单细胞Hi-C表明TADs是果蝇基因组折叠的稳定单位,持续存在于单个细胞中

V. V. Zakharova, Aleksandra Galitsyna, K. Polovnikov, E. Khrameeva, M. Logacheva, E. Mikhaleva, E. Vassetzky, A. Gavrilov, Y. Y. Shevelev, S. Nechaev, S. Ulianov, S. Razin
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引用次数: 0

摘要

基因组的三维组织似乎具有功能相关性,因为它允许在启动子和远程调控元件之间建立远程空间接触。然而,对三维基因组组织的大多数观察都是通过传统方法在细胞群体中进行的,其中只有所谓的典型细胞的平均特征可以被识别。另一方面,基于fish的研究表明,基因组的空间结构在单个细胞中是不同的。然而,微观方法不允许进行全基因组分析,这对于更好地理解在3D基因组组织水平上发生的调控事件至关重要。高通量染色体构象捕获方案(Hi-C)最近被修改,允许构建单个细胞的染色质接触频率图。利用这一改进方案,我们构建了20个果蝇细胞(细胞系Dm-BG3c2)的Hi-C图谱。在最好的电池中,我们捕获了约15%的理论可用触点。这允许以10 Kb的分辨率构建空间接触矩阵。对这些矩阵的分析表明,拓扑相关结构域(TADs)并不代表计算机生成的总体平均值,而是存在于单个细胞中。重要的是,使用一些统计方法,我们表明在单个细胞中观察到的接触染色质结构域的轮廓不能用随机波动来解释。此外,我们表明,在单个细胞中,tad是分层组织的,这种分层结构与种群图中看到的分层结构密切匹配。最后,我们表明,基因组区域经常拥有接触域边界具有特定的表观遗传特征。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Single-cell Hi-C demonstrates that TADs are stable units of Drosophila genome folding that persist in individual cells
The 3D organization of the genome appears to be functionally relevant as it allows establishing of long-range spatial contacts between promoters and remote regulatory elements. However, most of the observations on the 3D genome organization have been made by conventional methods in cell population where only average characteristics of the so-called typical cell can be identified. On the other hand, FISH-based studies demonstrated that the spatial configuration of the genome varies in individual cells. However, the microscopic approaches do not allow performing a genome-wide analysis that is critical to understand better the regulatory events occurring at the level of 3D genome organization. The high throughput chromosome conformation capture protocol (Hi-C) has been modified recently to allow construction of chromatin contact frequency maps for individual cells. Using this modified protocol we constructed Hi-C maps for 20 drosophila cells (line Dm-BG3c2). In the best cell we have captured ~15% of the theoretically available contacts. This allowed constructing of the spatial contact matrices with 10 Kb resolution. Analysis of these matrices demonstrated that topologically-associating domains (TADs) do not represent a computer-generated population average, but exist in individual cells. Importantly, using a number of statistical approaches we show that the observed profile of contact chromatin domains in individual cells cannot be explained by random fluctuations. Furthermore, we show that in individual cells TADs are organized hierarchically, and that this hierarchy closely matches the hierarchy seen in population maps. Finally, we show that genomic regions that frequently harbor the contact domain borders possess specific epigenetic signatures.
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