[PDF][PDF] BRCA1 is required for postreplication repair after UV-induced DNA damage
Molecular cell, 2011•cell.com
BRCA1 contributes to the response to UV irradiation. Utilizing its BRCT motifs, it is recruited
during S/G2 to UV-damaged sites in a DNA replication-dependent but nucleotide excision
repair (NER)-independent manner. More specifically, at UV-stalled replication forks, it
promotes photoproduct excision, suppression of translesion synthesis, and the localization
and activation of replication factor C complex (RFC) subunits. The last function, in turn,
triggers post-UV checkpoint activation and postreplicative repair. These BRCA1 functions …
during S/G2 to UV-damaged sites in a DNA replication-dependent but nucleotide excision
repair (NER)-independent manner. More specifically, at UV-stalled replication forks, it
promotes photoproduct excision, suppression of translesion synthesis, and the localization
and activation of replication factor C complex (RFC) subunits. The last function, in turn,
triggers post-UV checkpoint activation and postreplicative repair. These BRCA1 functions …
Summary
BRCA1 contributes to the response to UV irradiation. Utilizing its BRCT motifs, it is recruited during S/G2 to UV-damaged sites in a DNA replication-dependent but nucleotide excision repair (NER)-independent manner. More specifically, at UV-stalled replication forks, it promotes photoproduct excision, suppression of translesion synthesis, and the localization and activation of replication factor C complex (RFC) subunits. The last function, in turn, triggers post-UV checkpoint activation and postreplicative repair. These BRCA1 functions differ from those required for DSBR.
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