Simultaneous profiling of histone modifications and DNA methylation via nanopore sequencing

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作者
Xue Yue
Zhiyuan Xie
Moran Li
Kai Wang
Xiaojing Li
Xiaoqing Zhang
Jian Yan
Yimeng Yin
机构
[1] Tongji University,Translational Research Institute of Brain and Brain
[2] Tongji University,Like Intelligence, Shanghai Fourth People’s Hospital, School of Medicine
[3] Tongji University,Clinical Center for Brain and Spinal Cord Research
[4] Key Laboratory of Spine and Spinal Cord Injury Repair and Regeneration of Ministry of Education,Translational Medical Center for Stem Cell Therapy, Shanghai East Hospital, School of Medicine
[5] Orthopaedic Department of Tongji Hospital,Tung Biomedical Sciences Centre, Department of Biomedical Sciences
[6] School of Medicine,undefined
[7] Northwest University,undefined
[8] City University of Hong Kong,undefined
[9] Kowloon,undefined
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摘要
The interplay between histone modifications and DNA methylation drives the establishment and maintenance of the cellular epigenomic landscape, but it remains challenging to investigate the complex relationship between these epigenetic marks across the genome. Here we describe a nanopore-sequencing-based-method, nanoHiMe-seq, for interrogating the genome-wide localization of histone modifications and DNA methylation from single DNA molecules. nanoHiMe-seq leverages a nonspecific methyltransferase to exogenously label adenine bases proximal to antibody-targeted modified nucleosomes in situ. The labelled adenines and the endogenous methylated CpG sites are simultaneously detected on individual nanopore reads using a hidden Markov model, which is implemented in the nanoHiMe software package. We demonstrate the utility, robustness and sensitivity of nanoHiMe-seq by jointly profiling DNA methylation and histone modifications at low coverage depths, concurrently determining phased patterns of DNA methylation and histone modifications, and probing the intrinsic connectivity between these epigenetic marks across the genome.
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