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Impact of Germline BRCA Mutation Status on Survival in Women with Metastatic Triple Negative Breast Cancer

机译:种系BRCA突变状态对转移三重阴性乳腺癌妇女生存的影响

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Purpose: To investigate the association between germline deleterious BRCA1 or BRCA2 mutations (gBRCA+) and overall survival (OS) for patients with metastatic triple negative breast cancer (mTNBC). Methods: An IRB approved prospective multisite registry enrolling stage I-IV TNBC patients from 2011-2018 was utilized. Demographics, treatments, genetic results, recurrence and survival were collected. OS was estimated according to the Kaplan-Meier method and compared between groups (gBRCA+and BRCA wild type, wt) by log-rank test. Cox regression model was used for univariate and multivariate analysis of factors associated with risk of death. Results: 100 patients with mTNBC were enrolled on the registry between 2011- 2018. For 100 patients, 20% (20/100) had de novo stage IV whereas 80% (80/100) had metastatic recurrence. 12% had gBRCA+ status; 72% were gBRCA wt type; and 16% had unknown gBRCA status. gBRCA+ patients were younger (49 vs. 57 years, p=0.02) but otherwise well matched to gBRCA wt including similar metastatic disease burden and prior treatments. No patients received a PARP inhibitor. With 31 months median follow-up, median overall survival was 21 months (95% CI [13-23] months) for all patients, 18 months (95% CI [15-27] months) for gBRCA wt patients and has not yet been reached for gBRCA+ patients (p=0.023). 3-year estimated OS is 63% in gBRCA+ versus 28% in gBRCA wt (p=0.02). On multivariate analysis, gBRCA+ was associated with reduced risk of death (HR=0.33; 95%CI [0.23-0.91], p=0.033). Conclusions: In patients with mTNBC gBRCA+ patients have a clinically significantly improved 3-year OS compared to gBRCA wt patients. Further research is needed to understand tumor and host biological reasons for this observation. As these patients are at risk for primary site progression and secondary breast and ovarian cancers, further research regarding the role of proactive surgical treatment in mTNBC with gBRCA mutation is warranted.
机译:目的:探讨种系有毒BRCA1或BRCA2突变(GBRCA +)和整体存活(GBRCA +)和转移性三重阴性乳腺癌(MTNBC)的总体存活(OS)之间的关联。方法:采用IRB批准的预期多路型注册阶段I-IV TNBC患者2011-2018患者。收集人口统计,治疗,遗传结果,复发和存活。根据KAPLAN-MEIER方法估计OS,并通过记录秩检验对比较(GBRCA +和BRCA野生型,WT)进行比较。 Cox回归模型用于与死亡风险相关的因素的单变量和多变量分析。结果:2011年至2018年患有100名患有MTNBC的患者。对于100名患者,20%(20/100)患有诺夫阶段IV,而80%(80/100)具有转移性复发。 12%有GBRCA +状态; 72%是GBRCA WT型; 16%有未知的GBRCA状态。 GBRCA +患者年轻(49 vs.57岁,P = 0.02),但否则与GBRCA WT相匹配,包括类似的转移性疾病负担和现有治疗。没有患者接受PARP抑制剂。患有31个月的后续行动后,中位数总生存率为21个月(95%CI [13-23]月份,所有患者为GBRCA WT患者的18个月(95%CI [15-27个月),还没有已达到GBRCA +患者(P = 0.023)。 3年估计的OS在GBRCA +中为63%,而GBRCA WT的28%(P = 0.02)。在多变量分析中,GBRCA +与降低死亡风险降低(HR = 0.33; 95%CI [0.23-0.91],P = 0.033)。结论:与MTNBC GBRCA +患者的患者与GBRCA WT患者相比,临床上显着改善的3年OS。需要进一步的研究来了解这种观察的肿瘤和宿主生物学原因。由于这些患者面临着原发性部位进展和次乳腺癌和卵巢癌的风险,因此有助于与GBRCA突变进行MTNBC主动手术治疗的进一步研究。

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