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单细胞 Hi-C 将显微镜和全基因组测序方法相结合,用于研究 3D 染色质构象。

Single-cell Hi-C bridges microscopy and genome-wide sequencing approaches to study 3D chromatin organization.

机构信息

Institute of Gene Biology, Russian Academy of Sciences, Moscow, Russia.

Faculty of Biology, Lomonosov Moscow State University, Moscow, Russia.

出版信息

Bioessays. 2017 Oct;39(10). doi: 10.1002/bies.201700104. Epub 2017 Aug 9.

DOI:10.1002/bies.201700104
PMID:28792605
Abstract

Recent years have witnessed an explosion of the single-cell biochemical toolbox including chromosome conformation capture (3C)-based methods that provide novel insights into chromatin spatial organization in individual cells. The observations made with these techniques revealed that topologically associating domains emerge from cell population averages and do not exist as static structures in individual cells. Stochastic nature of the genome folding is likely to be biologically relevant and may reflect the ability of chromatin fibers to adopt a number of alternative configurations, some of which could be transiently stabilized and serve regulatory purposes. Single-cell Hi-C approaches provide an opportunity to analyze chromatin folding in rare cell types such as stem cells, tumor progenitors, oocytes, and totipotent cells, contributing to a deeper understanding of basic mechanisms in development and disease. Here, we review key findings of single-cell Hi-C and discuss possible biological reasons and consequences of the inferred dynamic chromatin spatial organization.

摘要

近年来,单细胞生化工具包呈爆炸式增长,其中包括基于染色体构象捕获(3C)的方法,这些方法为单个细胞中染色质空间组织提供了新的见解。这些技术的观察结果表明,拓扑关联域是从细胞群体平均值中出现的,而不是在单个细胞中作为静态结构存在。基因组折叠的随机性可能具有生物学相关性,并且可能反映了染色质纤维能够采用许多替代构象的能力,其中一些构象可能暂时稳定并具有调节作用。单细胞 Hi-C 方法提供了分析罕见细胞类型(如干细胞、肿瘤祖细胞、卵母细胞和全能细胞)中染色质折叠的机会,有助于更深入地了解发育和疾病中的基本机制。在这里,我们回顾了单细胞 Hi-C 的关键发现,并讨论了推断出的动态染色质空间组织的可能生物学原因和后果。

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