Cockayne syndrome group B protein (CSB) plays a general role in chromatin maintenance and remodeling

Newman, John C.; Bailey, Arnold D.; Weiner, Alan M.

doi:10.1073/pnas.0510909103

Cited by 137 publications

(140 citation statements)

References 58 publications

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“…The similar impairment of 8-OH-Gua repair reported in the absence of CSB (reviewed by Licht et al, 2003) or CSA (this study) suggests that these proteins act in the same pathway. We favor the hypothesis that the acceleration of repair at early repair times mediated by CSB (Osterod et al, 2002) or CSA (this study) reflects the role of CS proteins in the regulation of chromatin structure (for instance by ubiquitination and/or acetylation of histones) (Citterio et al, 2000;Groisman et al, 2003;Newman et al, 2006). CS-mediated chromatin remodeling activity might increase the accessibility of DNA damage to the repair machinery.…”

Section: Discussionmentioning

confidence: 60%

The role of CSA in the response to oxidative DNA damage in human cells

et al. 2007

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Cockayne syndrome (CS) is a rare genetic disease characterized by severe growth, mental retardation and pronounced cachexia. CS is most frequently due to mutations in either of two genes, CSB and CSA. Evidence for a role of CSB protein in the repair of oxidative DNA damage has been provided recently. Here, we show that CSA is also involved in the response to oxidative stress. CS-A human primary fibroblasts and keratinocytes showed hypersensitivity to potassium bromate, a specific inducer of oxidative damage. This was associated with inefficient repair of oxidatively induced DNA lesions, namely 8-hydroxyguanine (8-OH-Gua) and (5 0 S)-8,5 0 -cyclo 2 0 -deoxyadenosine. Expression of the wild-type CSA in the CS-A cell line CS3BE significantly decreased the steady-state level of 8-OH-Gua and increased its repair rate following oxidant treatment. CS-A cell extracts showed normal 8-OH-Gua cleavage activity in an in vitro assay, whereas CS-B cell extracts were confirmed to be defective. Our data provide the first in vivo evidence that CSA protein contributes to prevent accumulation of various oxidized DNA bases and underline specific functions of CSB not shared with CSA. These findings support the hypothesis that defective repair of oxidative DNA damage is involved in the clinical features of CS patients.

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Section: Discussionmentioning

confidence: 60%

The role of CSA in the response to oxidative DNA damage in human cells

et al. 2007

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“…Different approaches provide evidence that CSB might have an impact on transcription itself. Transcriptome analysis of CS-B cells revealed deregulation of gene expression similar to that caused by agents that disrupt chromatin structure [35]. When added to a stalled RNAPIIo (at a CPD photolesion) CSB can stimulate transcription elongation by addition of one nucleotide to the nascent transcript, but not bypass of the lesion [36].…”

Section: Transcription-coupled Nucleotide Excision Repair Requires Spmentioning

confidence: 99%

Transcription-coupled nucleotide excision repair in mammalian cells: molecular mechanisms and biological effects

2008

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The encounter of elongating RNA polymerase II (RNAPIIo) with DNA lesions has severe consequences for the cell as this event provides a strong signal for P53-dependent apoptosis and cell cycle arrest. To counteract prolonged blockage of transcription, the cell removes the RNAPIIo-blocking DNA lesions by transcription-coupled repair (TC-NER), a specialized subpathway of nucleotide excision repair (NER). Exposure of mice to UVB light or chemicals has elucidated that TC-NER is a critical survival pathway protecting against acute toxic and long-term effects (cancer) of genotoxic exposure. Deficiency in TC-NER is associated with mutations in the CSA and CSB genes giving rise to the rare human disorder Cockayne syndrome (CS). Recent data suggest that CSA and CSB play differential roles in mammalian TC-NER: CSB as a repair coupling factor to attract NER proteins, chromatin remodellers and the CSA-E3-ubiquitin ligase complex to the stalled RNAPIIo. CSA is dispensable for attraction of NER proteins, yet in cooperation with CSB is required to recruit XAB2, the nucleosomal binding protein HMGN1 and TFIIS. The emerging picture of TC-NER is complex: repair of transcription-blocking lesions occurs without displacement of the DNA damage-stalled RNAPIIo, and requires at least two essential assembly factors (CSA and CSB), the core NER factors (except for XPC-RAD23B), and TC-NER specific factors. These and yet unidentified proteins will accomplish not only efficient repair of transcription-blocking lesions, but are also likely to contribute to DNA damage signalling events.

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“…A study by Egly and co-workers (Proietti-De-Santis et al, 2006) supports a role for CSB in regulating the transcription pattern after UV damage as they found a function for CSB in transcription from some but not other promoters. Another comparative gene expression study established that CSB is involved in transcription of genes involved in chromatin maintenance and remodeling (Newman et al, 2006). CS cells display a stronger apoptotic response to DNA damaging agents than normal cells Laposa et al, 2007;Liu et al, 2006), which in part could explain why no cancer is seen in the patients.…”

Section: The Role Of Csb In Various Cellular Processesmentioning

confidence: 99%

“…When compared to CSB deficient cells, the transcription from chromatin in wild type cells was more resistant to the detergent Triton X-100, indicating that the transcription machinery is less tightly associated with chromatin in CSB deficient cells compared to wild type cells (Balajee et al, 1997). A study by Weiner and coworkers found that the transcription pattern of CSB deficient cells had a significant overlap with the transcription pattern of cells treated with the histone deacetylase (HDAC) inhibitor trichostatin A (TSA), indicating that CSB could play a role in chromatin maintenance (Newman et al, 2006). The similarity of HDAC inhibited cells to CSB deficient cells indicates that a role of CSB is to decrease the amount of histone acetylation.…”

Section: Csb and Chromatin Structurementioning

confidence: 99%

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

Stevnsner

Müftüoğlu

Aamann

et al. 2008

Mechanisms of Ageing and Development

124

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Cockayne Syndrome (CS) is a rare human genetic disorder characterized by progressive multisystem degeneration and segmental premature aging. The CS complementation group B (CSB) protein is engaged in transcription coupled and global nucleotide excision repair, base excision repair and general transcription. However, the precise molecular function of the CSB protein is still unclear. In the current review we discuss the involvement of CSB in some of these processes, with focus on the role of CSB in repair of oxidative damage, as deficiencies in the repair of these lesions may be an important aspect of the premature aging phenotype of CS.

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Cockayne syndrome group B protein (CSB) plays a general role in chromatin maintenance and remodeling

Cited by 137 publications

References 58 publications

The role of CSA in the response to oxidative DNA damage in human cells

The role of CSA in the response to oxidative DNA damage in human cells

Transcription-coupled nucleotide excision repair in mammalian cells: molecular mechanisms and biological effects

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

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