Literature DB >> 25724006

De-regulated expression of the BRG1 chromatin remodeling factor in bone marrow mesenchymal stromal cells induces senescence associated with the silencing of NANOG and changes in the levels of chromatin proteins.

Tiziana Squillaro1, Valeria Severino, Nicola Alessio, Annarita Farina, Giovanni Di Bernardo, Marilena Cipollaro, Gianfranco Peluso, Angela Chambery, Umberto Galderisi.   

Abstract

Stem cells have a peculiar chromatin architecture that contributes to their unique properties, including uncommitted status, multi/pluripotency and self-renewal. We analyzed the effect of the de-regulation of the SWI/SNF chromatin remodeling complex in mesenchymal stromal cells (MSC) through the silencing and up-regulation of BRG1, which is the ATPase subunit of the complex. The altered expression of BRG1 promoted the senescence of MSC with suppression of the NANOG transcription, which is part of the transcriptional circuitry governing stem cell functions. To gain insight on the way NANOG was silenced, we evaluated how the de-regulated BRG1 expression affect the binding of activators and repressors on the NANOG promoter. We found 4 E2F binding motifs on NANOG promoter, which can be occupied by RB1 and RB2/P130. These are members of the retinoblastoma gene family. In MSC with a silenced BRG1, the relative binding of the 2 retinoblastoma proteins increased, and this was associated with the recruitment of DNMT1. This induced the methylation of CpG on the NANOG promoter. Opposingly, when a high level of BRG1 was present, the same E2F binding motifs were docking sites for BRG1, which induced chromatin compaction without CpG methylation but with increased histone deacetylation, associated with the presence of HDAC1 on E2F binding sites. Besides the sharp regulation of the NANOG expression, we evidenced, through proteomic analysis, that the de-regulation of the SWI/SNF function affected the expression of histones and other nuclear proteins involved in "nuclear architecture," suggesting that BRG1 may act as global regulator of gene expression.

Entities:  

Keywords:  mesenchymal stem cells; proteome; retinoblastoma; senescence

Mesh:

Substances:

Year:  2015        PMID: 25724006      PMCID: PMC4614278          DOI: 10.4161/15384101.2014.995053

Source DB:  PubMed          Journal:  Cell Cycle        ISSN: 1551-4005            Impact factor:   4.534


  52 in total

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Journal:  Mol Cell       Date:  2003-04       Impact factor: 17.970

Review 3.  Histone variants: deviants?

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4.  Core transcriptional regulatory circuitry in human embryonic stem cells.

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Journal:  Cell       Date:  2005-09-23       Impact factor: 41.582

Review 5.  Mesenchymal stem cells as trophic mediators.

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6.  Exit from G1 and S phase of the cell cycle is regulated by repressor complexes containing HDAC-Rb-hSWI/SNF and Rb-hSWI/SNF.

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7.  MethPrimer: designing primers for methylation PCRs.

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9.  Partial silencing of methyl cytosine protein binding 2 (MECP2) in mesenchymal stem cells induces senescence with an increase in damaged DNA.

Authors:  Tiziana Squillaro; Nicola Alessio; Marilena Cipollaro; Alessandra Renieri; Antonio Giordano; Umberto Galderisi
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10.  Replicative senescence of mesenchymal stem cells causes DNA-methylation changes which correlate with repressive histone marks.

Authors:  Anne Schellenberg; Qiong Lin; Herdit Schüler; Carmen M Koch; Sylvia Joussen; Bernd Denecke; Gudrun Walenda; Norbert Pallua; Christoph V Suschek; Martin Zenke; Wolfga Wagner
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Review 1.  ATP-dependent chromatin remodelers in ageing and age-related disorders.

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Review 2.  Epigenetic regulation in cell senescence.

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3.  Cyclic DNA remethylation following active demethylation at euchromatic regions in mouse embryonic stem cells.

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4.  SATB2-Nanog axis links age-related intrinsic changes of mesenchymal stem cells from craniofacial bone.

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5.  Chromatin remodeling gene ARID2 targets cyclin D1 and cyclin E1 to suppress hepatoma cell progression.

Authors:  Yujie Duan; Ling Tian; Qingzhu Gao; Li Liang; Wenlu Zhang; Yi Yang; Yaqiu Zheng; E Pan; Shengwei Li; Ni Tang
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Review 6.  Senescence in Mesenchymal Stem Cells: Functional Alterations, Molecular Mechanisms, and Rejuvenation Strategies.

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Review 7.  Mesenchymal Stem/Stromal Cell Senescence: Hallmarks, Mechanisms, and Combating Strategies.

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Review 8.  The Mechanism of Stem Cell Aging.

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9.  SMARCD1 regulates senescence-associated lipid accumulation in hepatocytes.

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Review 10.  Molecular Mechanisms Contributing to Mesenchymal Stromal Cell Aging.

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