Author
Listed:
- Jianquan Xu
(University of Pittsburgh)
- Hongqiang Ma
(University of Pittsburgh)
- Hongbin Ma
(University of Pittsburgh
The First Affiliated Hospital of Dalian Medical University
Dalian Jinzhou First People’s Hospital)
- Wei Jiang
(University of Pittsburgh
Sichuan University)
- Christopher A. Mela
(University of Pittsburgh)
- Meihan Duan
(University of Pittsburgh
Tsinghua University)
- Shimei Zhao
(University of Pittsburgh
Guangxi University of Science and Technology)
- Chenxi Gao
(University of Pittsburgh
University of Pittsburgh Hillman Cancer Center)
- Eun-Ryeong Hahm
(University of Pittsburgh
University of Pittsburgh Hillman Cancer Center)
- Santana M. Lardo
(University of Pittsburgh)
- Kris Troy
(University of Pittsburgh)
- Ming Sun
(University of Pittsburgh)
- Reet Pai
(University of Pittsburgh School of Medicine)
- Donna B. Stolz
(University of Pittsburgh)
- Lin Zhang
(University of Pittsburgh
University of Pittsburgh Hillman Cancer Center)
- Shivendra Singh
(University of Pittsburgh
University of Pittsburgh Hillman Cancer Center)
- Randall E. Brand
(University of Pittsburgh Hillman Cancer Center
University of Pittsburgh)
- Douglas J. Hartman
(University of Pittsburgh School of Medicine)
- Jing Hu
(University of Pittsburgh Hillman Cancer Center
University of Pittsburgh)
- Sarah J. Hainer
(University of Pittsburgh)
- Yang Liu
(University of Pittsburgh
University of Pittsburgh Hillman Cancer Center
University of Pittsburgh)
Abstract
Genomic DNA is folded into a higher-order structure that regulates transcription and maintains genomic stability. Although progress has been made on understanding biochemical characteristics of epigenetic modifications in cancer, the in-situ higher-order folding of chromatin structure during malignant transformation remains largely unknown. Here, using optimized stochastic optical reconstruction microscopy (STORM) for pathological tissue (PathSTORM), we uncover a gradual decompaction and fragmentation of higher-order chromatin folding throughout all stages of carcinogenesis in multiple tumor types, and prior to tumor formation. Our integrated imaging, genomic, and transcriptomic analyses reveal functional consequences in enhanced transcription activities and impaired genomic stability. We also demonstrate the potential of imaging higher-order chromatin disruption to detect high-risk precursors that cannot be distinguished by conventional pathology. Taken together, our findings reveal gradual decompaction and fragmentation of higher-order chromatin structure as an enabling characteristic in early carcinogenesis to facilitate malignant transformation, which may improve cancer diagnosis, risk stratification, and prevention.
Suggested Citation
Jianquan Xu & Hongqiang Ma & Hongbin Ma & Wei Jiang & Christopher A. Mela & Meihan Duan & Shimei Zhao & Chenxi Gao & Eun-Ryeong Hahm & Santana M. Lardo & Kris Troy & Ming Sun & Reet Pai & Donna B. Sto, 2020.
"Super-resolution imaging reveals the evolution of higher-order chromatin folding in early carcinogenesis,"
Nature Communications, Nature, vol. 11(1), pages 1-17, December.
Handle:
RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-020-15718-7
DOI: 10.1038/s41467-020-15718-7
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Citations
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Cited by:
- Timothy A. Daugird & Yu Shi & Katie L. Holland & Hosein Rostamian & Zhe Liu & Luke D. Lavis & Joseph Rodriguez & Brian D. Strahl & Wesley R. Legant, 2024.
"Correlative single molecule lattice light sheet imaging reveals the dynamic relationship between nucleosomes and the local chromatin environment,"
Nature Communications, Nature, vol. 15(1), pages 1-20, December.
- Taichi Igarashi & Marianne Mazevet & Takaaki Yasuhara & Kimiyoshi Yano & Akifumi Mochizuki & Makoto Nishino & Tatsuya Yoshida & Yukihiro Yoshida & Nobuhiko Takamatsu & Akihide Yoshimi & Kouya Shiraish, 2023.
"An ATR-PrimPol pathway confers tolerance to oncogenic KRAS-induced and heterochromatin-associated replication stress,"
Nature Communications, Nature, vol. 14(1), pages 1-22, December.
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