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Nanopore sequencing of DNA concatemers reveals higher-order features of chromatin structure

Authors :
Marcin Imielinski
Daniel J. Turner
Matthew Pendleton
Priyesh Rughani
Stefan Schwenk
Netha Ulahannan
David Wilkes
Sarah Kudman
Huasong Tian
Xiaoguang Dai
Sissel Juul
Julie M. Behr
Aditya Deshpande
Juan Miguel Mosquera
David Stoddart
Eoghan D. Harrington
Carly Tyer
Emily M. Adney
Publication Year :
2019
Publisher :
Cold Spring Harbor Laboratory, 2019.

Abstract

Higher-order chromatin structure arises from the combinatorial physical interactions of many genomic loci. To investigate this aspect of genome architecture we developed Pore-C, which couples chromatin conformation capture with Oxford Nanopore Technologies (ONT) long reads to directly sequence multi-way chromatin contacts without amplification. In GM12878, we demonstrate that the pairwise interaction patterns implicit in Pore-C multi-way contacts are consistent with gold standard Hi-C pairwise contact maps at the compartment, TAD, and loop scales. In addition, Pore-C also detects higher-order chromatin structure at 18.5-fold higher efficiency and greater fidelity than SPRITE, a previously published higher-order chromatin profiling technology. We demonstrate Pore-C’s ability to detect and visualize multi-locus hubs associated with histone locus bodies and active / inactive nuclear compartments in GM12878. In the breast cancer cell line HCC1954, Pore-C contacts enable the reconstruction of complex and aneuploid rearranged alleles spanning multiple megabases and chromosomes. Finally, we apply Pore-C to generate a chromosome scalede novoassembly of the HG002 genome. Our results establish Pore-C as the most simple and scalable assay for the genome-wide assessment of combinatorial chromatin interactions, with additional applications for cancer rearrangement reconstruction andde novogenome assembly.

Details

Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....0483dcc3651516c0e3742b73fe36f2a1
Full Text :
https://doi.org/10.1101/833590