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Extensive promoter-centered chromatin interactions provide a topological basis for transcription regulation.
by:
Guoliang Li ,
Xiaoan Ruan ,
Raymond K. Auerbach ,
Kuljeet Singh S. Sandhu ,
Meizhen Zheng ,
Ping Wang ,
Huay Mei M. Poh ,
Yufen Goh ,
Joanne Lim ,
Jingyao Zhang ,
Hui Shan S. Sim ,
Su Qin Q. Peh ,
Fabianus Hendriyan H. Mulawadi ,
Chin Thing T. Ong ,
Yuriy L. Orlov ,
Shuzhen Hong ,
Zhizhuo Zhang ,
Steve Landt ,
Debasish Raha ,
Ghia Euskirchen ,
Chia-Lin L. Wei ,
Weihong Ge ,
Huaien Wang ,
Carrie Davis ,
Katherine I. Fisher-Aylor ,
Ali Mortazavi ,
Mark Gerstein ,
Thomas Gingeras ,
Barbara Wold ,
Yi Sun ,
Melissa J. Fullwood ,
Edwin Cheung ,
Edison Liu ,
Wing-Kin K. Sung ,
Michael Snyder ,
Yijun Ruan
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Abstract
Higher-order chromosomal organization for transcription regulation is poorly understood in eukaryotes. Using genome-wide Chromatin Interaction Analysis with Paired-End-Tag sequencing (ChIA-PET), we mapped long-range chromatin interactions associated with RNA polymerase II in human cells and uncovered widespread promoter-centered intragenic, extragenic, and intergenic interactions. These interactions further aggregated into higher-order clusters, wherein proximal and distal genes were engaged through promoter-promoter interactions. Most genes with promoter-promoter interactions were active and transcribed cooperatively, and some interacting promoters could influence each other implying combinatorial complexity of transcriptional controls. Comparative analyses of different cell lines showed that cell-specific chromatin interactions could provide structural frameworks for cell-specific transcription, and suggested significant enrichment of enhancer-promoter interactions for cell-specific functions. Furthermore, genetically-identified disease-associated noncoding elements were found to be spatially engaged with corresponding genes through long-range interactions. Overall, our study provides insights into transcription regulation by three-dimensional chromatin interactions for both housekeeping and cell-specific genes in human cells. Copyright © 2012 Elsevier Inc. All rights reserved.
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