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LIN28 coordinately promotes nucleolar/ribosomal functions and represses the 2C-like transcriptional program in pluripotent stem cells

林28 生物 核糖体生物发生 核仁 细胞生物学 重编程 胚胎干细胞 诱导多能干细胞 干细胞 核仁素 分子生物学 核糖核酸 细胞 遗传学 核糖体 基因 细胞质
作者
Zhen Sun,Hua Yu,Jing Zhao,Tianyu Tan,Hongru Pan,Yuqing Zhu,Lang Chen,Cheng Zhang,Li Zhang,Anhua Lei,Yuyan Xu,Xianju Bi,Xin Huang,Bo Gao,Long Wang,Cristina Correia,Ming Chen,Qiming Sun,Yu Feng,Li Shen,Hao Wu,Jianlong Wang,Xiaohua Shen,George Q. Daley,Hu Li,Jin Zhang
出处
期刊:Protein & Cell [Springer Nature]
卷期号:13 (7): 490-512 被引量:28
标识
DOI:10.1007/s13238-021-00864-5
摘要

LIN28 is an RNA binding protein with important roles in early embryo development, stem cell differentiation/reprogramming, tumorigenesis and metabolism. Previous studies have focused mainly on its role in the cytosol where it interacts with Let-7 microRNA precursors or mRNAs, and few have addressed LIN28's role within the nucleus. Here, we show that LIN28 displays dynamic temporal and spatial expression during murine embryo development. Maternal LIN28 expression drops upon exit from the 2-cell stage, and zygotic LIN28 protein is induced at the forming nucleolus during 4-cell to blastocyst stage development, to become dominantly expressed in the cytosol after implantation. In cultured pluripotent stem cells (PSCs), loss of LIN28 led to nucleolar stress and activation of a 2-cell/4-cell-like transcriptional program characterized by the expression of endogenous retrovirus genes. Mechanistically, LIN28 binds to small nucleolar RNAs and rRNA to maintain nucleolar integrity, and its loss leads to nucleolar phase separation defects, ribosomal stress and activation of P53 which in turn binds to and activates 2C transcription factor Dux. LIN28 also resides in a complex containing the nucleolar factor Nucleolin (NCL) and the transcriptional repressor TRIM28, and LIN28 loss leads to reduced occupancy of the NCL/TRIM28 complex on the Dux and rDNA loci, and thus de-repressed Dux and reduced rRNA expression. Lin28 knockout cells with nucleolar stress are more likely to assume a slowly cycling, translationally inert and anabolically inactive state, which is a part of previously unappreciated 2C-like transcriptional program. These findings elucidate novel roles for nucleolar LIN28 in PSCs, and a new mechanism linking 2C program and nucleolar functions in PSCs and early embryo development.
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