Insulator function and topological domain border strength scale with architectural protein occupancy

Kevin Van Bortle; Michael H. Nichols; Li Li; Chin Tong Ong; Naomi Takenaka; Zhaohui S. Qin; Victor G. Corces

doi:10.1186/gb-2014-15-5-r82

Insulator function and topological domain border strength scale with architectural protein occupancy

Kevin Van Bortle, Michael H. Nichols, Li Li, Chin Tong Ong, Naomi Takenaka, Zhaohui S. Qin, Victor G. Corces

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

Abstract

BACKGROUND: Chromosome conformation capture studies suggest that eukaryotic genomes are organized into structures called topologically associating domains. The borders of these domains are highly enriched for architectural proteins with characterized roles in insulator function. However, a majority of architectural protein binding sites localize within topological domains, suggesting sites associated with domain borders represent a functionally different subclass of these regulatory elements. How topologically associating domains are established and what differentiates border-associated from non-border architectural protein binding sites remain unanswered questions.

RESULTS: By mapping the genome-wide target sites for several Drosophila architectural proteins, including previously uncharacterized profiles for TFIIIC and SMC-containing condensin complexes, we uncover an extensive pattern of colocalization in which architectural proteins establish dense clusters at the borders of topological domains. Reporter-based enhancer-blocking insulator activity as well as endogenous domain border strength scale with the occupancy level of architectural protein binding sites, suggesting co-binding by architectural proteins underlies the functional potential of these loci. Analyses in mouse and human stem cells suggest that clustering of architectural proteins is a general feature of genome organization, and conserved architectural protein binding sites may underlie the tissue-invariant nature of topologically associating domains observed in mammals.

CONCLUSIONS: We identify a spectrum of architectural protein occupancy that scales with the topological structure of chromosomes and the regulatory potential of these elements. Whereas high occupancy architectural protein binding sites associate with robust partitioning of topologically associating domains and robust insulator function, low occupancy sites appear reserved for gene-specific regulation within topological domains.

Original language	English (US)
Pages (from-to)	R82
Journal	Genome biology
Volume	15
Issue number	6
DOIs	https://doi.org/10.1186/gb-2014-15-5-r82
State	Published - 2014
Externally published	Yes

ASJC Scopus subject areas

Ecology, Evolution, Behavior and Systematics
Genetics
Cell Biology

Online availability

10.1186/gb-2014-15-5-r82

Library availability

Discover UIUC Full Text

Cite this

@article{de051241e3384b23b4dc90dbfb44f5fa,

title = "Insulator function and topological domain border strength scale with architectural protein occupancy",

abstract = "BACKGROUND: Chromosome conformation capture studies suggest that eukaryotic genomes are organized into structures called topologically associating domains. The borders of these domains are highly enriched for architectural proteins with characterized roles in insulator function. However, a majority of architectural protein binding sites localize within topological domains, suggesting sites associated with domain borders represent a functionally different subclass of these regulatory elements. How topologically associating domains are established and what differentiates border-associated from non-border architectural protein binding sites remain unanswered questions.RESULTS: By mapping the genome-wide target sites for several Drosophila architectural proteins, including previously uncharacterized profiles for TFIIIC and SMC-containing condensin complexes, we uncover an extensive pattern of colocalization in which architectural proteins establish dense clusters at the borders of topological domains. Reporter-based enhancer-blocking insulator activity as well as endogenous domain border strength scale with the occupancy level of architectural protein binding sites, suggesting co-binding by architectural proteins underlies the functional potential of these loci. Analyses in mouse and human stem cells suggest that clustering of architectural proteins is a general feature of genome organization, and conserved architectural protein binding sites may underlie the tissue-invariant nature of topologically associating domains observed in mammals.CONCLUSIONS: We identify a spectrum of architectural protein occupancy that scales with the topological structure of chromosomes and the regulatory potential of these elements. Whereas high occupancy architectural protein binding sites associate with robust partitioning of topologically associating domains and robust insulator function, low occupancy sites appear reserved for gene-specific regulation within topological domains.",

author = "{Van Bortle}, Kevin and Nichols, {Michael H.} and Li Li and Ong, {Chin Tong} and Naomi Takenaka and Qin, {Zhaohui S.} and Corces, {Victor G.}",

note = "Funding Information: We are especially thankful to Drs Dale Dorsett, Hugo Bellen, Giovanni Bosco, and J{\o}rgen Johansen for graciously sharing antibodies against Rad21, Barren, CAP-H2, and Chromator. We thank the Drosophila Genomic Resource Center (supported by NIH grant OD010949-10) for reagents, and The Genomic Services Lab at the HudsonAlpha Institute for Biotechnology for their help in performing Illumina sequencing of ChIP-Seq samples. This work was supported by US Public Health Service Award R01GM035463 from the National Institutes of Health. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health.",

year = "2014",

doi = "10.1186/gb-2014-15-5-r82",

language = "English (US)",

volume = "15",

pages = "R82",

journal = "Genome biology",

issn = "1465-6906",

publisher = "BioMed Central",

number = "6",

}

TY - JOUR

T1 - Insulator function and topological domain border strength scale with architectural protein occupancy

AU - Van Bortle, Kevin

AU - Nichols, Michael H.

