Mouse totipotent stem cells captured and maintained through spliceosomal repression.

IF 5.7 1区化学 Q2 CHEMISTRY, PHYSICAL

Journal of Chemical Theory and Computation Pub Date : 2021-05-27 Epub Date: 2021-05-14 DOI:10.1016/j.cell.2021.04.020

Hui Shen, Min Yang, Shiyu Li, Jing Zhang, Bing Peng, Chunhui Wang, Zai Chang, Jennie Ong, Peng Du

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引用次数: 88

Abstract

Since establishment of the first embryonic stem cells (ESCs), in vitro culture of totipotent cells functionally and molecularly comparable with in vivo blastomeres with embryonic and extraembryonic developmental potential has been a challenge. Here we report that spliceosomal repression in mouse ESCs drives a pluripotent-to-totipotent state transition. Using the splicing inhibitor pladienolide B, we achieve stable in vitro culture of totipotent ESCs comparable at molecular levels with 2- and 4-cell blastomeres, which we call totipotent blastomere-like cells (TBLCs). Mouse chimeric assays combined with single-cell RNA sequencing (scRNA-seq) demonstrate that TBLCs have a robust bidirectional developmental capability to generate multiple embryonic and extraembryonic cell lineages. Mechanically, spliceosomal repression causes widespread splicing inhibition of pluripotent genes, whereas totipotent genes, which contain few short introns, are efficiently spliced and transcriptionally activated. Our study provides a means for capturing and maintaining totipotent stem cells.

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通过剪接体抑制捕获和维持小鼠全能干细胞。

自首例胚胎干细胞(ESCs)建立以来，在体外培养功能和分子上与体内卵裂球相当的具有胚胎和胚胎外发育潜力的全能细胞一直是一个挑战。在这里，我们报告剪接体抑制小鼠ESCs驱动多能到全能状态的转变。利用剪接抑制剂pladienolide B，我们在体外稳定培养出了与2细胞和4细胞卵裂球(我们称之为全能卵裂球样细胞(TBLCs))分子水平相当的全能ESCs。小鼠嵌合实验结合单细胞RNA测序(scRNA-seq)表明，TBLCs具有强大的双向发育能力，可以产生多个胚胎和胚胎外细胞系。从机械上讲，剪接体抑制导致多能基因广泛的剪接抑制，而含有少量短内含子的全能基因则被有效地剪接和转录激活。我们的研究为捕获和维持全能干细胞提供了一种方法。

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来源期刊

Journal of Chemical Theory and Computation 化学-物理：原子、分子和化学物理

CiteScore

9.90

自引率

16.40%

发文量

568

审稿时长

1 months

期刊介绍： The Journal of Chemical Theory and Computation invites new and original contributions with the understanding that, if accepted, they will not be published elsewhere. Papers reporting new theories, methodology, and/or important applications in quantum electronic structure, molecular dynamics, and statistical mechanics are appropriate for submission to this Journal. Specific topics include advances in or applications of ab initio quantum mechanics, density functional theory, design and properties of new materials, surface science, Monte Carlo simulations, solvation models, QM/MM calculations, biomolecular structure prediction, and molecular dynamics in the broadest sense including gas-phase dynamics, ab initio dynamics, biomolecular dynamics, and protein folding. The Journal does not consider papers that are straightforward applications of known methods including DFT and molecular dynamics. The Journal favors submissions that include advances in theory or methodology with applications to compelling problems.