| Literature DB >> 29937202 |
Ting Zhao1, Yao Fu2, Jialiang Zhu2, Yifang Liu3, Qian Zhang4, Zexuan Yi5, Shi Chen6, Zhonggang Jiao2, Xiaochan Xu7, Junquan Xu8, Shuguang Duo9, Yun Bai6, Chao Tang7, Cheng Li10, Hongkui Deng11.
Abstract
Chemical reprogramming provides a powerful platform for exploring the molecular dynamics that lead to pluripotency. Although previous studies have uncovered an intermediate extraembryonic endoderm (XEN)-like state during this process, the molecular underpinnings of pluripotency acquisition remain largely undefined. Here, we profile 36,199 single-cell transcriptomes at multiple time points throughout a highly efficient chemical reprogramming system using RNA-sequencing and reconstruct their progression trajectories. Through identifying sequential molecular events, we reveal that the dynamic early embryonic-like programs are key aspects of successful reprogramming from XEN-like state to pluripotency, including the concomitant transcriptomic signatures of two-cell (2C) embryonic-like and early pluripotency programs and the epigenetic signature of notable genome-wide DNA demethylation. Moreover, via enhancing the 2C-like program by fine-tuning chemical treatment, the reprogramming process is remarkably accelerated. Collectively, our findings offer a high-resolution dissection of cell fate dynamics during chemical reprogramming and shed light on mechanistic insights into the nature of induced pluripotency.Keywords: 2C-like program; CiPSC; XEN-like cell; Zscan4; chemical reprogramming; early embryonic-like programs; genome-wide hypomethylation; pluripotency; reprogramming trajectory; single-cell RNA-seq
Mesh:
Year: 2018 PMID: 29937202 DOI: 10.1016/j.stem.2018.05.025
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633