| Literature DB >> 30498128 |
Shuhui Bian1,2,3, Yu Hou1,2, Xin Zhou4, Xianlong Li1,2, Jun Yong1,5, Yicheng Wang1,2, Wendong Wang4, Jia Yan1,2, Boqiang Hu1,2, Hongshan Guo1,2, Jilian Wang4, Shuai Gao1,2, Yunuo Mao1,2, Ji Dong1,2, Ping Zhu1,2,3, Dianrong Xiu4, Liying Yan1,5, Lu Wen1,2, Jie Qiao6,3,5,7, Fuchou Tang6,2,3, Wei Fu8.
Abstract
Although genomic instability, epigenetic abnormality, and gene expression dysregulation are hallmarks of colorectal cancer, these features have not been simultaneously analyzed at single-cell resolution. Using optimized single-cell multiomics sequencing together with multiregional sampling of the primary tumor and lymphatic and distant metastases, we developed insights beyond intratumoral heterogeneity. Genome-wide DNA methylation levels were relatively consistent within a single genetic sublineage. The genome-wide DNA demethylation patterns of cancer cells were consistent in all 10 patients whose DNA we sequenced. The cancer cells' DNA demethylation degrees clearly correlated with the densities of the heterochromatin-associated histone modification H3K9me3 of normal tissue and those of repetitive element long interspersed nuclear element 1. Our work demonstrates the feasibility of reconstructing genetic lineages and tracing their epigenomic and transcriptomic dynamics with single-cell multiomics sequencing.Entities:
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Year: 2018 PMID: 30498128 DOI: 10.1126/science.aao3791
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728