Abstract :
Cockayne syndrome (CS) is a rare recessive disorder characterized by a number of developmental abnormalities and premature aging. Two complementation groups (A and B) have been identified so far in CS cases. Defective transcription-coupled nucleotide excision repair is the hallmark of these patients, but in recent years evidence has been presented for a possible defect in the base excision repair pathway that removes oxidized bases. Recent results indicate that both A and B complementation groups are involved but the phenotypical consequences of this flaw remain undetermined.
Keywords :
free radicals , Transcription-coupled repair , Oxidative DNA damage , 8-Oxo-7 , Glycosylase , 8-dihydroguanine , mutation , Cockayne syndrome , aging , Neurological deterioration , DNA base excision repair
