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Transcription-coupled nucleotide excision repair is coordinated by ubiquitin and SUMO in response to ultraviolet irradiation
TRiC controls transcription resumption after UV damage by regulating Cockayne syndrome protein A
The core spliceosome as target and effector of non-canonical ATM signalling
Human ISWI complexes are targeted by SMARCA5 ATPase and SLIDE domains to help resolve lesion-stalled transcription
Differential binding kinetics of replication protein A during replication and the pre- and post-incision steps of nucleotide
Poly(ADP-ribosyl)ation links the chromatin remodeler SMARCA5/SNF2H to RNF168-dependent DNA damage signaling
PARP1 promotes nucleotide excision repair through DDB2 stabilization and recruitment of ALC1
Experiences of environmental professionals in practice
Replication Factor C Recruits DNA Polymerase delta to Sites of Nucleotide Excision Repair but Is Not Required for PCNA Recruitment
A Ubiquitin-Binding Domain in Cockayne Syndrome B Required for Transcription-Coupled Nucleotide Excision Repair