| Literature DB >> 35817982 |
Shanshan Zhang1,2, Dylan Plummer3, Leina Lu1, Jian Cui1, Wanying Xu1,2, Miao Wang4, Xiaoxiao Liu1, Nachiketh Prabhakar3, Jatin Shrinet4, Divyaa Srinivasan4, Peter Fraser4, Yan Li5, Jing Li6,7, Fulai Jin8,9,10.
Abstract
Mapping chromatin loops from noisy Hi-C heatmaps remains a major challenge. Here we present DeepLoop, which performs rigorous bias correction followed by deep-learning-based signal enhancement for robust chromatin interaction mapping from low-depth Hi-C data. DeepLoop enables loop-resolution, single-cell Hi-C analysis. It also achieves a cross-platform convergence between different Hi-C protocols and micrococcal nuclease (micro-C). DeepLoop allowed us to map the genetic and epigenetic determinants of allele-specific chromatin interactions in the human genome. We nominate new loci with allele-specific interactions governed by imprinting or allelic DNA methylation. We also discovered that, in the inactivated X chromosome (Xi), local loops at the DXZ4 'megadomain' boundary escape X-inactivation but the FIRRE 'superloop' locus does not. Importantly, DeepLoop can pinpoint heterozygous single-nucleotide polymorphisms and large structure variants that cause allelic chromatin loops, many of which rewire enhancers with transcription consequences. Taken together, DeepLoop expands the use of Hi-C to provide loop-resolution insights into the genetics of the three-dimensional genome.Entities:
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Year: 2022 PMID: 35817982 DOI: 10.1038/s41588-022-01116-w
Source DB: PubMed Journal: Nat Genet ISSN: 1061-4036 Impact factor: 41.307