Robson M, Levin D, Federici M, Satagopan J, Bogolminy F, Heerdt A, Borgen P, McCormick B, Hudis C, Norton L, Boyd J, Offit K
Departments of Human Genetics and Medicine, Memorial Sloan-Kettering Cancer Center, New York, NY 10021, USA.
J Natl Cancer Inst. 1999 Dec 15;91(24):2112-7. doi: 10.1093/jnci/91.24.2112.
Germline mutations in the BRCA1 and BRCA2 genes are associated with an increased risk of breast cancer. Whether women with breast cancer who have inherited mutations in these genes have a different outcome after breast conservation therapy than women with "sporadic" cancer is unresolved. Consequently, we compared the outcomes after breast conservation therapy in Ashkenazi women with or without germline mutations in BRCA1 and/or BRCA2 (hereafter called BRCA).
We studied 305 women of Ashkenazi Jewish descent undergoing breast-conserving treatment for 329 invasive breast cancers. We reviewed their clinical records, retrieved their archival tissue samples, and tested those samples for the founder mutations BRCA1 185delAG, BRCA1 5382insC, and BRCA2 6174delT. Genetic results were linked to clinical data and outcomes by univariate and multivariate analyses. All Pvalues are two-sided.
We detected mutations in BRCA genes in 28 of 305 women. Women with BRCA mutations were more likely to be diagnosed with cancer before the age of 50 years (P<.001) and to have lymph node involvement (P =.04). Ipsilateral breast tumor recurrence was more common in women with BRCA mutations, although this did not reach statistical significance (relative risk [RR] = 1.79; 95% confidence interval [CI] = 0.64-5.03). Women with mutations were more likely to develop contralateral breast cancer (RR = 3.50; 95% CI = 1.78-8.74; P =.001). Distant disease-free survival was shorter in women with mutations (66.2% versus 84.3% at 10 years; P =.05), as was breast cancer-specific survival (71.9% versus 87.2% at 10 years; P =.02). Tumor stage and nodal status, but not mutation status, were predictive of distant disease-free and breast cancer-specific survival in multivariate analysis.
Women with BRCA founder mutations are at increased risk for breast cancer-related events after breast conservation. However, mutation status is not an independent predictor of survival and should not influence decisions regarding adjuvant therapy. The increased contralateral breast cancer risk in women heterozygous for BRCA mutations mandates careful surveillance.
BRCA1和BRCA2基因的种系突变与乳腺癌风险增加相关。与“散发性”癌症女性相比,携带这些基因遗传突变的乳腺癌女性在保乳治疗后的预后是否不同仍未明确。因此,我们比较了有或没有BRCA1和/或BRCA2基因种系突变(以下简称BRCA)的德系犹太女性保乳治疗后的预后。
我们研究了305名德系犹太裔女性,她们因329例浸润性乳腺癌接受了保乳治疗。我们查阅了她们的临床记录,获取了她们的存档组织样本,并检测这些样本是否存在BRCA1 185delAG、BRCA1 5382insC和BRCA2 6174delT这些始祖突变。通过单因素和多因素分析将基因检测结果与临床数据及预后相关联。所有P值均为双侧。
在305名女性中,我们检测到28名女性存在BRCA基因突变。携带BRCA基因突变的女性更有可能在50岁之前被诊断出患有癌症(P<0.001)且有淋巴结受累(P = 0.04)。携带BRCA基因突变的女性同侧乳腺肿瘤复发更为常见,尽管这未达到统计学意义(相对风险[RR]=1.79;95%置信区间[CI]=0.64 - 5.03)。携带突变的女性更有可能发生对侧乳腺癌(RR = 3.50;95%CI = 1.78 - 8.74;P = 0.001)。携带突变的女性远处无病生存期较短(10年时为66.2%对84.3%;P = 0.05),乳腺癌特异性生存期也较短(10年时为71.9%对87.2%;P = 0.02)。在多因素分析中肿瘤分期和淋巴结状态而非突变状态可预测远处无病生存期和乳腺癌特异性生存期。
携带BRCA始祖突变的女性在保乳治疗后发生乳腺癌相关事件的风险增加。然而,突变状态并非生存的独立预测因素,不应影响辅助治疗的决策。BRCA基因突变杂合女性对侧乳腺癌风险增加,需要进行仔细监测。
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