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abstract
Twenty-one–gene recurrence score assay in BRCA-associated versus sporadic breast cancers: Differences based on germline mutation status
BACKGROUND
Biological differences between BRCA-associated
breast cancer and sporadic breast cancer may warrant different adjuvant
chemotherapy (ACRx) recommendations despite similar phenotypic
features. A 21-gene expression profile (Oncotype DX) generates a
prognostic recurrence score (RS) that predicts the ACRx benefit in
patients with hormone receptor–positive breast cancer. No reports
describe assay results for BRCA-associated breast cancer.
METHODS
A
review of Memorial Sloan Kettering Cancer Center databases identified
4908 patients with hormone receptor–positive, node-negative breast
cancer who underwent Oncotype DX testing between July 2006 and March
2014. BRCA1/BRCA2 carriers (cases) were identified and
matched (1:2) by age at diagnosis and tumor size to noncarrier
controls. Two-sample nonparametric tests were used to compare the
baseline characteristics, RSs, and risk stratification between BRCA1 and BRCA2 patients. Conditional logistic regression was used to assess these differences by mutational status.
RESULTS
Fifty mutation-associated cases (19 BRCA1 cases and 31 BRCA2 cases) and 100 controls who were well matched for age (P = .9) and tumor size (P = .6) were included. BRCA1 and BRCA2 carriers had similar median RSs (P = .6) and risk category stratification (P = .3). The median RS was higher for cases versus controls (24 vs 16; P < .0001). Risk stratification also differed by mutational status (P
= .0002). Cases had more high-risk disease (28% vs 7%) and
intermediate-risk disease (56% vs 36%) and less low-risk disease (16% vs
57%). Cases were more likely than controls to receive ACRx (74% vs 46%;
P = .002).
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