Molecular Oncology
Volume 2, Issue 4 , Pages 296-316, December 2008

Aberrations of the MRE11–RAD50–NBS1 DNA damage sensor complex in human breast cancer: MRE11 as a candidate familial cancer-predisposing gene

  • Jirina Bartkova

      Affiliations

    • Institute Cancer Biology and Centre for Genotoxic Stress Research, Danish Cancer Society, Copenhagen, Denmark
    • These authors contributed equally to the work.
    • ,
  • Johanna Tommiska

      Affiliations

    • Department of Obstetrics and Gynecology, Helsinki University Central Hospital (HUCH), FI-00029 Helsinki, Finland
    • These authors contributed equally to the work.
    • ,
  • Lenka Oplustilova

      Affiliations

    • Institute Cancer Biology and Centre for Genotoxic Stress Research, Danish Cancer Society, Copenhagen, Denmark
    • Laboratory of Genome Integrity, Palacky University, Olomouc, Czech Republic;
    • These authors contributed equally to the work.
    • ,
  • Kirsimari Aaltonen

      Affiliations

    • Department of Obstetrics and Gynecology, Helsinki University Central Hospital (HUCH), FI-00029 Helsinki, Finland
    • Department of Oncology, HUCH, Helsinki, Finland
    • ,
  • Anitta Tamminen

      Affiliations

    • Department of Obstetrics and Gynecology, Helsinki University Central Hospital (HUCH), FI-00029 Helsinki, Finland
    • ,
  • Tuomas Heikkinen

      Affiliations

    • Department of Obstetrics and Gynecology, Helsinki University Central Hospital (HUCH), FI-00029 Helsinki, Finland
    • ,
  • Martin Mistrik

      Affiliations

    • Institute Cancer Biology and Centre for Genotoxic Stress Research, Danish Cancer Society, Copenhagen, Denmark
    • Laboratory of Genome Integrity, Palacky University, Olomouc, Czech Republic;
    • ,
  • Kristiina Aittomäki

      Affiliations

    • Department of Clinical Genetics, HUCH, Helsinki, Finland
    • ,
  • Carl Blomqvist

      Affiliations

    • Department of Oncology, HUCH, Helsinki, Finland
    • Department of Oncology, Uppsala University Hospital, Uppsala, Sweden
    • ,
  • Päivi Heikkilä

      Affiliations

    • Department of Pathology, HUCH, Helsinki, Finland
    • ,
  • Jiri Lukas

      Affiliations

    • Institute Cancer Biology and Centre for Genotoxic Stress Research, Danish Cancer Society, Copenhagen, Denmark
    • ,
  • Heli Nevanlinna

      Affiliations

    • Department of Obstetrics and Gynecology, Helsinki University Central Hospital (HUCH), FI-00029 Helsinki, Finland
    • Corresponding Author InformationCorresponding author.
    • ,
  • Jiri Bartek

      Affiliations

    • Institute Cancer Biology and Centre for Genotoxic Stress Research, Danish Cancer Society, Copenhagen, Denmark
    • Laboratory of Genome Integrity, Palacky University, Olomouc, Czech Republic;
    • Corresponding Author InformationCorresponding author. Institute of Cancer Biology and Centre for Genotoxic Stress Research, Danish Cancer Society, Strandboulevarden 49, DK-2100 Copenhagen, Denmark. Tel.: +45 35 25 73 57; fax: +45 35 25 77 21.

Received 17 August 2008; received in revised form 11 September 2008; accepted 14 September 2008. published online 22 October 2008.

Abstract 

The MRE11, RAD50, and NBS1 genes encode proteins of the MRE11–RAD50–NBS1 (MRN) complex critical for proper maintenance of genomic integrity and tumour suppression; however, the extent and impact of their cancer-predisposing defects, and potential clinical value remain to be determined. Here, we report that among a large series of approximately 1000 breast carcinomas, around 3%, 7% and 10% tumours showed aberrantly reduced protein expression for RAD50, MRE11 and NBS1, respectively. Such defects were more frequent among the ER/PR/ERBB2 triple-negative and higher-grade tumours, among familial (especially BRCA1/BRCA2-associated) rather than sporadic cases, and the NBS1 defects correlated with shorter patients’ survival. The BRCA1-associated and ER/PR/ERBB2 triple-negative tumours also showed high incidence of constitutively active DNA damage signalling (γH2AX) and p53 aberrations. Sequencing the RAD50, MRE11 and NBS1 genes of 8 patients from non-BRCA1/2 breast cancer families whose tumours showed concomitant reduction/loss of all three MRN-complex proteins revealed two germline mutations in MRE11: a missense mutation R202G and a truncating mutation R633STOP (R633X). Gene transfer and protein analysis of cell culture models with mutant MRE11 implicated various destabilization patterns among the MRN complex proteins including NBS1, the abundance of which was restored by re-expression of wild-type MRE11. We propose that germline mutations qualify MRE11 as a novel candidate breast cancer susceptibility gene in a subset of non-BRCA1/2 families. Our data have implications for the concept of the DNA damage response as an intrinsic anti-cancer barrier, various components of which become inactivated during cancer progression and also represent the bulk of breast cancer susceptibility genes discovered to date.

Keywords: DNA damage response, MRE11–RAD50–NBS1 complex, Breast cancer, Familial cancer predisposition, Tumour suppressors, BRCA1/BRCA2, p53, ER/PR/ERBB2-triple negative tumours

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PII: S1574-7891(08)00121-X

doi:10.1016/j.molonc.2008.09.007

Molecular Oncology
Volume 2, Issue 4 , Pages 296-316, December 2008

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