Gene panel testing of 5589 <i><scp>BRCA</scp>1/2</i>‐negative index patients with breast cancer in a routine diagnostic setting: results of the German Consortium for Hereditary Breast and Ovarian Cancer

Jan Hauke; Judit Horváth; Eva Groß; Andrea Gehrig; Ellen Honisch; Karl Hackmann; Gunnar Schmidt; Norbert Arnold; Ulrike Faust; Christian Sutter; Julia Hentschel; Shan Wang‐Gohrke; Mateja Smogavec; Bernhard H. F. Weber; Nana Weber‐Lassalle; Konstantin Weber‐Lassalle; Julika Borde; Corinna Ernst; Janine Altmüller; Alexander E. Volk; Hölger Thiele; Verena Hübbel; Peter Nürnberg; Katharina Keupp; Beatrix Versmold; Esther Pohl; Christian Kubisch; Sabine Grill; Victoria Paul; N Herold; Nadine Lichey; Kerstin Rhiem; Nina Ditsch; Christian Rückert; Barbara Wappenschmidt; Bernd Auber; Andreas Rump; Dieter Niederacher; Thomas Haaf; Juliane Ramser; Bernd Dworniczak; Christoph Engel; Alfons Meindl; Rita K. Schmutzler; Eric Hahnen

doi:10.1002/cam4.1376

Gene panel testing of 5589 <i><scp>BRCA</scp>1/2</i>‐negative index patients with breast cancer in a routine diagnostic setting: results of the German Consortium for Hereditary Breast and Ovarian Cancer

Jan Hauke(University Hospital Cologne), Judit Horváth(University Hospital Münster), Eva Groß(TUM Klinikum), Andrea Gehrig(University of Würzburg), Ellen Honisch(Düsseldorf University Hospital), Karl Hackmann(Technische Universität Dresden), Gunnar Schmidt(Medizinische Hochschule Hannover), Norbert Arnold(Christian-Albrechts-Universität zu Kiel), Ulrike Faust(University of Tübingen), Christian Sutter(Heidelberg University), Julia Hentschel(University Hospital Leipzig), Shan Wang‐Gohrke(University Hospital Ulm), Mateja Smogavec(University of Göttingen), Bernhard H. F. Weber(University of Regensburg), Nana Weber‐Lassalle(University Hospital Cologne), Konstantin Weber‐Lassalle(University Hospital Cologne), Julika Borde(University Hospital Cologne), Corinna Ernst(University Hospital Cologne), Janine Altmüller(University of Cologne), Alexander E. Volk(Universität Hamburg), Hölger Thiele(University of Cologne), Verena Hübbel(University Hospital Cologne), Peter Nürnberg(University of Cologne), Katharina Keupp(University Hospital Cologne), Beatrix Versmold(University Hospital Cologne), Esther Pohl(University Hospital Cologne), Christian Kubisch(Universität Hamburg), Sabine Grill(TUM Klinikum), Victoria Paul(University Hospital Münster), N Herold(University Hospital Cologne), Nadine Lichey(University Hospital Münster), Kerstin Rhiem(University Hospital Cologne), Nina Ditsch(Ludwig-Maximilians-Universität München), Christian Rückert(University Hospital Münster), Barbara Wappenschmidt(University Hospital Cologne), Bernd Auber(Medizinische Hochschule Hannover), Andreas Rump(Technische Universität Dresden), Dieter Niederacher(Düsseldorf University Hospital), Thomas Haaf(University of Würzburg), Juliane Ramser(TUM Klinikum), Bernd Dworniczak(University Hospital Münster), Christoph Engel(Leipzig University of Applied Sciences), Alfons Meindl(TUM Klinikum), Rita K. Schmutzler(University Hospital Cologne), Eric Hahnen(University Hospital Cologne)

Cancer Medicine

March 9, 2018

10.1002/cam4.1376

Cited by 165Open Access

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Abstract

The prevalence of germ line mutations in non-BRCA1/2 genes associated with hereditary breast cancer (BC) is low, and the role of some of these genes in BC predisposition and pathogenesis is conflicting. In this study, 5589 consecutive BC index patients negative for pathogenic BRCA1/2 mutations and 2189 female controls were screened for germ line mutations in eight cancer predisposition genes (ATM, CDH1, CHEK2, NBN, PALB2, RAD51C, RAD51D, and TP53). All patients met the inclusion criteria of the German Consortium for Hereditary Breast and Ovarian Cancer for germ line testing. The highest mutation prevalence was observed in the CHEK2 gene (2.5%), followed by ATM (1.5%) and PALB2 (1.2%). The mutation prevalence in each of the remaining genes was 0.3% or lower. Using Exome Aggregation Consortium control data, we confirm significant associations of heterozygous germ line mutations with BC for ATM (OR: 3.63, 95%CI: 2.67-4.94), CDH1 (OR: 17.04, 95%CI: 3.54-82), CHEK2 (OR: 2.93, 95%CI: 2.29-3.75), PALB2 (OR: 9.53, 95%CI: 6.25-14.51), and TP53 (OR: 7.30, 95%CI: 1.22-43.68). NBN germ line mutations were not significantly associated with BC risk (OR:1.39, 95%CI: 0.73-2.64). Due to their low mutation prevalence, the RAD51C and RAD51D genes require further investigation. Compared with control datasets, predicted damaging rare missense variants were significantly more prevalent in CHEK2 and TP53 in BC index patients. Compared with the overall sample, only TP53 mutation carriers show a significantly younger age at first BC diagnosis. We demonstrate a significant association of deleterious variants in the CHEK2, PALB2, and TP53 genes with bilateral BC. Both, ATM and CHEK2, were negatively associated with triple-negative breast cancer (TNBC) and estrogen receptor (ER)-negative tumor phenotypes. A particularly high CHEK2 mutation prevalence (5.2%) was observed in patients with human epidermal growth factor receptor 2 (HER2)-positive tumors.

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