Literature DB >> 22572957

Dualistic function of Daxx at centromeric and pericentromeric heterochromatin in normal and stress conditions.

Viacheslav M Morozov1, Ekaterina V Gavrilova, Vasily V Ogryzko, Alexander M Ishov.   

Abstract

Nuclear structures ND10/PML NBs are linked to multiple processes, including the maintenance of intranuclear homeostasis by sequestering proteins into "nuclear depot." This function presumes release of proteins from PML NBs and their redistribution to the alternative, supposedly "active" locations, in response to the external stress application. To further investigate this nuclear depot function, we focused on the intranuclear distribution of protein Daxx that in normal conditions is mainly accumulated at PML NBs, and has a minor association with centromeres and pericentromeres (CEN/periCEN). Here we report that application of physiological Heat Shock (HS) changes this balance forcing very robust and reversible accumulation of Daxx on CEN/periCEN heterochromatin.   Heterochromatin architecture is essential for the proper orchestration of nuclear processes, while transcription from this part of genome is required for its maintenance. To understand functional consequences of Daxx deposition at CEN/periCEN, we tested for Daxx-dependency of heterochromatin transcription. Depletion of Daxx reduces accumulation of CEN RNA in normal conditions and periCEN RNA after HS application. Searching for the mechanism of Daxx-dependent regulation of heterochromatin transcription, we found that depletion of Daxx decreases incorporation of transcription-associated histone H3 variant, H3.3, into both CEN and periCEN. Surprisingly, HS-induced deposition of Daxx does not further elevate incorporation of H3.3 into CEN/periCEN that remained steady during stress and recovery. Instead, depletion of Daxx leads to HS-induced changes in the balance of epigenetic modifications at heterochromatin, most dramatically elevating levels of active H3K4Me2 modification at periCEN. We propose dualistic function of Daxx-containing complexes at CEN/periCEN: (1) regulation of H3.3 loading in normal conditions and (2) protection of epigenetic status upon stress-induced accumulation, thus collectively guarding epigenetic identity of CEN/periCEN heterochromatin.

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Year:  2012        PMID: 22572957      PMCID: PMC3414404          DOI: 10.4161/nucl.20180

Source DB:  PubMed          Journal:  Nucleus        ISSN: 1949-1034            Impact factor:   4.197


  44 in total

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Review 5.  PML NBs (ND10) and Daxx: from nuclear structure to protein function.

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Journal:  Front Biosci       Date:  2008-05-01

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Review 8.  RNAi-dependent formation of heterochromatin and its diverse functions.

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Review 9.  New functions for an old variant: no substitute for histone H3.3.

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10.  A transcriptomic analysis of human centromeric and pericentric sequences in normal and tumor cells.

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Journal:  Nucleic Acids Res       Date:  2009-08-31       Impact factor: 16.971

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  19 in total

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4.  Identification of protein complexes that bind to histone H3 combinatorial modifications using super-SILAC and weighted correlation network analysis.

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Review 5.  Molecular turnover, the H3.3 dilemma and organismal aging (hypothesis).

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6.  Dynamics of histone H3.3 deposition in proliferating and senescent cells reveals a DAXX-dependent targeting to PML-NBs important for pericentromeric heterochromatin organization.

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Review 7.  Constitutive heterochromatin formation and transcription in mammals.

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8.  CENP-B protects centromere chromatin integrity by facilitating histone deposition via the H3.3-specific chaperone Daxx.

Authors:  Viacheslav M Morozov; Serena Giovinazzi; Alexander M Ishov
Journal:  Epigenetics Chromatin       Date:  2017-12-22       Impact factor: 4.954

9.  The histone chaperone DAXX maintains the structural organization of heterochromatin domains.

Authors:  Lindsy M Rapkin; Kashif Ahmed; Stanimir Dulev; Ren Li; Hiroshi Kimura; Alexander M Ishov; David P Bazett-Jones
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10.  Inheritance of the CENP-A chromatin domain is spatially and temporally constrained at human centromeres.

Authors:  Justyne E Ross; Kaitlin Stimpson Woodlief; Beth A Sullivan
Journal:  Epigenetics Chromatin       Date:  2016-05-31       Impact factor: 4.954

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