Spatial chromatin accessibility sequencing resolves high-order spatial interactions of epigenomic markers

Author:

Xie Yeming1,Ruan Fengying1,Li Yaning1,Luo Meng1,Zhang Chen1,Chen Zhichao12,Xie Zhe23,Weng Zhe1,Chen Weitian12,Chen Wenfang1,Fang Yitong1ORCID,Sun Yuxin1,Guo Mei1,Wang Juan1,Xu Shouping4,Wang Hongqi1,Tang Chong1ORCID

Affiliation:

1. BGI Genomics, BGI-Shenzhen

2. College of Life Sciences, University of Chinese Academy of Sciences

3. Department of Biology, Cell Biology and Physiology, University of Copenhagen

4. Department of Breast Surgery, Harbin Medical University Cancer Hospital

Abstract

As the genome is organized into a three-dimensional structure in intracellular space, epigenomic information also has a complex spatial arrangement. However, most epigenetic studies describe locations of methylation marks, chromatin accessibility regions, and histone modifications in the horizontal dimension. Proper spatial epigenomic information has rarely been obtained. In this study, we designed spatial chromatin accessibility sequencing (SCA-seq) to resolve the genome conformation by capturing the epigenetic information in single-molecular resolution while simultaneously resolving the genome conformation. Using SCA-seq, we are able to examine the spatial interaction of chromatin accessibility (e.g. enhancer–promoter contacts), CpG island methylation, and spatial insulating functions of the CCCTC-binding factor. We demonstrate that SCA-seq paves the way to explore the mechanism of epigenetic interactions and extends our knowledge in 3D packaging of DNA in the nucleus.

Funder

Shenzhen Municipal Science and Technology Innovation Council

Publisher

eLife Sciences Publications, Ltd

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