are functionally diverse and organize context-dependent higher order chromatin conformations.

Original language	English (US)
Pages (from-to)	361-369
Number of pages	9
Journal	Epigenetics
Volume	7
Issue number	4
DOIs	https://doi.org/10.4161/epi.19487
State	Published - Apr 2012

Keywords

CTCF
Chromatin
H19
Imprinting
Insulator
Replication timing

ASJC Scopus subject areas

Molecular Biology
Cancer Research

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10.4161/epi.19487

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title = "CTCF-binding sites within the H19 ICR differentially regulate local chromatin structures and cis-acting functions",

abstract = "It is generally assumed that CTCF-binding sites are synonymous with the demarcation of expression domains by promoting the formation of chromatin loops. We have proposed earlier, however, that such features may be contextdependent. In support of this notion, we show here that chromatin loop structures, impinging on CTCF-binding sites 1/2 and 3/4 at the 5' and 3'-ends, respectively, within the maternal allele of the H19 imprinting control region (ICR), differ significantly. Although abrogation of CTCF binding to the maternal H19 ICR allele results in loss of chromatin loops in the 3'-region, there is a dramatic gain of long-range chromatin loops impinging on the 5'-region. As the degree of occupancy of its four CTCF-binding sites discriminates between the chromatin insulator and replication timing functions, we submit that the CTCF-binding sites within the H19 ICR are functionally diverse and organize context-dependent higher order chromatin conformations.",

keywords = "CTCF, Chromatin, H19, Imprinting, Insulator, Replication timing",

author = "Sylvain Guibert and Zhihu Zhao and Mikael Sj{\"o}linder and Anita G{\"o}nd{\"o}r and Alejandro Fernandez and Vinod Pant and Rolf Ohlsson",

note = "Funding Information: 173F17) containing target regions nearby or within genes Abcg2 Expert help from Anita Mattsson and Olle Israelsson are gratefully (chromosome 6), Tbl1X (X chromosome) and Osbpl1a (chro-acknowledged. This work was supported by the Swedish Science mosome 18) was labeled with SpectrumOrange-dUTP (Abbott Research Council, the Swedish Cancer Research Foundation, the Molecular) using the BioPrime Array CGH Genomic Labeling Swedish Pediatric Cancer Foundation, the Lundberg Foundation system (Invitrogen). Hybridization with labeled DNA (10 ng/l) and HEROIC (EU integrated project). and mouse Cot1 DNA (100 ng/l) was done overnight at 38°C in 2x SSC, 50% formamide and 12% dextran sulfate. Cells were washed with 2x SSC and 50% formamide (15 min; 38°C) and 2x SSC (15 min; 38°C). For PCNA staining, the cells were",

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doi = "10.4161/epi.19487",

language = "English (US)",

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AU - Guibert, Sylvain

AU - Zhao, Zhihu

AU - Sjölinder, Mikael

AU - Göndör, Anita

AU - Fernandez, Alejandro

AU - Pant, Vinod

AU - Ohlsson, Rolf

N1 - Funding Information: 173F17) containing target regions nearby or within genes Abcg2 Expert help from Anita Mattsson and Olle Israelsson are gratefully (chromosome 6), Tbl1X (X chromosome) and Osbpl1a (chro-acknowledged. This work was supported by the Swedish Science mosome 18) was labeled with SpectrumOrange-dUTP (Abbott Research Council, the Swedish Cancer Research Foundation, the Molecular) using the BioPrime Array CGH Genomic Labeling Swedish Pediatric Cancer Foundation, the Lundberg Foundation system (Invitrogen). Hybridization with labeled DNA (10 ng/l) and HEROIC (EU integrated project). and mouse Cot1 DNA (100 ng/l) was done overnight at 38°C in 2x SSC, 50% formamide and 12% dextran sulfate. Cells were washed with 2x SSC and 50% formamide (15 min; 38°C) and 2x SSC (15 min; 38°C). For PCNA staining, the cells were

PY - 2012/4

Y1 - 2012/4

N2 - It is generally assumed that CTCF-binding sites are synonymous with the demarcation of expression domains by promoting the formation of chromatin loops. We have proposed earlier, however, that such features may be contextdependent. In support of this notion, we show here that chromatin loop structures, impinging on CTCF-binding sites 1/2 and 3/4 at the 5' and 3'-ends, respectively, within the maternal allele of the H19 imprinting control region (ICR), differ significantly. Although abrogation of CTCF binding to the maternal H19 ICR allele results in loss of chromatin loops in the 3'-region, there is a dramatic gain of long-range chromatin loops impinging on the 5'-region. As the degree of occupancy of its four CTCF-binding sites discriminates between the chromatin insulator and replication timing functions, we submit that the CTCF-binding sites within the H19 ICR are functionally diverse and organize context-dependent higher order chromatin conformations.

AB - It is generally assumed that CTCF-binding sites are synonymous with the demarcation of expression domains by promoting the formation of chromatin loops. We have proposed earlier, however, that such features may be contextdependent. In support of this notion, we show here that chromatin loop structures, impinging on CTCF-binding sites 1/2 and 3/4 at the 5' and 3'-ends, respectively, within the maternal allele of the H19 imprinting control region (ICR), differ significantly. Although abrogation of CTCF binding to the maternal H19 ICR allele results in loss of chromatin loops in the 3'-region, there is a dramatic gain of long-range chromatin loops impinging on the 5'-region. As the degree of occupancy of its four CTCF-binding sites discriminates between the chromatin insulator and replication timing functions, we submit that the CTCF-binding sites within the H19 ICR are functionally diverse and organize context-dependent higher order chromatin conformations.

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CTCF-binding sites within the H19 ICR differentially regulate local chromatin structures and cis-acting functions

Abstract

Keywords

ASJC Scopus subject areas

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