Genome-wide CRISPR-KO Screen Uncovers mTORC1-Mediated Gsk3 Regulation in Naive Pluripotency Maintenance and Dissolution

Meng Li; Jason S.L. Yu; Katarzyna Tilgner; Swee Hoe Ong; Hiroko Koike-Yusa; Kosuke Yusa

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Genome-wide CRISPR-KO Screen Uncovers mTORC1-Mediated Gsk3 Regulation in Naive Pluripotency Maintenance and Dissolution

机译：全基因组CRISPR-KO筛查揭示了mTORC1介导的Gsk3调控在幼稚多能性维持和溶解中的作用

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Summary The genetic basis of naive pluripotency maintenance and loss is a central question in embryonic stem cell biology. Here, we deploy CRISPR-knockout-based screens in mouse embryonic stem cells to interrogate this question through a genome-wide, non-biased approach using the Rex1GFP reporter as a phenotypic readout. This highly sensitive and efficient method identified genes in diverse biological processes and pathways. We uncovered a key role for negative regulators of mTORC1 in maintenance and exit from naive pluripotency and provided an integrated account of how mTORC1 activity influences naive pluripotency through Gsk3. Our study therefore reinforces Gsk3 as the central node and provides a comprehensive, data-rich resource that will improve our understanding of mechanisms regulating pluripotency and stimulate avenues for further mechanistic studies.

机译：小结天真多能性维持和丧失的遗传基础是胚胎干细胞生物学中的一个核心问题。在这里，我们在小鼠胚胎干细胞中部署了基于CRISPR敲除的屏幕，通过使用Rex1GFP报告基因作为表型读数的全基因组，无偏倚的方法来询问这个问题。这种高度灵敏和有效的方法可以鉴定多种生物学过程和途径中的基因。我们发现了mTORC1负调节剂在维持和退出幼稚多能性中的关键作用，并提供了有关mTORC1活性如何通过Gsk3影响幼稚多能性的综合说明。因此，我们的研究加强了Gsk3作为中心节点的作用，并提供了一个全面的，数据丰富的资源，这将增进我们对调节多能性机制的理解，并为进一步的机理研究提供刺激途径。

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《Cell Reports》 |2018年第2期|共14页
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Meng Li; Jason S.L. Yu; Katarzyna Tilgner; Swee Hoe Ong; Hiroko Koike-Yusa; Kosuke Yusa;
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中图分类细胞生物学;
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1. Decoding pluripotency: Genetic screens to interrogate the acquisition, maintenance, and exit of pluripotency [J] . Li Qing V., Rosen Bess P., Huangfu Danwei Wiley interdisciplinary reviews. Systems biology and medicine . 2020,第1期

机译：解码多能性：遗传屏幕，用于询问多能性的获取，维护和退出
2. Identification of ALPPL2 as a Naive Pluripotent State-Specific Surface Protein Essential for Human Naive Pluripotency Regulation [J] . Yan Bi, Zhifen Tu, Yanping Zhang, Cell Reports . 2020,第11期

机译：鉴定AlPPL2作为人幼稚多能性调节的天真多能状态特异性表面蛋白质
3. Pten-mediated Gsk3β modulates the na?ve pluripotency maintenance in embryonic stem cells [J] . Wuming Wang, Gang Lu, Xianwei Su, Cell death & disease. . 2020,第2期

机译：PTEN介导的GSK3β在胚胎干细胞中调节Na ve多能性维持
4. Biological Networks Governing the Acquisition, Maintenance, and Dissolution of Pluripotency: Insights from Functional Genomics Approaches [C] . Kevin Andrew Uy Gonzales, Huck-Hui Ng Cold Spring Harbor Symposium on Quantitative Biology . 2015

机译：有关多能性的收购，维护和解溶解的生物网络：功能基因组学方法的见解
5. Regulation of differentiation and the maintenance of pluripotency in embryonic stem cells by beta-catenin. [D] . Otero, Jose Javier. 2005

机译：β-catenin调节胚胎干细胞的分化并维持多能性。
6. Genome-wide CRISPR-KO Screen Uncovers mTORC1-Mediated Gsk3 Regulation in Naive Pluripotency Maintenance and Dissolution [O] . Meng Li, Jason S.L. Yu, Katarzyna Tilgner, -1

机译：全基因组CRISPR-KO筛查揭示了mTORC1介导的Gsk3调节在幼稚多能性维持和溶解中的作用
7. Genome-wide CRISPR-KO Screen Uncovers mTORC1-Mediated Gsk3 Regulation in Naive Pluripotency Maintenance and Dissolution [O] . Meng Li, Jason S.L. Yu, Katarzyna Tilgner, 2018

机译：基因组 - 宽CRISPR-KO筛网在幼稚多能性维护和溶解中发现MTORC1介导的GSK3调节

Genome-wide CRISPR-KO Screen Uncovers mTORC1-Mediated Gsk3 Regulation in Naive Pluripotency Maintenance and Dissolution

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