Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 Mitotic phosphorylation prevents the binding of HMGN proteins to chromatin.

Literature DB >> 11438671

Mitotic phosphorylation prevents the binding of HMGN proteins to chromatin.

M Prymakowska-Bosak¹, T Misteli, J E Herrera, H Shirakawa, Y Birger, S Garfield, M Bustin.

Abstract

Condensation of the chromatin fiber and transcriptional inhibition during mitosis is associated with the redistribution of many DNA- and chromatin-binding proteins, including members of the high-mobility-group N (HMGN) family. Here we study the mechanism governing the organization of HMGN proteins in mitosis. Using site-specific antibodies and quantitative gel analysis with proteins extracted from synchronized HeLa cells, we demonstrate that, during mitosis, the conserved serine residues in the nucleosomal binding domain (NBD) of this protein family are highly and specifically phosphorylated. Nucleosome mobility shift assays with both in vitro-phosphorylated proteins and with point mutants bearing negative charges in the NBD demonstrate that the negative charge abolishes the ability of the proteins to bind to nucleosomes. Fluorescence loss of photobleaching demonstrates that, in living cells, the negative charge in the NBD increases the intranuclear mobility of the protein and significantly decreases the relative time that it is bound to chromatin. Expression of wild-type and mutant proteins in HmgN1(-/-) cells indicates that the negatively charged protein is not bound to chromosomes. We conclude that during mitosis the NBD of HMGN proteins is highly phosphorylated and that this modification regulates the interaction of the proteins with chromatin.

Entities: Chemical Disease Gene Species

Mesh：

Substances：

Year: 2001 PMID： 11438671 PMCID： PMC87241 DOI： 10.1128/MCB.21.15.5169-5178.2001

Source DB: PubMed Journal: Mol Cell Biol ISSN： 0270-7306 Impact factor: 4.272

61 in total

1. Nucleosome core binding region of chromosomal protein HMG-17 acts as an independent functional domain.

Authors: M P Crippa; P J Alfonso; M Bustin
Journal: J Mol Biol Date: 1992-11-20 Impact factor: 5.469

2. Mitotic phosphorylation of the Oct-1 homeodomain and regulation of Oct-1 DNA binding activity.

Authors: N Segil; S B Roberts; N Heintz
Journal: Science Date: 1991-12-20 Impact factor: 47.728

3. A critical appraisal of synchronization methods applied to achieve maximal enrichment of HeLa cells in specific cell cycle phases.

Authors: M Knehr; M Poppe; M Enulescu; W Eickelbaum; M Stoehr; D Schroeter; N Paweletz
Journal: Exp Cell Res Date: 1995-04 Impact factor: 3.905

4. Analysis of the binding of high mobility group protein 17 to the nucleosome core particle by 1H NMR spectroscopy.

Authors: G R Cook; M Minch; G P Schroth; E M Bradbury
Journal: J Biol Chem Date: 1989-01-25 Impact factor: 5.157

5. Displacement of sequence-specific transcription factors from mitotic chromatin.

Authors: M A Martínez-Balbás; A Dey; S K Rabindran; K Ozato; C Wu
Journal: Cell Date: 1995-10-06 Impact factor: 41.582

6. Homodimers of chromosomal proteins HMG-14 and HMG-17 in nucleosome cores.

Authors: Y V Postnikov; L Trieschmann; A Rickers; M Bustin
Journal: J Mol Biol Date: 1995-09-29 Impact factor: 5.469

7. Two classes of proteins dependent on either the presence or absence of thyroid hormone for interaction with the thyroid hormone receptor.

Authors: J W Lee; H S Choi; J Gyuris; R Brent; D D Moore
Journal: Mol Endocrinol Date: 1995-02

8. The footprint of chromosomal proteins HMG-14 and HMG-17 on chromatin subunits.

Authors: P J Alfonso; M P Crippa; J J Hayes; M Bustin
Journal: J Mol Biol Date: 1994-02-11 Impact factor: 5.469

9. The cooperative binding of chromosomal protein HMG-14 to nucleosome cores is reduced by single point mutations in the nucleosomal binding domain.

