January 22, 2015
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BRCA testing has 'clear role' for triple-negative breast cancer

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The high prevalence of deleterious mutations in predisposition genes in patients with triple-negative breast cancer unselected for family history suggests germline genetic testing for BRCA1 and BRCA2 mutations may be appropriate in this population, according to study results.

However, further analyses of non-BRCA genes are needed to assess their utility in this setting, researchers wrote.

Fergus J. Couch, PhD, of the department of laboratory medicine and pathology at Mayo Clinic in Rochester, Minn., and colleagues evaluated data from 1,824 women with triple-negative breast cancer who were enrolled on one of 12 studies. All women were unselected for family history of breast or ovarian cancer, and most were non-Hispanic white (97%). The median age of the population at diagnosis was 51 years (range, 22-93).

Among the 1,510 patients with available data on family history, 34% (n=514) had one first- or second-degree relative with breast cancer, and 4% had a family history of ovarian cancer.

Researchers conducted germline DNA sequencing to identify the frequency of mutations in 17 predisposition genes. Overall, researchers identified 271 deleterious mutations in 14.6% of the population.

A majority of the mutations occurred in BRCA1 (57%) or BRCA2 (18%). Mutations in one of the other 15 genes occurred in 3.7% of patients, the most common of which were PALB2 (n=21), BARD1 (n=9), BRIP1 (n=8), RAD51D (n=7), RAD51C (n=6) and RAD50 (n=6).

Patients who harbored deleterious mutations were significantly younger at diagnosis (45 years vs. 52 years; P˂.001) and were more likely to have higher-grade tumors (P˂.001) than patients with wild-type genes.

A significant proportion of BRCA1 mutation carriers had a family history of breast cancer (50%; P˂.001) or ovarian cancer (18%; P˂.001). BRCA2 mutations were associated with a family history of ovarian cancer (13%; P˂.001). However, mutations in non-BRCA1/2 genes were not associated with a family history of breast or ovarian cancers.

BRCA1 and BRCA2 mutation testing has a clear role for patients with triple-negative breast cancer, many of whom will meet the current probability threshold guidelines,” Couch and colleagues concluded. “However, although inclusion of other susceptibility genes in the genetic testing panel is already a widely adopted strategy, it is important that clinical care providers appreciate the current lack of robust estimates of penetrance for many of these genes.”

Disclosure: See the study for a list of the researchers’ relevant financial disclosures.