We selected from the database of our genetic clinic all BRCA1 or BRCA2 mutation carriers and patients with family history but non-carriers who were treated and followed-up for breast cancer in our institution (19692004). We reviewed the prospectively registered case notes of these patients in order to describe the spectrum of metastases observed during the course of the disease in these three categories.
Fifteen of 70 BRCA1 mutation carriers, 12 of 49 BRCA2 mutation carriers and 58 of 254 patients with a family history of breast cancer but no mutation identified, developed metastatic disease. Thirteen of 15 BRCA1 carriers had been screened for mutation because of personal history of breast cancer associated with a family history of breast/ovarian cancer, according to the French Federation of Cancer Centres/INSERM guidelines [2], while two of them had pre-symptomatic BRCA1 testing. In addition, one BRCA2 carrier had pre-symptomatic testing, while 11 were identified as carriers because of personal and family history. All non-carriers had been screened for BRCA1 and BRCA2 mutation because of personal history and pedigree, according to the same guidelines. The median follow-up from the diagnosis of the first metastasis to the last visit or death was, respectively, 17.2 months (range 1.842) for BRCA1 patients, 44 months (range 1.8121) for BRCA2 and 46.5 months (range 1.5210) for non-carriers. As expected, tumours in BRCA1 carriers expressed estrogen receptors less frequently (Table 1). The spectrum of sites where metastases arose at any time during the course of the disease differed significantly within the three groups. BRCA1 carriers developed less bone (P = 0.01) and more lung (P = 0.005) metastases (Table 1). In addition, 10 of 15 (67%) BRCA1 mutation carriers developed brain metastases, while no (0%) BRCA2 carriers and six of 58 (10.3%) non-carriers did (P = 105). In line with the general policy of the centre, none of the patients had undergone screening for brain metastases; all cases were discovered because specific symptoms occurred. In BRCA1 carriers, the median time from the diagnosis of the first metastasis to that of brain involvement was 7.8 months (range 025). At follow-up, 12 of 15 BRCA1 carriers (80%), nine of 12 BRCA2 (75%) and 40 of 58 non-carriers (69%) had died. The shorter median follow-up registered among BRCA1 carriers seemed to be mostly related to shorter survival after the diagnosis of metastatic breast cancer, although the limited size of the sample prevents from any conclusion regarding this observation.
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Departments of 1 Medicine and 2 Radiology, Institut Gustave Roussy, Villejuif, France
* E-mail: delaloge{at}igr.fr
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