| Literature DB >> 26832419 |
Jun Chen1, Xiaolong Chen2, Min Li2, Xiaoyu Liu3, Yawei Gao2, Xiaochen Kou2, Yanhong Zhao2, Weisheng Zheng2, Xiaobai Zhang2, Yi Huo3, Chuan Chen2, You Wu2, Hong Wang2, Cizhong Jiang4, Shaorong Gao5.
Abstract
The core pluripotency factor Oct4 plays key roles in somatic cell reprogramming through transcriptional control. Here, we profile Oct4 occupancy, epigenetic changes, and gene expression in reprogramming. We find that Oct4 binds in a hierarchical manner to target sites with primed epigenetic modifications. Oct4 binding is temporally continuous and seldom switches between bound and unbound. Oct4 occupancy in most of promoters is maintained throughout the entire reprogramming process. In contrast, somatic cell-specific enhancers are silenced in the early and intermediate stages, whereas stem cell-specific enhancers are activated in the late stage in parallel with cell fate transition. Both epigenetic remodeling and Oct4 binding contribute to the hyperdynamic enhancer signature transitions. The hierarchical Oct4 bindings are associated with distinct functional themes at different stages. Collectively, our results provide a comprehensive molecular roadmap of Oct4 binding in concert with epigenetic rearrangements and rich resources for future reprogramming studies.Entities:
Keywords: Oct4; histone modification; iPSC; reprogramming
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Year: 2016 PMID: 26832419 DOI: 10.1016/j.celrep.2016.01.013
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423