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Large-Scale Topological Changes Restrain Malignant Progression in Colorectal Cancer
Author(s) -
Sarah E. Johnstone,
Alejandro Reyes,
Yifeng Qi,
Carmen Adriaens,
E. M. Hegazi,
Karin Pelka,
Jonathan H. Chen,
Luli S. Zou,
Yotam Drier,
Vivian C. Hecht,
Noam Shoresh,
Martin K. Selig,
Caleb A. Lareau,
Sowmya Iyer,
Son C. Nguyen,
Eric F. Joyce,
Nir Hacohen,
Rafael A. Irizarry,
Bin Zhang,
Martin J. Aryee,
B Bernstein
Publication year - 2020
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2020.07.030
Subject(s) - biology , chromatin , epigenomics , epigenetics , compartment (ship) , dna methylation , cancer research , cancer , genome , tumor progression , microbiology and biotechnology , gene , computational biology , genetics , gene expression , oceanography , geology
Widespread changes to DNA methylation and chromatin are well documented in cancer, but the fate of higher-order chromosomal structure remains obscure. Here we integrated topological maps for colon tumors and normal colons with epigenetic, transcriptional, and imaging data to characterize alterations to chromatin loops, topologically associated domains, and large-scale compartments. We found that spatial partitioning of the open and closed genome compartments is profoundly compromised in tumors. This reorganization is accompanied by compartment-specific hypomethylation and chromatin changes. Additionally, we identify a compartment at the interface between the canonical A and B compartments that is reorganized in tumors. Remarkably, similar shifts were evident in non-malignant cells that have accumulated excess divisions. Our analyses suggest that these topological changes repress stemness and invasion programs while inducing anti-tumor immunity genes and may therefore restrain malignant progression. Our findings call into question the conventional view that tumor-associated epigenomic alterations are primarily oncogenic.

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