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Article

Cell-Cycle Control of Developmentally Regulated Transcription Factors Accounts for Heterogeneity in Human Pluripotent Cells

by Amar M. Singh; James Chappell; Robert Trost; Li Lin; Tao Wang; Jie Tang; Hao Wu; Shaying Zhao; Peng Jin; Stephen Dalton

2013

Subjects
  • Chemistry, Biochemistry
  • Biology, Genetics
  • Biology, Bioinformatics
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Abstract:Close

Heterogeneity within pluripotent stem cell (PSC) populations is indicative of dynamic changes that occur when cells drift between different states. Although the role of metastability in PSCs is unclear, it appears to reflect heterogeneity in cell signaling. Using the Fucci cell-cycle indicator system, we show that elevated expression of developmental regulators in G1 is a major determinant of heterogeneity in human embryonic stem cells. Although signaling pathways remain active throughout the cell cycle, their contribution to heterogeneous gene expression is restricted to G1. Surprisingly, we identify dramatic changes in the levels of global 5-hydroxymethylcytosine, an unanticipated source of epigenetic heterogeneity that is tightly linked to cell-cycle progression and the expression of developmental regulators. When we evaluated gene ex pression in differentiating cells, we found that cell-cycle regulation of developmental regulators was maintained during lineage specification. Cell-cycle regulation of developmentally regulated transcription factors is therefore an inherent feature of the mechanisms underpinning differentiation.

Article

Ten-eleven translocation 2 interacts with forkhead box O3 and regulates adult neurogenesis

by Xuekun Li; Bing Yao; Li Chen; Yunhee Kang; Yujing Li; Yujing Cheng; Liping Lin; Li Lin; Zhiqin Wang; Mengli Wang; Feng Pan; Qing Dai; Wei Zhang; Hao Wu; Qiang Shu; Zhaohui Qin; Chuan He; Mingjiang Xu; Peng Jin

2017

Subjects
  • Biology, Biostatistics
  • Biology, Bioinformatics
  • Biology, Genetics
  • File Download
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Abstract:Close

Emerging evidence suggests that active DNA demethylation machinery plays important epigenetic roles in mammalian adult neurogenesis; however, the precise molecular mechanisms and critical functional players of DNA demethylation in this process remain largely unexplored. Ten-eleven translocation (Tet) proteins convert 5-methylcytosine (5mC) to 5-hydroxymethylcytosine (5hmC) and its downstream derivatives. Here we show that 5hmC is elevated during the differentiation of adult neural stem cells (aNSCs), and Tet2 is primarily responsible for modulating 5hmC dynamics. Depletion of Tet2 leads to increased aNSC proliferation and reduced differentiation in vitro and in vivo. Genome-wide transcriptional analyses reveal important epigenetic roles of Tet2 in maintaining the transcriptome landscape related to neurogenesis. Mechanistically, transcription factor forkhead box O3 (Foxo3a) physically interacts with Tet2 and regulates the expression of genes related to aNSC proliferation. These data together establish an important role for the Tet2-Foxo3a axis in epigenetically regulating critical genes in aNSCs during adult neurogenesis.
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