Literature DB >> 21235343

SAF-A has a role in transcriptional regulation of Oct4 in ES cells through promoter binding.

Dzeneta Vizlin-Hodzic1, Helena Johansson, Jessica Ryme, Tomas Simonsson, Stina Simonsson.   

Abstract

Methodologies to reprogram somatic cells into patient-specific pluripotent cells, which could potentially be used in personalized drug discovery and cell replacement therapies, are currently under development. Oct4 activation is essential for successful reprogramming and pluripotency of embryonic stem (ES) cells, albeit molecular details of Oct4 activation are not completely understood. Here we report that endogenous SAF-A is involved in regulation of Oct4 expression, binds the Oct4 proximal promoter in ES cells, and dissociates from the promoter upon early differentiation induced by LIF withdrawal. Depletion of SAF-A decreases Oct4 expression even in the presence of LIF, and results in an increase of the mesodermal marker Brachyury. The overexpression of wild-type human SAF-A rescues the mouse knock-down phenotype and results in increased Oct4 level. We also demonstrate that endogenous SAF-A interacts with the C-terminal domain (CTD) of endogenous RNA polymerase II and that the interaction is independent of CTD phosphorylation and mRNA. Moreover, we show that SAF-A exist in complexes with transcription factors Sox2 and Oct4 as well as STAT3 in ES cells. The number of endogenous SAF-A:Oct4 and SAF-A:Sox2 complexes decreases upon LIF depletion. These discoveries allow us to propose a model for activation of Oct4 transcription.

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Year:  2011        PMID: 21235343      PMCID: PMC3030915          DOI: 10.1089/cell.2010.0075

Source DB:  PubMed          Journal:  Cell Reprogram        ISSN: 2152-4971            Impact factor:   1.987


  45 in total

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10.  Induction of pluripotent stem cells from adult human fibroblasts by defined factors.

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Journal:  Cell       Date:  2007-11-30       Impact factor: 41.582

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6.  SAF-A forms a complex with BRG1 and both components are required for RNA polymerase II mediated transcription.

Authors:  Dzeneta Vizlin-Hodzic; Rikard Runnberg; Jessica Ryme; Stina Simonsson; Tomas Simonsson
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Review 8.  Computational analysis of single-cell transcriptomics data elucidates the stabilization of Oct4 expression in the E3.25 mouse preimplantation embryo.

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9.  The long non-coding RNA Snhg3 is essential for mouse embryonic stem cell self-renewal and pluripotency.

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Review 10.  Functions of heterogeneous nuclear ribonucleoproteins in stem cell potency and differentiation.

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