Cell Reports
Volume 2, Issue 5, 29 November 2012, Pages 1207-1219
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Article
Large-Scale Functional Organization of Long-Range Chromatin Interaction Networks

https://doi.org/10.1016/j.celrep.2012.09.022Get rights and content
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Summary

Chromatin interactions play important roles in transcription regulation. To better understand the underlying evolutionary and functional constraints of these interactions, we implemented a systems approach to examine RNA polymerase-II-associated chromatin interactions in human cells. We found that 40% of the total genomic elements involved in chromatin interactions converged to a giant, scale-free-like, hierarchical network organized into chromatin communities. The communities were enriched in specific functions and were syntenic through evolution. Disease-associated SNPs from genome-wide association studies were enriched among the nodes with fewer interactions, implying their selection against deleterious interactions by limiting the total number of interactions, a model that we further reconciled using somatic and germline cancer mutation data. The hubs lacked disease-associated SNPs, constituted a nonrandomly interconnected core of key cellular functions, and exhibited lethality in mouse mutants, supporting an evolutionary selection that favored the nonrandom spatial clustering of the least-evolving key genomic domains against random genetic or transcriptional errors in the genome. Altogether, our analyses reveal a systems-level evolutionary framework that shapes functionally compartmentalized and error-tolerant transcriptional regulation of human genome in three dimensions.

Highlights

► Strong regulatory marks govern the modular topology of the chromatin interaction network ► Analysis reveals functionally specific and evolutionarily constrained communities ► Disease-associated genetic errors are enriched among nodes with fewer interactions ► Hubs conform to a “rich-club” organization of key cellular functions

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