| Literature DB >> 34038708 |
Jia Wang1, Haopeng Yu2, Qian Ma1, Pengguihang Zeng1, Danya Wu3, Yingping Hou4, Xinyi Liu1, Lumeng Jia5, Jun Sun1, Yilong Chen2, Diana Guallar6, Miguel Fidalgo6, Jiahao Chen1, Yangyinhui Yu7, Shaoshuai Jiang1, Fenjie Li1, Cai Zhao1, Xianglin Huang1, Jianlong Wang8, Cheng Li9, Yujie Sun10, Xiaoxi Zeng2, Wei Zhang2, Yiliang Miao3, Junjun Ding11.
Abstract
Topological-associated domains (TADs) are thought to be relatively stable across cell types, although some TAD reorganization has been observed during cellular differentiation. However, little is known about the mechanisms through which TAD reorganization affects cell fate or how master transcription factors affect TAD structures during cell fate transitions. Here, we show extensive TAD reorganization during somatic cell reprogramming, which is correlated with gene transcription and changes in cellular identity. Manipulating TAD reorganization promotes reprogramming, and the dynamics of concentrated chromatin loops in OCT4 phase separated condensates contribute to TAD reorganization. Disrupting OCT4 phase separation attenuates TAD reorganization and reprogramming, which can be rescued by fusing an intrinsically disordered region (IDR) to OCT4. We developed an approach termed TAD reorganization-based multiomics analysis (TADMAN), which identified reprogramming regulators. Together, these findings elucidate a role and mechanism of TAD reorganization, regulated by OCT4 phase separation, in cellular reprogramming.Entities:
Keywords: OCT4; TAD reorganization; TADMAN; phase separation; reprogramming
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Year: 2021 PMID: 34038708 DOI: 10.1016/j.stem.2021.04.023
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633