在靶向治疗时代激素受体阳性 HER2 阴性转移性乳腺癌中依维莫司联合依西美坦的治疗模式。
Patterns of treatment with everolimus exemestane in hormone receptor-positive HER2-negative metastatic breast cancer in the era of targeted therapy.
机构信息
Yale School of Medicine, 333 Cedar St., PO Box 208032, New Haven, CT, 05620, USA.
Yale COPPER, Harkness Office Building, 367 Cedar Street, New Haven, CT, 06510, USA.
出版信息
Breast Cancer Res. 2021 Jan 29;23(1):14. doi: 10.1186/s13058-021-01394-y.
BACKGROUND
There is currently no clinical trial data regarding the efficacy of everolimus exemestane (EE) following prior treatment with CDK4/6 inhibitors (CDK4/6i). This study assesses the use and efficacy of everolimus exemestane in patients with metastatic HR+ HER2- breast cancer previously treated with endocrine therapy (ET) or endocrine therapy + CDK4/6i.
METHODS
Retrospective analysis of electronic health record-derived data for HR+ HER2- metastatic breast cancer from 2012 to 2018. The proportion of patients receiving EE first-line, second-line, or third-line, and the median duration of EE prior to next line of treatment (TTNT) by line of therapy was calculated. OS for patients receiving EE first-line, second-line, or third-line, indexed to the date of first-line therapy initiation and stratified by prior treatment received, was calculated with Kaplan-Meier method with multivariable Cox proportional hazards regression analysis.
RESULTS
Six hundred twenty-two patients received EE first-line (n = 104, 16.7%), second-line (n = 273, 43.9%) or third-line (n = 245, 39.4%). Median TTNT was 8.3 months, 5.5 months, and 4.8 months respectively. Median TTNT of EE second-line was longer following prior ET alone compared to prior ET + CDK4/6i (6.2 months (95% CI 5.2, 7.3) vs 4.3 months (95% CI 3.2, 5.7) respectively, p = 0.03). Similarly, EE third-line following ET alone vs ET + CDK4/6i in first- or second-line resulted in median TTNT 5.6 months (95% CI 4.4, 6.9) vs 4.1 months (95% CI 3.6, 6.1) respectively, although this was not statistically significant (p = 0.08). Median OS was longer for patients who received EE following prior ET + CDK4/6i. EE second-line following ET + CDK 4/6i vs ET alone resulted in median OS 37.7 months vs. 32.7 months (p = 0.449). EE third-line following ET + CDK4/6i vs prior ET alone resulted in median OS 59.2 months vs. 40.8 months (p < 0.010). This difference in OS was not statistically significant when indexed to the start of EE therapy.
CONCLUSION
This study suggests that EE remains an effective treatment option after prior ET or ET + CDK4/6i use. Median TTNT of EE was longer for patients who received prior ET, whereas median OS was longer for patients who received prior ET + CDK4/6i. However, this improvement in OS was not statistically significant when indexed to the start of EE therapy suggesting that OS benefit is primarily driven by prior CDK4/6i use. EE remains an effective treatment option regardless of prior treatment option.
背景
目前尚无关于 CDK4/6 抑制剂(CDK4/6i)治疗后依维莫司联合依西美坦(EE)疗效的临床试验数据。本研究评估了转移性 HR+HER2-乳腺癌患者在接受内分泌治疗(ET)或 ET+CDK4/6i 治疗后的依维莫司联合依西美坦的使用和疗效。
方法
回顾性分析 2012 年至 2018 年电子病历中 HR+HER2-转移性乳腺癌患者的数据。计算按治疗线接受 EE 一线、二线或三线治疗的患者比例,以及按治疗线计算的 EE 治疗前的中位时间(TTNT)。采用 Kaplan-Meier 法计算接受 EE 一线、二线或三线治疗的患者的 OS,以一线治疗开始日期为索引,并按既往接受的治疗进行分层,同时采用多变量 Cox 比例风险回归分析。
结果
622 例患者接受 EE 一线(n=104,16.7%)、二线(n=273,43.9%)或三线(n=245,39.4%)治疗。中位 TTNT 分别为 8.3、5.5 和 4.8 个月。与 ET+CDK4/6i 相比,仅接受 ET 治疗的患者接受 EE 二线治疗的 TTNT 更长(6.2 个月(95%CI,5.2-7.3)比 4.3 个月(95%CI,3.2-5.7),p=0.03)。同样,与 ET+CDK4/6i 相比,在一线或二线接受 ET 后接受 EE 三线治疗的患者 TTNT 也更长,分别为 5.6 个月(95%CI,4.4-6.9)和 4.1 个月(95%CI,3.6-6.1),尽管这并不具有统计学意义(p=0.08)。与仅接受 ET 治疗的患者相比,接受 ET+CDK4/6i 后接受 EE 治疗的患者中位 OS 更长。与 ET 相比,ET+CDK4/6i 后接受 EE 二线治疗的患者中位 OS 为 37.7 个月 vs. 32.7 个月(p=0.449)。与 ET 相比,ET+CDK4/6i 后接受 EE 三线治疗的患者中位 OS 为 59.2 个月 vs. 40.8 个月(p<0.010)。当按 EE 治疗开始日期进行索引时,OS 差异没有统计学意义。
结论
本研究表明,依维莫司联合依西美坦在接受 ET 或 ET+CDK4/6i 治疗后仍然是一种有效的治疗选择。与接受 ET 治疗的患者相比,接受 EE 治疗的患者 TTNT 更长,而接受 ET+CDK4/6i 治疗的患者 OS 更长。然而,当按 EE 治疗开始日期进行索引时,OS 获益没有统计学意义,这表明 OS 获益主要由先前的 CDK4/6i 治疗驱动。依维莫司联合依西美坦仍然是一种有效的治疗选择,无论先前的治疗方案如何。
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