The ERCC1/XPF endonuclease is required for completion of homologous recombination at DNA replication forks stalled by inter-strand cross-links

نویسندگان

  • Ali Z. Al-Minawi
  • Yin-Fai Lee
  • Daniel Håkansson
  • Fredrik Johansson
  • Cecilia Lundin
  • Nasrollah Saleh-Gohari
  • Niklas Schultz
  • Dag Jenssen
  • Helen E. Bryant
  • Mark Meuth
  • John M. Hinz
  • Thomas Helleday
چکیده

Both the ERCC1-XPF complex and the proteins involved in homoIogous recombination (HR) have critical roles in inter-strand cross-link (ICL) repair. Here, we report that mitomycin C-induced lesions inhibit replication fork elongation. Furthermore, mitomycin C-induced DNA double-strand breaks (DSBs) are the result of the collapse of ICL-stalled replication forks. These are not formed through replication run off, as we show that mitomycin C or cisplatin-induced DNA lesions are not incised by global genome nucleotide excision repair (GGR). We also suggest that ICL-lesion repair is initiated either by replication or transcription, as the GGR does not incise ICL-lesions. Furthermore, we report that RAD51 foci are induced by cisplatin or mitomycin C independently of ERCC1, but that mitomycin C-induced HR measured in a reporter construct is impaired in ERCC1-defective cells. These data suggest that ERCC1-XPF plays a role in completion of HR in ICL repair. We also find no additional sensitivity to cisplatin by siRNA co-depletion of XRCC3 and ERCC1, showing that the two proteins act on the same pathway to promote survival.

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عنوان ژورنال:

دوره 37  شماره 

صفحات  -

تاریخ انتشار 2009