Single-cell Hi-C reveals cell-to-cell variability in chromosome structure

被引:0
|
作者
Takashi Nagano
Yaniv Lubling
Tim J. Stevens
Stefan Schoenfelder
Eitan Yaffe
Wendy Dean
Ernest D. Laue
Amos Tanay
Peter Fraser
机构
[1] Nuclear Dynamics Programme,Department of Computer Science and Applied Mathematics and Department of Biological Regulation
[2] The Babraham Institute,Department of Biochemistry
[3] Cambridge CB22 3AT,undefined
[4] UK,undefined
[5] Weizmann Institute,undefined
[6] Rehovot 76100,undefined
[7] Israel,undefined
[8] University of Cambridge,undefined
[9] Cambridge CB2 1GA,undefined
[10] UK,undefined
[11] Epigenetics Programme,undefined
[12] The Babraham Institute,undefined
[13] Cambridge CB22 3AT,undefined
[14] UK,undefined
来源
Nature | 2013年 / 502卷
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摘要
Large-scale chromosome structure and spatial nuclear arrangement have been linked to control of gene expression and DNA replication and repair. Genomic techniques based on chromosome conformation capture (3C) assess contacts for millions of loci simultaneously, but do so by averaging chromosome conformations from millions of nuclei. Here we introduce single-cell Hi-C, combined with genome-wide statistical analysis and structural modelling of single-copy X chromosomes, to show that individual chromosomes maintain domain organization at the megabase scale, but show variable cell-to-cell chromosome structures at larger scales. Despite this structural stochasticity, localization of active gene domains to boundaries of chromosome territories is a hallmark of chromosomal conformation. Single-cell Hi-C data bridge current gaps between genomics and microscopy studies of chromosomes, demonstrating how modular organization underlies dynamic chromosome structure, and how this structure is probabilistically linked with genome activity patterns.
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页码:59 / 64
页数:5
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