Freeze substitution Hi-C, a convenient and cost-effective method for capturing the natural 3D chromatin conformation from frozen samples

替代(逻辑) 染色质 自然(考古学) 化学 计算机科学 计算生物学 DNA 生物 生物化学 古生物学 程序设计语言
作者
Zheng Wu,Zhaoen Yang,Xiaoyang Ge,Yijia Feng,Ye Wang,Chang Liu,Yanan Luan,Cai Kun,Serhii Vakal,Feng You,Wei Guo,Wei Wang,Zhenhua Feng,Fuguang Li
出处
期刊:Journal of Genetics and Genomics [Elsevier BV]
卷期号:48 (3): 237-247 被引量:7
标识
DOI:10.1016/j.jgg.2020.11.002
摘要

Chromatin interactions functionally affect genome architecture and gene regulation, but to date, only fresh samples must be used in High-through chromosome conformation capture (Hi-C) to keep natural chromatin conformation intact. This requirement has impeded the advancement of 3D genome research by limiting sample collection and storage options for researchers and severely limiting the number of samples that can be processed in a short time. Here, we develop a freeze substitution Hi-C (FS-Hi-C) technique that overcomes the need for fresh samples. FS-Hi-C can be used with samples stored in liquid nitrogen (LN2): the water in a vitreous form in the sample cells is replaced with ethanol via automated freeze substitution. After confirming that the FS step preserves the natural chromosome conformation during sample thawing, we tested the performance of FS-Hi-C with Drosophila melanogaster and Gossypium hirsutum. Beyond allowing the use of frozen samples and confirming that FS-Hi-C delivers robust data for generating contact heat maps and delineating A/B compartments and topologically associating domains, we found that FS-Hi-C outperforms the in situ Hi-C in terms of library quality, reproducibility, and valid interactions. Thus, FS-Hi-C will probably extend the application of 3D genome structure analysis to the vast number of experimental contexts in biological and medical research for which Hi-C methods have been unfeasible to date.

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