Hassan Hend, Allen Isaac, Rahman Tameera, Allen Sophie, Knott Craig, Huntley Catherine, Loong Lucy, Garrett Alice, Walburga Yvonne, Morris Eva, Hardy Steven, Torr Bethany, McRonald Fiona, Vernon Sally, Lüchtenborg Margreet, Pethick Joanna, Santaniello Francesco, Goel Shilpi, Eccles Diana M, Turnbull Clare, Tischkowitz Marc, Pharoah Paul, Antoniou Antonis C
Centre for Cancer Genetic Epidemiology, Department of Public Health and Primary Care, University of Cambridge, Cambridge, UK; NHS England, National Disease Registration Service, Leeds, UK.
Centre for Cancer Genetic Epidemiology, Department of Public Health and Primary Care, University of Cambridge, Cambridge, UK; NHS England, National Disease Registration Service, Leeds, UK.
Lancet Oncol. 2025 Jun;26(6):771-780. doi: 10.1016/S1470-2045(25)00156-1. Epub 2025 May 8.
Carriers of BRCA1 and BRCA2 pathogenic variants are at elevated risk of developing breast and ovarian cancers. To mitigate ovarian cancer risk, bilateral salpingo-oophorectomy (BSO) is commonly recommended for unaffected carriers and those with personal breast cancer history. Assessing BSO's long-term health outcomes in carriers with previous breast cancer history is essential. This study aims to examine the association between BSO and long-term health outcomes in individuals carrying pathogenic variants in BRCA1 and BRCA2 and with personal history of breast cancer.
Data from the National Cancer Registration Dataset (NCRD) were linked with data from genetic testing laboratories to identify carriers of BRCA1 and BRCA2 pathogenic variants affected by breast cancer using pseudonymised patient identifiers. Further linkage to the Hospital Episode Statistics-Admitted Patient Care (HES-APC) dataset identified patients who had undergone BSO. Women aged 20-75 years, with a diagnosis of breast cancer as their first primary malignancy in 1995-2019 were eligible. Long-term health outcomes were identified from HES-APC and NCRD. Missing data were imputed using multivariate imputations by chained equations. Multivariable Cox regression was used to examine the associations with mortality (all-cause mortality, breast cancer-specific mortality, and non-breast cancer-specific mortality), second non-breast cancer, cardiovascular diseases, ischaemic heart disease, cerebrovascular diseases, contralateral breast cancer, and depression. Analyses were adjusted for age at diagnosis, diagnosis year, ethnicity, deprivation index, tumour characteristics, Charlson comorbidity index, cancer treatment, and second cancer diagnosis before the start of follow-up.
We included 1674 BRCA1, 1740 BRCA2, and nine BRCA1 and BRCA2 carriers who were diagnosed with breast cancer between 1995 and 2019, with median follow-up time of 5·5 years (IQR 3·4-8·2). The study population (n=3423) consisted of 3002 (88·7%) White, 170 (5·0%) Asian, 59 (1·7%) Black, 26 (0·8%) mixed, and 74 (2·2%) other ethnic groups, and 92 (2·7%) had missing ethnicity. The uptake of BSO was significantly lower among Black women (odds ratio [OR] vs White women 0·48, 95% CI 0·34-0·67), and Asian women (0·47, 0·27-0·82). BSO uptake was higher in women living in the least socioeconomically deprived areas (OR vs most deprived 1·38, 95% CI [1·10-1·72]). BSO was associated with a reduced risk of all-cause mortality for both BRCA1 and BRCA2 pathogenic variant carriers (HR 0·52, 95% CI 0·41-0·64) and reduced breast cancer-specific mortality (BRCA1: HR 0·62, 95% CI 0·42-0·92 and BRCA2: 0·48, 0·34-0·68). It was also associated with a reduced risk of second non-breast cancer in the combined BRCA1 and BRCA2 sample (HR 0·59, 95% CI 0·37-0·94). There BSO was not associated with increased risk of cardiovascular diseases (HR 0·73, 95% CI 0·53-1·01), ischaemic heart disease (1·04, 0·48-2·26), cerebrovascular disease (0·32, 0·11-0·90), non-breast cancer specific mortality (0·72, 0·45-1·16), contralateral breast cancer (1·18, 0·64-2·16), or depression (0·94, 0·62-1·42).