Authors: Y V Postnikov; D A Lehn; R C Robinson; F K Friedman; J Shiloach; M Bustin
Journal: Nucleic Acids Res Date: 1994-10-25 Impact factor: 16.971

10. A mitogen- and anisomycin-stimulated kinase phosphorylates HMG-14 in its basic amino-terminal domain in vivo and on isolated mononucleosomes.

Authors: M J Barratt; C A Hazzalin; N Zhelev; L C Mahadevan
Journal: EMBO J Date: 1994-10-03 Impact factor: 11.598

39 in total

1. Competition between histone H1 and HMGN proteins for chromatin binding sites.

Authors: Frédéric Catez; David T Brown; Tom Misteli; Michael Bustin
Journal: EMBO Rep Date: 2002-07-15 Impact factor: 8.807

2. Global nature of dynamic protein-chromatin interactions in vivo: three-dimensional genome scanning and dynamic interaction networks of chromatin proteins.

Authors: Robert D Phair; Paola Scaffidi; Cem Elbi; Jaromíra Vecerová; Anup Dey; Keiko Ozato; David T Brown; Gordon Hager; Michael Bustin; Tom Misteli
Journal: Mol Cell Biol Date: 2004-07 Impact factor: 4.272

10. cAMP-response element-binding protein (CREB) controls MSK1-mediated phosphorylation of histone H3 at the c-fos promoter in vitro.

Authors: Miho Shimada; Tomoyoshi Nakadai; Aya Fukuda; Koji Hisatake
Journal: J Biol Chem Date: 2010-01-20 Impact factor: 5.157

Mitotic phosphorylation prevents the binding of HMGN proteins to chromatin.

1. Nucleosome core binding region of chromosomal protein HMG-17 acts as an independent functional domain.

2. Mitotic phosphorylation of the Oct-1 homeodomain and regulation of Oct-1 DNA binding activity.

3. A critical appraisal of synchronization methods applied to achieve maximal enrichment of HeLa cells in specific cell cycle phases.

4. Analysis of the binding of high mobility group protein 17 to the nucleosome core particle by 1H NMR spectroscopy.

5. Displacement of sequence-specific transcription factors from mitotic chromatin.

6. Homodimers of chromosomal proteins HMG-14 and HMG-17 in nucleosome cores.

7. Two classes of proteins dependent on either the presence or absence of thyroid hormone for interaction with the thyroid hormone receptor.

8. The footprint of chromosomal proteins HMG-14 and HMG-17 on chromatin subunits.

9. The cooperative binding of chromosomal protein HMG-14 to nucleosome cores is reduced by single point mutations in the nucleosomal binding domain.

10. A mitogen- and anisomycin-stimulated kinase phosphorylates HMG-14 in its basic amino-terminal domain in vivo and on isolated mononucleosomes.

1. Competition between histone H1 and HMGN proteins for chromatin binding sites.

2. Global nature of dynamic protein-chromatin interactions in vivo: three-dimensional genome scanning and dynamic interaction networks of chromatin proteins.

3. Cell cycle-dependent binding of HMGN proteins to chromatin.

4. Delineation of the protein module that anchors HMGN proteins to nucleosomes in the chromatin of living cells.

5. HMGN2 inducibly binds a novel transactivation domain in nuclear PRLr to coordinate Stat5a-mediated transcription.

Review 6. High mobility group proteins and their post-translational modifications.

Review 7. The dynamics of HMG protein-chromatin interactions in living cells.

8. Sodium arsenite modulates histone acetylation, histone deacetylase activity and HMGN protein dynamics in human cells.

9. Increased tumorigenicity and sensitivity to ionizing radiation upon loss of chromosomal protein HMGN1.

10. cAMP-response element-binding protein (CREB) controls MSK1-mediated phosphorylation of histone H3 at the c-fos promoter in vitro.