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HiCAR is a robust and sensitive method to analyze open-chromatin-associated genome organization.


ABSTRACT: The long-range interactions of cis-regulatory elements (cREs) play a central role in gene regulation. cREs can be characterized as accessible chromatin sequences. However, it remains technically challenging to comprehensively identify their spatial interactions. Here, we report a new method HiCAR (Hi-C on accessible regulatory DNA), which utilizes Tn5 transposase and chromatin proximity ligation, for the analysis of open-chromatin-anchored interactions with low-input cells. By applying HiCAR in human embryonic stem cells and lymphoblastoid cells, we demonstrate that HiCAR identifies high-resolution chromatin contacts with an efficiency comparable with that of in situ Hi-C over all distance ranges. Interestingly, we found that the "poised" gene promoters exhibit silencer-like function to repress the expression of distal genes via promoter-promoter interactions. Lastly, we applied HiCAR to 30,000 primary human muscle stem cells and demonstrated that HiCAR is capable of analyzing chromatin accessibility and looping using low-input primary cells and clinical samples.

SUBMITTER: Wei X 

PROVIDER: S-EPMC8934281 | biostudies-literature | 2022 Mar

REPOSITORIES: biostudies-literature

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HiCAR is a robust and sensitive method to analyze open-chromatin-associated genome organization.

Wei Xiaolin X   Xiang Yu Y   Peters Derek T DT   Marius Choiselle C   Sun Tongyu T   Shan Ruocheng R   Ou Jianhong J   Lin Xin X   Yue Feng F   Li Wei W   Southerland Kevin W KW   Diao Yarui Y  

Molecular cell 20220222 6


The long-range interactions of cis-regulatory elements (cREs) play a central role in gene regulation. cREs can be characterized as accessible chromatin sequences. However, it remains technically challenging to comprehensively identify their spatial interactions. Here, we report a new method HiCAR (Hi-C on accessible regulatory DNA), which utilizes Tn5 transposase and chromatin proximity ligation, for the analysis of open-chromatin-anchored interactions with low-input cells. By applying HiCAR in  ...[more]

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