Modifications of DNA clamps and their role in DNA damage management

Modifications of DNA clamps and their role in DNA damage management

Authors	N. Wit
Supervisors	J.G. Borst
Cosupervisors	H. Jacobs
Award date	01-07-2013
ISBN	9789461822680
Number of pages	130
Organisations	Faculty of Science (FNWI) - Swammerdam Institute for Life Sciences (SILS)
Abstract	We show that proliferating cell nuclear antigen (PCNA) modification plays an important role in the efficient regulation of mammalian translesion DNA synthesis (TLS), but, as opposed to lower eukaryotes such as yeast, TLS polymerases can also be activated without ubiquitinated PCNA (PCNA-Ub). Future experiments should investigate the molecular nature of PCNA-Ub-independent TLS activation. Furthermore, DNA damage tolerance (DDT) by TLS is clinically relevant, as shown by deregulation in certain cancers and a suspected role in chemoresistance. Moreover, inhibition of DDT provides an attractive therapeutic drug target for chemosensitization.
Document type	PhD thesis
Note	Research conducted at: Universiteit van Amsterdam
Language	English
Downloads	Thesis Cover Title pages Contents Chapter 1: General introduction Chapter 2: PCNA ubiquitination-independent activation of polymerase eta during somatic hypermutation and DNA damage tolerance Chapter 3: Mammalian DNA polymerase kappa can be activated in the presence or absence of proliferating cell nuclear antigen (PCNA) ubiquitination Chapter 4: HLTF and SHPRH are not essential for PCNA polyubiquitination, survival and somatic hypermutation: Existence of an alternative E3 ligase Chapter 5: Lysine residue 185 of RAD1 is a topological but not a functional counterpart of lysine residue 164 of PCNA Chapter 6: Summarizing discussion Nederlandse samenvatting voor niet-ingewijden Curriculum vitae Publications Dankwoord
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Modifications of DNA clamps and their role in DNA damage management