AU - Li, Li

AU - Ong, Chin Tong

AU - Takenaka, Naomi

AU - Qin, Zhaohui S.

AU - Corces, Victor G.

N1 - Funding Information: We are especially thankful to Drs Dale Dorsett, Hugo Bellen, Giovanni Bosco, and Jørgen Johansen for graciously sharing antibodies against Rad21, Barren, CAP-H2, and Chromator. We thank the Drosophila Genomic Resource Center (supported by NIH grant OD010949-10) for reagents, and The Genomic Services Lab at the HudsonAlpha Institute for Biotechnology for their help in performing Illumina sequencing of ChIP-Seq samples. This work was supported by US Public Health Service Award R01GM035463 from the National Institutes of Health. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health.

PY - 2014

Y1 - 2014

N2 - BACKGROUND: Chromosome conformation capture studies suggest that eukaryotic genomes are organized into structures called topologically associating domains. The borders of these domains are highly enriched for architectural proteins with characterized roles in insulator function. However, a majority of architectural protein binding sites localize within topological domains, suggesting sites associated with domain borders represent a functionally different subclass of these regulatory elements. How topologically associating domains are established and what differentiates border-associated from non-border architectural protein binding sites remain unanswered questions.RESULTS: By mapping the genome-wide target sites for several Drosophila architectural proteins, including previously uncharacterized profiles for TFIIIC and SMC-containing condensin complexes, we uncover an extensive pattern of colocalization in which architectural proteins establish dense clusters at the borders of topological domains. Reporter-based enhancer-blocking insulator activity as well as endogenous domain border strength scale with the occupancy level of architectural protein binding sites, suggesting co-binding by architectural proteins underlies the functional potential of these loci. Analyses in mouse and human stem cells suggest that clustering of architectural proteins is a general feature of genome organization, and conserved architectural protein binding sites may underlie the tissue-invariant nature of topologically associating domains observed in mammals.CONCLUSIONS: We identify a spectrum of architectural protein occupancy that scales with the topological structure of chromosomes and the regulatory potential of these elements. Whereas high occupancy architectural protein binding sites associate with robust partitioning of topologically associating domains and robust insulator function, low occupancy sites appear reserved for gene-specific regulation within topological domains.

AB - BACKGROUND: Chromosome conformation capture studies suggest that eukaryotic genomes are organized into structures called topologically associating domains. The borders of these domains are highly enriched for architectural proteins with characterized roles in insulator function. However, a majority of architectural protein binding sites localize within topological domains, suggesting sites associated with domain borders represent a functionally different subclass of these regulatory elements. How topologically associating domains are established and what differentiates border-associated from non-border architectural protein binding sites remain unanswered questions.RESULTS: By mapping the genome-wide target sites for several Drosophila architectural proteins, including previously uncharacterized profiles for TFIIIC and SMC-containing condensin complexes, we uncover an extensive pattern of colocalization in which architectural proteins establish dense clusters at the borders of topological domains. Reporter-based enhancer-blocking insulator activity as well as endogenous domain border strength scale with the occupancy level of architectural protein binding sites, suggesting co-binding by architectural proteins underlies the functional potential of these loci. Analyses in mouse and human stem cells suggest that clustering of architectural proteins is a general feature of genome organization, and conserved architectural protein binding sites may underlie the tissue-invariant nature of topologically associating domains observed in mammals.CONCLUSIONS: We identify a spectrum of architectural protein occupancy that scales with the topological structure of chromosomes and the regulatory potential of these elements. Whereas high occupancy architectural protein binding sites associate with robust partitioning of topologically associating domains and robust insulator function, low occupancy sites appear reserved for gene-specific regulation within topological domains.

UR - http://www.scopus.com/inward/record.url?scp=85006305723&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85006305723&partnerID=8YFLogxK

U2 - 10.1186/gb-2014-15-5-r82

DO - 10.1186/gb-2014-15-5-r82

M3 - Article

C2 - 24981874

AN - SCOPUS:85006305723

SN - 1465-6906

VL - 15

SP - R82

JO - Genome biology

JF - Genome biology

IS - 6

ER -

Insulator function and topological domain border strength scale with architectural protein occupancy

Abstract

ASJC Scopus subject areas

Online availability

Library availability

Related links

Fingerprint

Cite this