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Literature DB >> 19106109

p53 Oligomerization is essential for its C-terminal lysine acetylation.

Yoko Itahana¹, Hengming Ke, Yanping Zhang.

Abstract

Acetylation of multiple lysine residues in the p53 plays critical roles in the protein stability and transcriptional activity of p53. To better understand how p53 acetylation is regulated, we generated a number of p53 mutants and examined acetylation of each mutant in transfected cells. We found that p53 mutants that are defective in tetramer formation are also defective in C-terminal lysine residue acetylation. Consistently, we found that several cancer-derived p53 mutants that bear mutations in the tetramerization domain cannot form oligomers and are defective in C-terminal lysine acetylation, and these mutants are inactive in p21 transactivation. We demonstrated that the acetyltransferase p300 interacts with and promotes acetylation of wild-type p53 but not with any of the artificially generated or human cancer-derived p53 mutants that are defective in oligomerization. These results, combined with a computer-aided crystal structure analysis, suggest a model in which p53 oligomerization precedes its acetylation by providing docking sites for acetyltransferases.

Entities: Chemical

Mesh：

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Year: 2008 PMID： 19106109 PMCID： PMC2643511 DOI： 10.1074/jbc.M805696200

Source DB: PubMed Journal: J Biol Chem ISSN： 0021-9258 Impact factor: 5.157

38 in total

1. Acetylation of p53 activates transcription through recruitment of coactivators/histone acetyltransferases.

Authors: N A Barlev; L Liu; N H Chehab; K Mansfield; K G Harris; T D Halazonetis; S L Berger
Journal: Mol Cell Date: 2001-12 Impact factor: 17.970

2. Multiple lysine mutations in the C-terminal domain of p53 interfere with MDM2-dependent protein degradation and ubiquitination.

Authors: S Nakamura; J A Roth; T Mukhopadhyay
Journal: Mol Cell Biol Date: 2000-12 Impact factor: 4.272

3. Mechanism of folding and assembly of a small tetrameric protein domain from tumor suppressor p53.

Authors: M G Mateu; M M Sánchez Del Pino; A R Fersht
Journal: Nat Struct Biol Date: 1999-02

4. Phosphorylation of serine 392 stabilizes the tetramer formation of tumor suppressor protein p53.

Authors: K Sakaguchi; H Sakamoto; M S Lewis; C W Anderson; J W Erickson; E Appella; D Xie
Journal: Biochemistry Date: 1997-08-19 Impact factor: 3.162

5. Mechanistic insights into maintenance of high p53 acetylation by PTEN.

Authors: Andrew G Li; Landon G Piluso; Xin Cai; Gang Wei; William R Sellers; Xuan Liu
Journal: Mol Cell Date: 2006-08 Impact factor: 17.970

6. C-terminal modifications regulate MDM2 dissociation and nuclear export of p53.

Authors: Stephanie Carter; Oliver Bischof; Anne Dejean; Karen H Vousden
Journal: Nat Cell Biol Date: 2007-03-18 Impact factor: 28.824

7. Acetylation is indispensable for p53 activation.

Authors: Yi Tang; Wenhui Zhao; Yue Chen; Yingming Zhao; Wei Gu
Journal: Cell Date: 2008-05-16 Impact factor: 41.582

8. DNA damage activates p53 through a phosphorylation-acetylation cascade.

Authors: K Sakaguchi; J E Herrera; S Saito; T Miki; M Bustin; A Vassilev; C W Anderson; E Appella
Journal: Genes Dev Date: 1998-09-15 Impact factor: 11.361

9. Crystal structure of the tetramerization domain of the p53 tumor suppressor at 1.7 angstroms.

Authors: P D Jeffrey; S Gorina; N P Pavletich
Journal: Science Date: 1995-03-10 Impact factor: 47.728

10. Li-Fraumeni and related syndromes: correlation between tumor type, family structure, and TP53 genotype.

Authors: Magali Olivier; David E Goldgar; Nayanta Sodha; Hiroko Ohgaki; Paul Kleihues; Pierre Hainaut; Rosalind A Eeles
Journal: Cancer Res Date: 2003-10-15 Impact factor: 12.701

41 in total

1. Planck-Benzinger thermal work function: thermodynamic characterization of the carboxy-terminus of p53 peptide fragments.

Authors: Paul W Chun; Marc S Lewis
Journal: Protein J Date: 2010-11 Impact factor: 2.371

2. The Protein Acetyltransferase PatZ from Escherichia coli Is Regulated by Autoacetylation-induced Oligomerization.

Authors: Teresa de Diego Puente; Julia Gallego-Jara; Sara Castaño-Cerezo; Vicente Bernal Sánchez; Vanesa Fernández Espín; José García de la Torre; Arturo Manjón Rubio; Manuel Cánovas Díaz
Journal: J Biol Chem Date: 2015-08-06 Impact factor: 5.157

3. Cancer-associated p53 tetramerization domain mutants: quantitative analysis reveals a low threshold for tumor suppressor inactivation.

Authors: Rui Kamada; Takao Nomura; Carl W Anderson; Kazuyasu Sakaguchi
Journal: J Biol Chem Date: 2010-10-26 Impact factor: 5.157

p53 Oligomerization is essential for its C-terminal lysine acetylation.

1. Acetylation of p53 activates transcription through recruitment of coactivators/histone acetyltransferases.

2. Multiple lysine mutations in the C-terminal domain of p53 interfere with MDM2-dependent protein degradation and ubiquitination.

3. Mechanism of folding and assembly of a small tetrameric protein domain from tumor suppressor p53.

4. Phosphorylation of serine 392 stabilizes the tetramer formation of tumor suppressor protein p53.

5. Mechanistic insights into maintenance of high p53 acetylation by PTEN.

6. C-terminal modifications regulate MDM2 dissociation and nuclear export of p53.

7. Acetylation is indispensable for p53 activation.

8. DNA damage activates p53 through a phosphorylation-acetylation cascade.

9. Crystal structure of the tetramerization domain of the p53 tumor suppressor at 1.7 angstroms.

10. Li-Fraumeni and related syndromes: correlation between tumor type, family structure, and TP53 genotype.

1. Planck-Benzinger thermal work function: thermodynamic characterization of the carboxy-terminus of p53 peptide fragments.

2. The Protein Acetyltransferase PatZ from Escherichia coli Is Regulated by Autoacetylation-induced Oligomerization.

3. Cancer-associated p53 tetramerization domain mutants: quantitative analysis reveals a low threshold for tumor suppressor inactivation.

4. Extensive post-translational modification of active and inactivated forms of endogenous p53.

5. Structural evolution of p53, p63, and p73: implication for heterotetramer formation.

6. A new era of studying p53-mediated transcription activation.

7. The E3 ubiquitin protein ligase HERC2 modulates the activity of tumor protein p53 by regulating its oligomerization.

8. p53 oligomerization status modulates cell fate decisions between growth, arrest and apoptosis.

9. p53 sumoylation: mechanistic insights from reconstitution studies.

10. Hypoxia inactivates the VHL tumor suppressor through PIASy-mediated SUMO modification.