Article ID Journal Published Year Pages File Type
2040998 Cell Reports 2012 13 Pages PDF
Abstract

SummaryChromatin 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.

Graphical AbstractFigure optionsDownload full-size imageDownload as PowerPoint slideHighlights► 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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Life Sciences Agricultural and Biological Sciences Agricultural and Biological Sciences (General)
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