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A high proportion of founder BRCA1 mutations in Polish breast cancer families
Authors:Górski Bohdan  Jakubowska Anna  Huzarski Tomasz  Byrski Tomasz  Gronwald Jacek  Grzybowska Ewa  Mackiewicz Andrzej  Stawicka Malgorzata  Bebenek Marek  Sorokin Dagmara  Fiszer-Maliszewska Łucja  Haus Olga  Janiszewska Hanna  Niepsuj Stanisław  Góźdź Stanisław  Zaremba Lech  Posmyk Michał  Płuzańska Maria  Kilar Ewa  Czudowska Dorota  Waśko Bernard  Miturski Roman  Kowalczyk Jerzy R  Urbański Krzysztof  Szwiec Marek  Koc Jan  Debniak Bogusław  Rozmiarek Andrzej  Debniak Tadeusz  Cybulski Cezary  Kowalska Elzbieta  Tołoczko-Grabarek Aleksandra  Zajaczek Stanisław  Menkiszak Janusz  Medrek Krzysztof  Masojć Bartłomiej
Affiliation:Department of Genetics and Pathology, International Hereditary Cancer Center, Pomeranian Medical University, Szczecin, Poland. gorskib@sci.pam.szczecin.pl
Abstract:Three mutations in BRCA1 (5382insC, C61G and 4153delA) are common in Poland and account for the majority of mutations identified to date in Polish breast and breast-ovarian cancer families. It is not known, however, to what extent these 3 founder mutations account for all of the BRCA mutations distributed throughout the country. This question has important implications for health policy and the design of epidemiologic studies. To establish the relative contributions of founder and nonfounder BRCA mutations, we established the entire spectrum of BRCA1 and BRCA2 mutations in a large set of breast-ovarian cancer families with origins in all regions of Poland. We sequenced the entire coding regions of the BRCA1 and BRCA2 genes in 100 Polish families with 3 or more cases of breast cancer and in 100 families with cases of both breast and ovarian cancer. A mutation in BRCA1 or BRCA2 was detected in 66% of breast cancer families and in 63% of breast-ovarian cancer families. Of 129 mutations, 122 (94.6%) were in BRCA1 and 7 (5.4%) were in BRCA2. Of the 122 families with BRCA1 mutations, 119 (97.5%) had a recurrent mutation (i.e., one that was seen in at least 2 families). In particular, 111 families (91.0%) carried one of the 3 common founder mutations. The mutation spectrum was not different between families with and without ovarian cancer. These findings suggest that a rapid and inexpensive assay directed at identifying the 3 common founder mutations will have a sensitivity of 86% compared to a much more costly and labor-intensive full-sequence analysis of both genes. This rapid test will facilitate large-scale national epidemiologic and clinical studies of hereditary breast cancer, potentially including studies of chemoprevention.
Keywords:breast cancer  ovarian cancer  inherited predisposition  BRCA1  BRCA2
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