Lineage-specific dynamic and pre-established enhancer–promoter contacts cooperate in terminal differentiation

增强子 生物 遗传学 转录因子 染色质 细胞分化 基因 细胞生物学 增强子rna
作者
Adam J. Rubin,Brook C. Barajas,Mayra Furlan-Magaril,Vanessa Lopez-Pajares,Maxwell R. Mumbach,I. Brian Howard,Daniel Sunwook Kim,Lisa D. Boxer,Jonathan Cairns,Mikhail Spivakov,Steven Wingett,Minyi Shi,Zhixin Zhao,William J. Greenleaf,Anshul Kundaje,M Snyder,Howard Y. Chang,Peter Fraser,Paul A. Khavari
出处
期刊:Nature Genetics [Nature Portfolio]
卷期号:49 (10): 1522-1528 被引量:276
标识
DOI:10.1038/ng.3935
摘要

Chromosome conformation is an important feature of metazoan gene regulation; however, enhancer-promoter contact remodeling during cellular differentiation remains poorly understood. To address this, genome-wide promoter capture Hi-C (CHi-C) was performed during epidermal differentiation. Two classes of enhancer-promoter contacts associated with differentiation-induced genes were identified. The first class ('gained') increased in contact strength during differentiation in concert with enhancer acquisition of the H3K27ac activation mark. The second class ('stable') were pre-established in undifferentiated cells, with enhancers constitutively marked by H3K27ac. The stable class was associated with the canonical conformation regulator cohesin, whereas the gained class was not, implying distinct mechanisms of contact formation and regulation. Analysis of stable enhancers identified a new, essential role for a constitutively expressed, lineage-restricted ETS-family transcription factor, EHF, in epidermal differentiation. Furthermore, neither class of contacts was observed in pluripotent cells, suggesting that lineage-specific chromatin structure is established in tissue progenitor cells and is further remodeled in terminal differentiation.

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