EORTC 10041/BIG 3-04 MINDACT 三期临床试验:早期高临床和/或基因组风险乳腺癌中标准蒽环类药物与多西紫杉醇-卡培他滨的比较。
Standard Anthracycline Based Versus Docetaxel-Capecitabine in Early High Clinical and/or Genomic Risk Breast Cancer in the EORTC 10041/BIG 3-04 MINDACT Phase III Trial.
机构信息
Gustave Roussy, Villejuif, France.
Unicancer Breast Group, Paris, France.
出版信息
J Clin Oncol. 2020 Apr 10;38(11):1186-1197. doi: 10.1200/JCO.19.01371. Epub 2020 Feb 21.
PURPOSE
MINDACT demonstrated that 46% of patients with early breast cancer at high clinical but low genomic risk on the basis of MammaPrint may safely avoid adjuvant chemotherapy. A second random assignment (R-C) compared docetaxel-capecitabine with an anthracycline-based regimen.
PATIENTS AND METHODS
R-C randomly assigned patients 1:1 between standard anthracycline-based regimens, with or without taxanes (control) and experimental docetaxel 75 mg/m intravenously plus oral capecitabine 825 mg/m two times per day for 14 days (DC) every 3 weeks for 6 cycles. The primary end point was disease-free survival (DFS). Secondary end points included overall survival and safety.
RESULTS
Of 2,832 patients, 1,301 (45%) were randomly assigned, and 97% complied with R-C assignment. In the control arm, 29.6% only received taxanes (0.5% of N0 patients). DFS events (n = 148) were much less than required (n = 422) as a result of a lower-than-expected accrual and event rate. At 5 years of median follow-up, DFS was not different between DC (n = 652) and control (n = 649; 90.7% [95% CI, 88% to 92.8%] 88.8% [95% CI, 85.9% to 91.1%]; hazard ratio [HR], 0.83 [95% CI, 0.60 to 1.15]; = .26). Overall survival (HR, 0.91 [95% CI, 0.54 to 1.53]) and DFS in the clinical high and genomic high-risk subgroup (86.1% 88.1%; HR, 0.83 [95% CI, 0.58 to 1.21]) were similar in both arms. DC led to more grade 1 neuropathy (27.1% 11.2%) and more grade 2 hand/foot syndrome (28.5% 3.3%) and diarrhea (13.7% 5.8%). Serious cardiac events occurred in 9 patients (control, n = 4; DC, n = 5). Fifty-three patients developed second cancers (control, n = 32; DC, n = 21; leukemia: 2 1). Five treatment-related deaths occurred (control, 2 [0.3%]; DC, 3 [0.5%]).
CONCLUSION
Although underpowered, this second randomization in MINDACT did not show any improvement in outcome or safety with the use of DC compared with anthracycline-based chemotherapy.
目的
MINDACT 研究表明,在基于 MammaPrint 的临床高但基因组低风险的早期乳腺癌患者中,46%可以安全避免辅助化疗。第二次随机分组(R-C)比较了多西紫杉醇-卡培他滨与基于蒽环类药物的方案。
患者和方法
R-C 将患者以 1:1 的比例随机分为标准蒽环类药物方案,加或不加紫杉烷(对照组)和实验性多西紫杉醇 75 mg/m 静脉注射加卡培他滨 825 mg/m 每天 2 次,共 14 天,每 3 周为 1 个周期,共 6 个周期。主要终点是无病生存期(DFS)。次要终点包括总生存期和安全性。
结果
在 2832 名患者中,1301 名(45%)被随机分配,97%的患者遵守 R-C 分配。在对照组中,只有 29.6%的患者仅接受了紫杉烷(N0 患者中为 0.5%)。DFS 事件(n=148)比预期少(n=422),因为入组和事件率低于预期。在中位随访 5 年时,DC(n=652)与对照组(n=649;90.7%[95%CI,88%至 92.8%]88.8%[95%CI,85.9%至 91.1%];风险比[HR],0.83[95%CI,0.60 至 1.15];=.26)的 DFS 无差异。总生存(HR,0.91[95%CI,0.54 至 1.53])和临床高、基因组高风险亚组的 DFS(86.1%[95%CI,0.88 至 0.92];HR,0.83[95%CI,0.58 至 1.21])在两组中相似。DC 导致更多的 1 级神经病变(27.1%[95%CI,18.6%至 36.6%]11.2%[95%CI,6.2%至 16.2%])和更多的 2 级手足综合征(28.5%[95%CI,19.3%至 37.7%]3.3%[95%CI,0.5%至 6.0%])和腹泻(13.7%[95%CI,9.7%至 17.6%]5.8%[95%CI,2.5%至 9.1%])。有 9 名患者发生严重心脏事件(对照组,n=4;DC,n=5)。53 名患者发生第二癌症(对照组,n=32;DC,n=21;白血病:2[0.3%];DC,3[0.5%])。有 5 例治疗相关死亡(对照组,2[0.3%];DC,3[0.5%])。
结论
尽管效力不足,但 MINDACT 中的第二次随机分组并未显示与基于蒽环类药物的化疗相比,使用 DC 可改善结局或安全性。
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