Affiliations of authors: K. Syrjäkoski, K. Kivinummi, Laboratory of Cancer Genetics, Institute of Medical Technology, Tampere University and Tampere University Hospital, Finland; P. Vahteristo, A. Tamminen, L. Sarantaus, H. Nevanlinna, Department of Obstetrics and Gynecology, Helsinki University Central Hospital, Finland; H. Eerola, Departments of Obstetrics and Gynecology and Oncology, Helsinki University Central Hospital; K. Holli, Department of Oncology, Tampere University Hospital; C. Blomqvist, Department of Oncology, Helsinki University Central Hospital, and Department of Oncology, Uppsala University Hospital, Sweden; O.-P. Kallioniemi, T. Kainu, Laboratory of Cancer Genetics, Institute of Medical Technology, Tampere University and Tampere University Hospital, and Cancer Genetics Branch, National Human Genome Research Institute, Bethesda, MD.
Correspondence to: Heli Nevanlinna, Ph.D., Department of Obsterics and Gynecology, P.O. Box 140, Haartmaninkatu 2, FIN-00029, Helsinki University Central Hospital, Helsinki, Finland (e-mail: Heli.Nevanlinna{at}hus.fi).
Two highly penetrant genes involved in hereditary breast and/or ovarian cancer syndromes, BRCA1 and BRCA2, have been identified (1,2). Mutations in these genes occur throughout their coding sequences, making large-scale testing for mutations challenging. It is, therefore, not surprising that only a few studies have reported estimates of the mutation frequencies among unselected breast cancer patients. Usually, only a few hundred patients have been analyzed in each study, with mutation frequencies ranging from 3.3% to 5.7% for BRCA1 (35). The largest studies of BRCA1 and BRCA2 mutations have been carried out in isolated populations, such as the Icelanders or Ashkenazi Jews (6), where individual, highly recurrent founder mutations account for the majority of all mutations (7,8). Results derived from such populations may, however, be biased by the specific nature of these mutations.
In whole-gene mutation screening performed by two independent groups (911) on 188 breast and breastovarian cancer families in Finland, 11 mutations accounted for the vast majority (84%) of all detected BRCA1 and BRCA2 mutations. Besides these recurrent BRCA1 and BRCA2 founder mutations, eight other mutations have been identified only once in the Finnish population [(912); Vahteristo P, Eerola H, Tamminen A, Blomqvist C, Nevanlinna H: unpublished observations]. The 11 known mutations provide a unique, rapid way to analyze the impact of BRCA1 and BRCA2 mutations at the population level, without a bias toward any individual founder mutation.
We collected blood samples from 1035 consecutive, newly diagnosed breast cancer patients treated at the Departments of Oncology at the Helsinki University Central Hospital, Finland (n = 627) from April 1997 through March 1998, and at the Tampere University Hospital, Finland (n = 408), from January 1997 through May 1999. These cohorts cover 82% (87% in Helsinki and 75% in Tampere) of all breast cancer patients who visited the clinics during the study period. The two university hospitals accrue patients from a large, geographically defined region covering a large part of southern Finland and account for about 30% of all breast cancer patients diagnosed in Finland. Because of the recent migration patterns within Finland, the patients diagnosed in Tampere and, particularly, those diagnosed in Helsinki have their ancestral origins throughout Finland. Written, informed consent was obtained from the patients. The patients were asked to fill out a questionnaire on breast, ovarian, and other cancers in their family. Only patients reporting breast and/or ovarian cancers in first- or second-degree relatives were considered to have a family history of the disease. The study did not alter treatment protocols or patient management, and those patients with a strong family history of breast or ovarian cancer were referred to genetic counseling and possible BRCA1 and BRCA2 mutation screening, regardless of the results of this study. The mean age at diagnosis was 56.2 years in Helsinki and 58.9 years in Tampere, which is comparable to the average age of diagnosis of breast cancer in Finland (13). The study has been approved by the Ethical Committees of the Departments of Oncology and Obstetrics and Gynecology, Helsinki University Central Hospital and Tampere University Hospital, and appropriate permissions were obtained from the Ministry of Social Affairs and Health in Finland.
All 11 BRCA1 and eight BRCA2 mutations found previously in the Finnish population were screened in the 1035 patient samples. Detection of the mutations was performed by use of allele-specific oligonucleotide hybridization or by restriction fragment length polymorphism analysis. The results were confirmed by direct sequencing by use of an ABI PRISM 310 Genetic Analyzer (The Perkin-Elmer Corp., Foster City, CA).
Statistical analyses of differences in dichotomous variables were done by Fisher's exact test (Statistical Package for Social Sciences, Chicago, IL; version 8.0 for Windows). All P values are two-sided. Confidence intervals (CIs) for proportions are based on exact CIs based on the binomial distribution.
The frequency of the BRCA1 and BRCA2 mutations in unselected Finnish breast cancer patients was 1.8% (Table 1), which is much lower than the reported prevalence of BRCA1 and BRCA2 founder mutations in unselected Icelandic (7.7%10.4%) (1416) and Ashkenazi (11.7%) (17) breast cancer patients. In contrast, a recent, large retrospective study of early-onset breast cancer case subjects (<36 years) in England by Peto et al. (18) estimated a similar frequency for both BRCA1 and BRCA2 mutations (2.8%) as obtained in this study. This figure was based on correction for assuming a 63% mutation detection sensitivity, as well as extrapolation of findings from early-onset breast cancer to the total breast cancer population assuming high penetrance for the mutations. The frequency of 1.8% reported in this study obviously also represents an underestimate, since only the 19 mutations identified previously in the Finnish population were studied. However, we believe that the result is well representative of the BRCA1 and BRCA2 mutation burden because the 11 founder mutations account for a major fraction of all mutations in these genes in Finnish breast cancer famillies (911). Nine of the 11 founder mutations were detected in this independent population-based study and accounted for 17 of the 19 mutations. In addition, one mutation seen previously only once was found here in two patients.
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Collectively, these three criteria (ovarian cancer family history, early age at diagnosis of breast cancer, and family history of two or more breast cancers) would have distinguished 15 mutation carriers in a subset of 181 patients (8.3%). This number should be compared with the presence of 19 mutations in the entire series of 1035 patients (1.8% mutation carriers). Furthermore, the prevalence of BRCA1 or BRCA2 mutations was very low (four [0.5%] of 854) in breast cancer patients who do not belong to the above-mentioned subgroup. The results illustrate that BRCA1 and BRCA2 mutation screening is not warranted in the general breast cancer population and substantiate the suggested strict criteria for BRCA1 testing in breast cancer (4,21,22).
NOTES
K. Syrjäkoski and P. Vahteristo as well as T. Kainu and H. Nevanlinna contributed equally to this work.
Supported by the Academy of Finland, The Sigrid Juselius Foundation, The Nordic Cancer Union, The Finnish Cancer Society, The Clinical Research Fund of Helsinki University Central Hospital, The Research Fund of Tampere University Hospital, and The Pirkanmaa Cancer Society.
We thank Minna Merikivi, Päivi Virtanen, and Kristiina Selkee for their help in patient contacts and sample collection and Kati Rouhento for her technical assistance. We also acknowledge the patients participating in this study.
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Manuscript received January 5, 2000; revised June 23, 2000; accepted July 11, 2000.
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