| Literature DB >> 12483520 |
Tinna Stevnsner1, Simon Nyaga, Nadja C de Souza-Pinto, Gijsbertus T J van der Horst, Theo G M F Gorgels, Barbara A Hogue, Tina Thorslund, Vilhelm A Bohr.
Abstract
Reactive oxygen species, which are prevalent in mitochondria, cause oxidative DNA damage including the mutagenic DNA lesion 7,8-dihydroxyguanine (8-oxoG). Oxidative damage to mitochondrial DNA has been implicated as a causative factor in a wide variety of degenerative diseases, and in cancer and aging. 8-oxoG is repaired efficiently in mammalian mitochondrial DNA by enzymes in the base excision repair pathway, including the 8-oxoguanine glycosylase (OGG1), which incizes the lesion in the first step of repair. Cockayne syndrome (CS) is a segmental premature aging syndrome in humans that has two complementation groups, CSA and CSB. Previous studies showed that CSB-deficient cells have reduced capacity to repair 8-oxoG. This study examines the role of the CSB gene in regulating repair of 8-oxoG in mitochondrial DNA in human and mouse cells. 8-oxoG repair was measured in liver cells from CSB deficient mice and in human CS-B cells carrying expression vectors for wild type or mutant forms of the human CSB gene. For the first time we report that CSB stimulates repair of 8-oxoG in mammalian mitochondrial DNA. Furthermore, evidence is presented to support the hypothesis that wild type CSB regulates expression of OGG1.Entities:
Mesh:
Substances:
Year: 2002 PMID: 12483520 DOI: 10.1038/sj.onc.1205994
Source DB: PubMed Journal: Oncogene ISSN: 0950-9232 Impact factor: 9.867