<em>ATM</em>, <em>ATR</em> and Mre11 complex genes in hereditary susceptibility to breast cancer

Abstract

<div lang="en" class="abs"><p class="abs_header">Abstract</p><p>Mutations in <em>BRCA1</em> and <em>BRCA2</em> explain only about 20% of familial aggregation of breast cancer, suggesting involvement of additional susceptibility genes. In this study five DNA damage response genes, <em>ATM</em>, <em>ATR</em>, <em>MRE11</em>, <em>NBS1</em> and <em>RAD50</em>, were considered as putative candidates to explain some of the remaining familial breast cancer risk, and were screened for germline mutations in families displaying genetic predisposition. </p><p>Analysis of <em>ATM</em> indicated that clearly pathogenic mutations seem to be restricted to those reported in ataxia-telangiectasia (A-T). However, a cancer risk modifying effect was suggested for a combination of two <em>ATM</em> polymorphisms, 5557G>A and IVS38-8T>C, as this allele seemed to associate with bilateral breast cancer (OR 10.2, 95% CI 3.1–33.8, <em>p</em> = 0.001). </p><p>The relevance of <em>ATM</em> mutations, originally identified in Finnish A-T patients, in breast cancer susceptibility was evaluated by a large case-control study. Two such alleles, 6903insA and 7570G>C, in addition to 8734A>G previously associated with breast cancer susceptibility, were observed. The overall mutation frequency in unselected cases (7/1124) was higher than in controls (1/1107), but a significantly elevated frequency was observed only in familial cases (6/541, <em>p</em> = 0.006, OR 12.4, 95% CI 1.5–103.3). These three mutations showed founder effects in their geographical occurrence, and had different functional consequences at protein level. </p><p>In <em>ATR</em> no disease-related mutations were observed, suggesting that it is not a breast cancer susceptibility gene.</p><p>The mutation screening of the Mre11 complex genes, <em>MRE11</em>, <em>NBS1</em> and <em>RAD50</em>, revealed two novel potentially breast cancer associated alleles: <em>NBS1</em> Leu150Phe and <em>RAD50</em> 687delT were observed in 2.0% (3/151) of the studied families. The subsequent study of newly diagnosed, unselected breast cancer cases indicated that <em>RAD50</em> 687delT is a relatively common low-penetrance susceptibility allele in Northern Finland (cases 8/317 vs. controls 6/1000, OR 4.3, 95% CI 1.5–12.5, <em>p</em> = 0.008). <em>NBS1</em> Leu150Phe (2/317) together with a novel <em>RAD50</em> IVS3-1G>A mutation (1/317) was also observed, both being absent from controls. Loss of the wild-type allele was not observed in the tumors of the studied mutation carriers, but they all showed an increase in chromosomal instability of peripheral T-lymphocytes. This suggests an effect for <em>RAD50</em> and <em>NBS1</em> haploinsufficiency on genomic integrity and susceptibility to cancer. </p></div>