Comprehensive profiling reveals mechanisms of SOX2-mediated cell fate specification in human ESCs and NPCs

被引:0
|
作者
Chenlin Zhou
Xiaoqin Yang
Yiyang Sun
Hongyao Yu
Yong Zhang
Ying Jin
机构
[1] Key Laboratory of Stem Cell Biology,
[2] CAS Center for Excellence in Molecular Cell Science,undefined
[3] Institute of Health Sciences,undefined
[4] Shanghai Institutes for Biological Sciences,undefined
[5] Chinese Academy of Sciences/Shanghai JiaoTong University School of Medicine,undefined
[6] School of Life Sciences and Technology,undefined
[7] Tongji University,undefined
[8] Laboratory of Molecular Developmental Biology,undefined
[9] Shanghai JiaoTong University School of Medicine,undefined
[10] University of Chinese Academy of Sciences,undefined
来源
Cell Research | 2016年 / 26卷
关键词
SOX2; hESCs; hNPCs; Wnt; H2A.Z;
D O I
暂无
中图分类号
学科分类号
摘要
SOX2 is a key regulator of multiple types of stem cells, especially embryonic stem cells (ESCs) and neural progenitor cells (NPCs). Understanding the mechanism underlying the function of SOX2 is of great importance for realizing the full potential of ESCs and NPCs. Here, through genome-wide comparative studies, we show that SOX2 executes its distinct functions in human ESCs (hESCs) and hESC-derived NPCs (hNPCs) through cell type- and stage-dependent transcription programs. Importantly, SOX2 suppresses non-neural lineages in hESCs and regulates neurogenesis from hNPCs by inhibiting canonical Wnt signaling. In hESCs, SOX2 achieves such inhibition by direct transcriptional regulation of important Wnt signaling modulators, WLS and SFRP2. Moreover, SOX2 ensures pluripotent epigenetic landscapes via interacting with histone variant H2A.Z and recruiting polycomb repressor complex 2 to poise developmental genes in hESCs. Together, our results advance our understanding of the mechanism by which cell type-specific transcription factors control lineage-specific gene expression programs and specify cell fate.
引用
收藏
页码:171 / 189
页数:18
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