DNA lesions resulting from impaired progression of replication forks are implicated in genetic instability and tumorigenesis. Because the cellular response to these lesions poses an important tumorigenesis barrier, the responsible signalling and repair pathways are often mutated or inactive in tumours. Here, we discuss how such deficiencies can in turn be exploited for cancer therapy.

Keywords:
cancer therapy, DNA replication, homologous recombination, poly(ADP-ribose) polymerase (PARP), repair, tumorigenesis
© The Authors Journal compilation © 2007 Biochemical Society
2007
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