Literature DB >> 22822199

DNA and chromatin modification networks distinguish stem cell pluripotent ground states.

Jing Song1, Sudipto Saha, Giridharan Gokulrangan, Paul J Tesar, Rob M Ewing.   

Abstract

Pluripotent stem cells are capable of differentiating into all cell types of the body and therefore hold tremendous promise for regenerative medicine. Despite their widespread use in laboratories across the world, a detailed understanding of the molecular mechanisms that regulate the pluripotent state is currently lacking. Mouse embryonic (mESC) and epiblast (mEpiSC) stem cells are two closely related classes of pluripotent stem cells, derived from distinct embryonic tissues. Although both mESC and mEpiSC are pluripotent, these cell types show important differences in their properties suggesting distinct pluripotent ground states. To understand the molecular basis of pluripotency, we analyzed the nuclear proteomes of mESCs and mEpiSCs to identify protein networks that regulate their respective pluripotent states. Our study used label-free LC-MS/MS to identify and quantify 1597 proteins in embryonic and epiblast stem cell nuclei. Immunoblotting of a selected protein subset was used to confirm that key components of chromatin regulatory networks are differentially expressed in mESCs and mEpiSCs. Specifically, we identify differential expression of DNA methylation, ATP-dependent chromatin remodeling and nucleosome remodeling networks in mESC and mEpiSC nuclei. This study is the first comparative study of protein networks in cells representing the two distinct, pluripotent states, and points to the importance of DNA and chromatin modification processes in regulating pluripotency. In addition, by integrating our data with existing pluripotency networks, we provide detailed maps of protein networks that regulate pluripotency that will further both the fundamental understanding of pluripotency as well as efforts to reliably control the differentiation of these cells into functional cell fates.

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Year:  2012        PMID: 22822199      PMCID: PMC3494154          DOI: 10.1074/mcp.M111.011114

Source DB:  PubMed          Journal:  Mol Cell Proteomics        ISSN: 1535-9476            Impact factor:   5.911


  55 in total

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2.  Isolation and maintenance of mouse epiblast stem cells.

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3.  Maintenance of self-renewal ability of mouse embryonic stem cells in the absence of DNA methyltransferases Dnmt1, Dnmt3a and Dnmt3b.

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4.  Isolation of epiblast stem cells from preimplantation mouse embryos.

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Review 5.  Chromatin remodelling during development.

Authors:  Lena Ho; Gerald R Crabtree
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Authors:  Benjamin L Kidder; Stephen Palmer; Jason G Knott
Journal:  Stem Cells       Date:  2009-02       Impact factor: 6.277

7.  BAF60a interacts with p53 to recruit the SWI/SNF complex.

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8.  Regulatory networks define phenotypic classes of human stem cell lines.

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Journal:  Cell       Date:  2008-03-21       Impact factor: 41.582

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Review 2.  Chromatin features and the epigenetic regulation of pluripotency states in ESCs.

Authors:  Wee-Wei Tee; Danny Reinberg
Journal:  Development       Date:  2014-06       Impact factor: 6.868

3.  Cdx2 efficiently induces trophoblast stem-like cells in naïve, but not primed, pluripotent stem cells.

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4.  PKC inhibitors regulate stem cell self-renewal by regulating H3K27me3 and H3K9me3.

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5.  Cited2, a transcriptional modulator protein, regulates metabolism in murine embryonic stem cells.

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6.  RISC-mediated control of selected chromatin regulators stabilizes ground state pluripotency of mouse embryonic stem cells.

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Review 7.  The many faces of Pluripotency: in vitro adaptations of a continuum of in vivo states.

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