Literature DB >> 19449340

Changing nuclear landscape and unique PML structures during early epigenetic transitions of human embryonic stem cells.

John T Butler1, Lisa L Hall, Kelly P Smith, Jeanne B Lawrence.   

Abstract

The complex nuclear structure of somatic cells is important to epigenomic regulation, yet little is known about nuclear organization of human embryonic stem cells (hESC). Here we surveyed several nuclear structures in pluripotent and transitioning hESC. Observations of centromeres, telomeres, SC35 speckles, Cajal Bodies, lamin A/C and emerin, nuclear shape and size demonstrate a very different "nuclear landscape" in hESC. This landscape is remodeled during a brief transitional window, concomitant with or just prior to differentiation onset. Notably, hESC initially contain abundant signal for spliceosome assembly factor, SC35, but lack discrete SC35 domains; these form as cells begin to specialize, likely reflecting cell-type specific genomic organization. Concomitantly, nuclear size increases and shape changes as lamin A/C and emerin incorporate into the lamina. During this brief window, hESC exhibit dramatically different PML-defined structures, which in somatic cells are linked to gene regulation and cancer. Unlike the numerous, spherical somatic PML bodies, hES cells often display approximately 1-3 large PML structures of two morphological types: long linear "rods" or elaborate "rosettes", which lack substantial SUMO-1, Daxx, and Sp100. These occur primarily between Day 0-2 of differentiation and become rare thereafter. PML rods may be "taut" between other structures, such as centromeres, but clearly show some relationship with the lamina, where PML often abuts or fills a "gap" in early lamin A/C staining. Findings demonstrate that pluripotent hES cells have a markedly different overall nuclear architecture, remodeling of which is linked to early epigenomic programming and involves formation of unique PML-defined structures. 2009 Wiley-Liss, Inc.

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Year:  2009        PMID: 19449340      PMCID: PMC2937361          DOI: 10.1002/jcb.22183

Source DB:  PubMed          Journal:  J Cell Biochem        ISSN: 0730-2312            Impact factor:   4.429


  44 in total

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3.  Epigenome and chromatin structure in human embryonic stem cells undergoing differentiation.

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7.  Large-scale identification of mammalian proteins localized to nuclear sub-compartments.

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8.  The transcription coactivator CBP is a dynamic component of the promyelocytic leukemia nuclear body.

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10.  Clustering of multiple specific genes and gene-rich R-bands around SC-35 domains: evidence for local euchromatic neighborhoods.

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  34 in total

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4.  Gene expression, chromosome position and lamin A/C mutations.

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5.  The nuclear periphery of embryonic stem cells is a transcriptionally permissive and repressive compartment.

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6.  Human cytomegalovirus infection of human embryonic stem cell-derived primitive neural stem cells is restricted at several steps but leads to the persistence of viral DNA.

Authors:  Jean-Philippe Belzile; Thomas J Stark; Gene W Yeo; Deborah H Spector
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Review 7.  Sizing and shaping the nucleus: mechanisms and significance.

Authors:  Predrag Jevtić; Lisa J Edens; Lidija D Vuković; Daniel L Levy
Journal:  Curr Opin Cell Biol       Date:  2014-02-04       Impact factor: 8.382

Review 8.  Nuclear hubs built on RNAs and clustered organization of the genome.

Authors:  Kelly P Smith; Lisa L Hall; Jeanne B Lawrence
Journal:  Curr Opin Cell Biol       Date:  2020-04-04       Impact factor: 8.382

Review 9.  The role of PML in hematopoietic and leukemic stem cell maintenance.

Authors:  Fumio Nakahara; Cary N Weiss; Keisuke Ito
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10.  Cytoplasmic localization of PML particles in laminopathies.

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Journal:  Histochem Cell Biol       Date:  2012-08-25       Impact factor: 4.304

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