Literature DB >> 26616585

Elements That Regulate the DNA Damage Response of Proteins Defective in Cockayne Syndrome.

Teruaki Iyama1, David M Wilson2.   

Abstract

Cockayne syndrome (CS) is a premature aging disorder characterized by developmental defects, multisystem progressive degeneration and sensitivity to ultraviolet light. CS is divided into two primary complementation groups, A and B, with the CSA and CSB proteins presumably functioning in DNA repair and transcription. Using laser microirradiation and confocal microscopy, we characterized the nature and regulation of the CS protein response to oxidative DNA damage, double-strand breaks (DSBs), angelicin monoadducts and trioxsalen interstrand crosslinks (ICLs). Our data indicate that CSB recruitment is influenced by the type of DNA damage and is most rapid and robust as follows: ICLs>DSBs>monoadducts>oxidative lesions. Transcription inhibition reduced accumulation of CSB at sites of monoadducts and ICLs, but it did not affect recruitment to (although slightly affected retention at) oxidative damage. Inhibition of histone deacetylation altered the dynamics of CSB assembly, suggesting a role for chromatin status in the response to DNA damage, whereas the proteasome inhibitor MG132 had no effect. The C-terminus of CSB and, in particular, its ubiquitin-binding domain were critical to recruitment, while the N-terminus and a functional ATPase domain played a minor role at best in facilitating protein accumulation. Although the absence of CSA had no effect on CSB recruitment, CSA itself localized at sites of ICLs, DSBs and monoadducts but not at oxidative lesions. Our results reveal molecular components of the CS protein response and point to a major involvement of complex lesions in the pathology of CS. Published by Elsevier Ltd.

Entities:  

Keywords:  CSA/ERCC8; CSB/ERCC6; Cockayne syndrome; DNA damage response; DNA repair

Mesh:

Substances:

Year:  2015        PMID: 26616585      PMCID: PMC4738086          DOI: 10.1016/j.jmb.2015.11.020

Source DB:  PubMed          Journal:  J Mol Biol        ISSN: 0022-2836            Impact factor:   5.469


  67 in total

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6.  Meta-analysis of DNA double-strand break response kinetics.

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7.  ATM and CDK2 control chromatin remodeler CSB to inhibit RIF1 in DSB repair pathway choice.

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8.  Cockayne syndrome B protein regulates recruitment of the Elongin A ubiquitin ligase to sites of DNA damage.

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9.  Differential RPA-1 and RAD-51 recruitment in vivo throughout the C. elegans germline, as revealed by laser microirradiation.

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10.  Are parents of children with Cockayne syndrome manifesting features of the disorder?: Case reports.

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