Loss of Tet hydroxymethylase activity causes mouse embryonic stem cell differentiation bias and developmental defects.

IF 8 2区 生物学 Q1 BIOLOGY Science China Life Sciences Pub Date : 2024-10-01 Epub Date: 2024-07-05 DOI:10.1007/s11427-024-2631-x
Mengting Wang, Liping Wang, Yanxin Huang, Zhibin Qiao, Shanru Yi, Weina Zhang, Jing Wang, Guang Yang, Xinyu Cui, Xiaochen Kou, Yanhong Zhao, Hong Wang, Cizhong Jiang, Shaorong Gao, Jiayu Chen
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Abstract

The TET family is well known for active DNA demethylation and plays important roles in regulating transcription, the epigenome and development. Nevertheless, previous studies using knockdown (KD) or knockout (KO) models to investigate the function of TET have faced challenges in distinguishing its enzymatic and nonenzymatic roles, as well as compensatory effects among TET family members, which has made the understanding of the enzymatic role of TET not accurate enough. To solve this problem, we successfully generated mice catalytically inactive for specific Tet members (Tetm/m). We observed that, compared with the reported KO mice, mutant mice exhibited distinct developmental defects, including growth retardation, sex imbalance, infertility, and perinatal lethality. Notably, Tetm/m mouse embryonic stem cells (mESCs) were successfully established but entered an impaired developmental program, demonstrating extended pluripotency and defects in ectodermal differentiation caused by abnormal DNA methylation. Intriguingly, Tet3, traditionally considered less critical for mESCs due to its lower expression level, had a significant impact on the global hydroxymethylation, gene expression, and differentiation potential of mESCs. Notably, there were common regulatory regions between Tet1 and Tet3 in pluripotency regulation. In summary, our study provides a more accurate reference for the functional mechanism of Tet hydroxymethylase activity in mouse development and ESC pluripotency regulation.

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Tet 羟甲基化酶活性缺失会导致小鼠胚胎干细胞分化偏差和发育缺陷。
众所周知,TET家族具有活跃的DNA去甲基化作用,在调节转录、表观基因组和发育方面发挥着重要作用。然而,以往利用基因敲除(KD)或基因剔除(KO)模型研究 TET 功能的研究在区分其酶作用和非酶作用以及 TET 家族成员之间的代偿效应方面面临挑战,这使得对 TET 酶作用的认识不够准确。为了解决这个问题,我们成功培育出了对特定 TET 成员无催化作用的小鼠(Tetm/m)。我们观察到,与已报道的 KO 小鼠相比,突变小鼠表现出明显的发育缺陷,包括生长迟缓、性别失衡、不育和围产期致死。值得注意的是,Tetm/m小鼠胚胎干细胞(mESCs)成功建立,但进入了受损的发育程序,表现出DNA甲基化异常导致的多能性延长和外胚层分化缺陷。耐人寻味的是,传统上认为对 mESCs 不太关键的 Tet3 因其表达水平较低而对 mESCs 的全局羟甲基化、基因表达和分化潜能有显著影响。值得注意的是,Tet1 和 Tet3 在多能性调控方面存在共同的调控区域。总之,我们的研究为Tet羟甲基化酶活性在小鼠发育和ESC多能性调控中的功能机制提供了更准确的参考。
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来源期刊
CiteScore
15.10
自引率
8.80%
发文量
2907
审稿时长
3.2 months
期刊介绍: Science China Life Sciences is a scholarly journal co-sponsored by the Chinese Academy of Sciences and the National Natural Science Foundation of China, and it is published by Science China Press. The journal is dedicated to publishing high-quality, original research findings in both basic and applied life science research.
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