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Literature DB >> 12374749

SSRP1 functions as a co-activator of the transcriptional activator p63.

Shelya X Zeng¹, Mu-Shui Dai, David M Keller, Hua Lu.

Abstract

The p53 homolog p63 is a transcriptional activator. Here, we describe the identification of an HMG1-like protein SSRP1 as a co-activator of p63. Over expression of wild-type, but not deletion mutant, SSRP1 remarkably enhanced p63gamma-dependent luciferase activity, G1 arrest, apoptosis and expression of endogenous PIG3, p21(Waf1/cip1) and MDM2 in human p53-deficient lung carcinoma H1299 cells and mouse embryonic fibroblasts. Also, SSRP1 interacted to p63gamma in vitro and in cells, and resided with p63gamma at the p53-responsive DNA element sites of the cellular endogenous MDM2 and p21(Waf1/cip1) promoters. Moreover, N-terminus-deleted p63 (DeltaN-p63) bound to neither SSRP1 nor its central domain in vitro. Accordingly, SSRP1 was unable to stimulate DeltaN-p63-mediated residual luciferase activity and apoptosis in cells. Finally, the ectopic expression of the central p63-binding domain of SSRP1 inhibited p63-dependent transcription in cells. Thus, these results suggest that SSRP1 stimulates p63 activity by associating with this activator at the promoter.

Entities: Disease Gene Species

Mesh：

Substances：

Year: 2002 PMID： 12374749 PMCID： PMC129072 DOI： 10.1093/emboj/cdf540

Source DB: PubMed Journal: EMBO J ISSN： 0261-4189 Impact factor: 11.598

55 in total

1. DNA damage-dependent acetylation of p73 dictates the selective activation of apoptotic target genes.

Authors: Antonio Costanzo; Paola Merlo; Natalia Pediconi; Marcella Fulco; Vittorio Sartorelli; Philip A Cole; Giulia Fontemaggi; Maurizio Fanciulli; Louis Schiltz; Giovanni Blandino; Clara Balsano; Massimo Levrero
Journal: Mol Cell Date: 2002-01 Impact factor: 17.970

Review 2. p53 family update: p73 and p63 develop their own identities.

Authors: M S Irwin; W G Kaelin
Journal: Cell Growth Differ Date: 2001-07

3. p63 and p73 are required for p53-dependent apoptosis in response to DNA damage.

Authors: Elsa R Flores; Kenneth Y Tsai; Denise Crowley; Shomit Sengupta; Annie Yang; Frank McKeon; Tyler Jacks
Journal: Nature Date: 2002-04-04 Impact factor: 49.962

Review 4. Commitment and activation at pol II promoters: a tail of protein-protein interactions.

Authors: B Lewin
Journal: Cell Date: 1990-06-29 Impact factor: 41.582

5. Synergistic activation of transcription by CBP and p53.

Authors: W Gu; X L Shi; R G Roeder
Journal: Nature Date: 1997-06-19 Impact factor: 49.962

6. High mobility group proteins 1 and 2 stimulate binding of a specific transcription factor to the adenovirus major late promoter.

Authors: F Watt; P L Molloy
Journal: Nucleic Acids Res Date: 1988-02-25 Impact factor: 16.971

7. Tissue specific expression of p53 target genes suggests a key role for KILLER/DR5 in p53-dependent apoptosis in vivo.

Authors: T F Burns; E J Bernhard; W S El-Deiry
Journal: Oncogene Date: 2001-08-02 Impact factor: 9.867

8. Differential chromatin association and nucleosome binding of the maize HMGA, HMGB, and SSRP1 proteins.

Authors: J Lichota; K D Grasser
Journal: Biochemistry Date: 2001-07-03 Impact factor: 3.162

9. Interaction of FACT, SSRP1, and the high mobility group (HMG) domain of SSRP1 with DNA damaged by the anticancer drug cisplatin.

Authors: A T Yarnell; S Oh; D Reinberg; S J Lippard
Journal: J Biol Chem Date: 2001-05-08 Impact factor: 5.157

10. LEF-1, a gene encoding a lymphoid-specific protein with an HMG domain, regulates T-cell receptor alpha enhancer function [corrected].

Authors: A Travis; A Amsterdam; C Belanger; R Grosschedl
Journal: Genes Dev Date: 1991-05 Impact factor: 11.361

37 in total

1. Autoregulatory suppression of c-Myc by miR-185-3p.

Authors: Jun-Ming Liao; Hua Lu
Journal: J Biol Chem Date: 2011-08-08 Impact factor: 5.157

2. SAK, a new polo-like kinase, is transcriptionally repressed by p53 and induces apoptosis upon RNAi silencing.

Authors: Jun Li; Mingjia Tan; Ling Li; Deepika Pamarthy; Theodore S Lawrence; Yi Sun
Journal: Neoplasia Date: 2005-04 Impact factor: 5.715

3. Insights into gene expression changes impacting B-cell transformation: cross-species microarray analysis of bovine leukemia virus tax-responsive genes in ovine B cells.

Authors: Pavel Klener; Maud Szynal; Yvette Cleuter; Makram Merimi; Hugues Duvillier; Françoise Lallemand; Claude Bagnis; Philip Griebel; Christos Sotiriou; Arsène Burny; Philippe Martiat; Anne Van den Broeke
Journal: J Virol Date: 2006-02 Impact factor: 5.103

SSRP1 functions as a co-activator of the transcriptional activator p63.

1. DNA damage-dependent acetylation of p73 dictates the selective activation of apoptotic target genes.

Review 2. p53 family update: p73 and p63 develop their own identities.

3. p63 and p73 are required for p53-dependent apoptosis in response to DNA damage.

Review 4. Commitment and activation at pol II promoters: a tail of protein-protein interactions.

5. Synergistic activation of transcription by CBP and p53.

6. High mobility group proteins 1 and 2 stimulate binding of a specific transcription factor to the adenovirus major late promoter.

7. Tissue specific expression of p53 target genes suggests a key role for KILLER/DR5 in p53-dependent apoptosis in vivo.

8. Differential chromatin association and nucleosome binding of the maize HMGA, HMGB, and SSRP1 proteins.

9. Interaction of FACT, SSRP1, and the high mobility group (HMG) domain of SSRP1 with DNA damaged by the anticancer drug cisplatin.

10. LEF-1, a gene encoding a lymphoid-specific protein with an HMG domain, regulates T-cell receptor alpha enhancer function [corrected].

1. Autoregulatory suppression of c-Myc by miR-185-3p.

2. SAK, a new polo-like kinase, is transcriptionally repressed by p53 and induces apoptosis upon RNAi silencing.

3. Insights into gene expression changes impacting B-cell transformation: cross-species microarray analysis of bovine leukemia virus tax-responsive genes in ovine B cells.

4. MDMX promotes proteasomal turnover of p21 at G1 and early S phases independently of, but in cooperation with, MDM2.

5. 14-3-3gamma binds to MDMX that is phosphorylated by UV-activated Chk1, resulting in p53 activation.

Review 6. Plant proteins containing high mobility group box DNA-binding domains modulate different nuclear processes.

7. SUMOylation of hnRNP-K is required for p53-mediated cell-cycle arrest in response to DNA damage.

8. IκB kinase β (IKKβ) inhibits p63 isoform γ (TAp63γ) transcriptional activity.

9. Molecular characterization and expression of p63 isoforms in human keloids.

10. The high-mobility-group box protein SSRP1/T160 is essential for cell viability in day 3.5 mouse embryos.