Literature DB >> 10698517

Role of the ATPase domain of the Cockayne syndrome group B protein in UV induced apoptosis.

A S Balajee1, L Proietti De Santis, R M Brosh, R Selzer, V A Bohr.   

Abstract

Cockayne syndrome (CS) is a human autosomal recessive disorder characterized by many neurological and developmental abnormalities. CS cells are defective in the transcription coupled repair (TCR) pathway that removes DNA damage from the transcribed strand of active genes. The individuals suffering from CS do not generally develop cancer but show increased neurodegeneration. Two genetic complementation groups (CS-A and CS-B) have been identified. The lack of cancer formation in CS may be due to selective elimination of cells containing DNA damage by a suicidal pathway. In this study, we have evaluated the role of the CSB gene in UV induced apoptosis in human and hamster cells. The hamster cell line UV61 carries a mutation in the homolog of the human CSB gene. We show that both human CS-B and hamster UV61 cells display increased apoptotic response following UV exposure compared with normal cells. The increased sensitivity of UV61 cells to apoptosis is complemented by the transfection of the wild type human CSB gene. In order to determine which functional domain of the CSB gene participates in the apoptotic pathway, we constructed stable cell lines with different CSB domain disruptions. UV61 cells were stably transfected with the human CSB cDNA containing a point mutation in the highly conserved glutamic acid residue in ATPase motif II. This cell line (UV61/ pc3.1-CSBE646Q) showed the same increased apoptosis as the UV61 cells. In contrast, cells containing a deletion in the acidic domain at the N-terminal end of the CSB protein had no effect on apoptosis. This indicates that the integrity of the ATPase domain of CSB protein is critical for preventing the UV induced apoptotic pathway. In primary human CS-B cells, the induction and stabilization of the p53 protein seems to correlate with their increased apoptotic potential. In contrast, no change in the level of either p53 or activation of mdm2 protein by p53 was observed in hamster UV61 cells after UV exposure. This suggests that the CSB dependent apoptotic pathway can occur independently of the transactivation potential of p53 in hamster cells.

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Year:  2000        PMID: 10698517     DOI: 10.1038/sj.onc.1203372

Source DB:  PubMed          Journal:  Oncogene        ISSN: 0950-9232            Impact factor:   9.867


  16 in total

1.  Molecular characterization of an acidic region deletion mutant of Cockayne syndrome group B protein.

Authors:  M Sunesen; R R Selzer; R M Brosh; A S Balajee; T Stevnsner; V A Bohr
Journal:  Nucleic Acids Res       Date:  2000-08-15       Impact factor: 16.971

Review 2.  Cockayne syndrome group B cellular and biochemical functions.

Authors:  Cecilie Löe Licht; Tinna Stevnsner; Vilhelm A Bohr
Journal:  Am J Hum Genet       Date:  2003-11-24       Impact factor: 11.025

3.  Cockayne syndrome, underlying molecular defects and p53.

Authors:  Brian R Berquist; Vilhelm A Bohr
Journal:  Cell Cycle       Date:  2011-12-01       Impact factor: 4.534

4.  Differential requirement for the ATPase domain of the Cockayne syndrome group B gene in the processing of UV-induced DNA damage and 8-oxoguanine lesions in human cells.

Authors:  Rebecca R Selzer; Simon Nyaga; Jingsheng Tuo; Alfred May; Meltem Muftuoglu; Mette Christiansen; Elisabetta Citterio; Robert M Brosh; Vilhelm A Bohr
Journal:  Nucleic Acids Res       Date:  2002-02-01       Impact factor: 16.971

5.  Testicular nuclear receptor 4 (TR4) regulates UV light-induced responses via Cockayne syndrome B protein-mediated transcription-coupled DNA repair.

Authors:  Su Liu; Shian-Jang Yan; Yi-Fen Lee; Ning-Chun Liu; Huei-Ju Ting; Gonghui Li; Qiao Wu; Lu-Min Chen; Chawnshang Chang
Journal:  J Biol Chem       Date:  2011-09-14       Impact factor: 5.157

6.  Cockayne syndrome group B protein promotes mitochondrial DNA stability by supporting the DNA repair association with the mitochondrial membrane.

Authors:  Maria D Aamann; Martin M Sorensen; Christina Hvitby; Brian R Berquist; Meltem Muftuoglu; Jingyan Tian; Nadja C de Souza-Pinto; Morten Scheibye-Knudsen; David M Wilson; Tinna Stevnsner; Vilhelm A Bohr
Journal:  FASEB J       Date:  2010-02-24       Impact factor: 5.191

7.  Restoration of nucleotide excision repair in a helicase-deficient XPD mutant from intragenic suppression by a trichothiodystrophy mutation.

Authors:  J W George; E P Salazar; M P Vreeswijk; J E Lamerdin; J T Reardon; M Z Zdzienicka; A Sancar; S Kadkhodayan; R S Tebbs; L H Mullenders; L H Thompson
Journal:  Mol Cell Biol       Date:  2001-11       Impact factor: 4.272

8.  Genomic DNA of Nostoc commune (Cyanobacteria) becomes covalently modified during long-term (decades) desiccation but is protected from oxidative damage and degradation.

Authors:  Breanne Shirkey; Nicole J McMaster; Sue C Smith; Deborah J Wright; Henry Rodriguez; Pawel Jaruga; Mustafa Birincioglu; Richard F Helm; Malcolm Potts
Journal:  Nucleic Acids Res       Date:  2003-06-15       Impact factor: 16.971

Review 9.  The role of Cockayne Syndrome group B (CSB) protein in base excision repair and aging.

Authors:  Tinna Stevnsner; Meltem Muftuoglu; Maria Diget Aamann; Vilhelm A Bohr
Journal:  Mech Ageing Dev       Date:  2008-04-30       Impact factor: 5.432

10.  Complete release of (5'S)-8,5'-cyclo-2'-deoxyadenosine from dinucleotides, oligodeoxynucleotides and DNA, and direct comparison of its levels in cellular DNA with other oxidatively induced DNA lesions.

Authors:  Pawel Jaruga; Jacob Theruvathu; Miral Dizdaroglu; Philip J Brooks
Journal:  Nucleic Acids Res       Date:  2004-06-23       Impact factor: 16.971
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