Rolling back human pluripotent stem cells to an eight-cell embryo-like stage

被引:0
|
作者
Md. Abdul Mazid
Carl Ward
Zhiwei Luo
Chuanyu Liu
Yunpan Li
Yiwei Lai
Liang Wu
Jinxiu Li
Wenqi Jia
Yu Jiang
Hao Liu
Lixin Fu
Yueli Yang
David P. Ibañez
Junjian Lai
Xiaoyu Wei
Juan An
Pengcheng Guo
Yue Yuan
Qiuting Deng
Yang Wang
Ying Liu
Fei Gao
Junwen Wang
Shahriar Zaman
Baoming Qin
Guangming Wu
Patrick H. Maxwell
Xun Xu
Longqi Liu
Wenjuan Li
Miguel A. Esteban
机构
[1] Guangzhou Institutes of Biomedicine and Health,Laboratory of Integrative Biology
[2] Chinese Academy of Sciences,Jilin Provincial Key Laboratory of Animal Embryo Engineering, Key Laboratory of Zoonoses Research, Ministry of Education, College of Veterinary Medicine
[3] University of Chinese Academy of Sciences,School of Life Sciences, Division of Life Sciences and Medicine
[4] BGI-Shenzhen,Genome Analysis Laboratory of the Ministry of Agriculture
[5] Jilin University,Department of Genetic Engineering and Biotechnology, Faculty of Life and Earth Sciences
[6] University of Science and Technology of China,Laboratory of Metabolism and Cell Fate
[7] Agricultural Genomics Institute at Shenzhen,Cambridge Institute for Medical Research, Department of Medicine
[8] Chinese Academy of Agricultural Sciences,Institute of Stem Cells and Regeneration
[9] E-GENE,undefined
[10] University of Rajshahi,undefined
[11] Guangzhou Institutes of Biomedicine and Health,undefined
[12] Chinese Academy of Sciences,undefined
[13] Guangzhou Laboratory,undefined
[14] University of Cambridge,undefined
[15] Guangdong Provincial Key Laboratory of Genome Read and Write,undefined
[16] Chinese Academy of Sciences,undefined
来源
Nature | 2022年 / 605卷
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摘要
After fertilization, the quiescent zygote experiences a burst of genome activation that initiates a short-lived totipotent state. Understanding the process of totipotency in human cells would have broad applications. However, in contrast to in mice1,2, demonstration of the time of zygotic genome activation or the eight-cell (8C) stage in in vitro cultured human cells has not yet been reported, and the study of embryos is limited by ethical and practical considerations. Here we describe a transgene-free, rapid and controllable method for producing 8C-like cells (8CLCs) from human pluripotent stem cells. Single-cell analysis identified key molecular events and gene networks associated with this conversion. Loss-of-function experiments identified fundamental roles for DPPA3, a master regulator of DNA methylation in oocytes3, and TPRX1, a eutherian totipotent cell homeobox (ETCHbox) family transcription factor that is absent in mice4. DPPA3 induces DNA demethylation throughout the 8CLC conversion process, whereas TPRX1 is a key executor of 8CLC gene networks. We further demonstrate that 8CLCs can produce embryonic and extraembryonic lineages in vitro or in vivo in the form of blastoids5 and complex teratomas. Our approach provides a resource to uncover the molecular process of early human embryogenesis.
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页码:315 / 324
页数:9
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