The evidence supports offering BSO to BRCA1 and BRCA2 pathogenic variant carrriers with a personal history of breast cancer, as they appear to benefit from having the procedure, without evidence of an increased risk of adverse long-term health outcomes.
Cancer Research UK.
携带BRCA1和BRCA2致病变异的个体患乳腺癌和卵巢癌的风险升高。为降低卵巢癌风险,对于未受影响的携带者以及有个人乳腺癌病史的携带者,通常建议进行双侧输卵管卵巢切除术(BSO)。评估BSO对有乳腺癌病史的携带者的长期健康结局至关重要。本研究旨在探讨BRCA1和BRCA2致病变异携带者且有个人乳腺癌病史者中,BSO与长期健康结局之间的关联。
将国家癌症登记数据集(NCRD)的数据与基因检测实验室的数据相链接,使用匿名患者标识符识别受乳腺癌影响的BRCA1和BRCA2致病变异携带者。进一步与医院事件统计-住院患者护理(HES-APC)数据集相链接,以识别接受过BSO的患者。纳入1995年至2019年期间诊断为乳腺癌作为首个原发性恶性肿瘤的20至75岁女性。从HES-APC和NCRD中确定长期健康结局。使用链式方程的多变量插补法对缺失数据进行插补。采用多变量Cox回归分析来研究与死亡率(全因死亡率、乳腺癌特异性死亡率和非乳腺癌特异性死亡率)、第二种非乳腺癌、心血管疾病、缺血性心脏病、脑血管疾病、对侧乳腺癌和抑郁症之间的关联。分析对诊断时年龄、诊断年份、种族、贫困指数、肿瘤特征、Charlson合并症指数、癌症治疗以及随访开始前的第二种癌症诊断进行了校正。
我们纳入了1674名BRCA1携带者、1740名BRCA2携带者以及9名同时携带BRCA1和BRCA2变异且在1995年至2019年间被诊断为乳腺癌的携带者,中位随访时间为5.5年(四分位间距3.4 - 8.2年)。研究人群(n = 3423)包括3002名(88.7%)白人、170名(5.0%)亚洲人、59名(1.7%)黑人、26名(0.8%)混血以及74名(2.2%)其他种族群体,92名(2.7%)种族信息缺失。黑人女性接受BSO的比例显著低于白人女性(比值比[OR]对比白人女性为0.48,95%置信区间0.34 - 0.67),亚洲女性也较低(0.47,0.27 - 0.82)。生活在社会经济最不贫困地区的女性接受BSO的比例更高(OR对比最贫困地区为1.38,95%置信区间[1.10 - 1.72])。对于BRCA1和BRCA2致病变异携带者,BSO与全因死亡率降低相关(风险比[HR]0.52,95%置信区间0.41 - 0.64),且乳腺癌特异性死亡率降低(BRCA1:HR 0.62,95%置信区间0.42 - 0.92;BRCA2:0.48,0.34 - 0.68)。在BRCA1和BRCA2合并样本中,它还与第二种非乳腺癌风险降低相关(HR 0.59,95%置信区间0.37 - 0.94)。BSO与心血管疾病风险增加无关(HR 0.73,95%置信区间0.53 - 1. 01)、缺血性心脏病(1.04,0.48 - 2.26)、脑血管疾病(0.32,0.11 - 0.90)、非乳腺癌特异性死亡率(0.72,0.45 - 1.16)、对侧乳腺癌(1.18,0.64 - 2.16)或抑郁症(0.94,0.62 - 1.42)无关。
有证据支持为有个人乳腺癌病史的BRCA1和BRCA2致病变异携带者提供BSO,因为他们似乎从该手术中获益,且没有证据表明长期健康不良结局风险增加。
英国癌症研究基金会。
