Goss Paul E, Ingle James N, Martino Silvana, Robert Nicholas J, Muss Hyman B, Piccart Martine J, Castiglione Monica, Tu Dongsheng, Shepherd Lois E, Pritchard Kathleen I, Livingston Robert B, Davidson Nancy E, Norton Larry, Perez Edith A, Abrams Jeffrey S, Cameron David A, Palmer Michael J, Pater Joseph L
Division of Hematology and Oncology, Massachusetts General Hospital, Boston, MA, USA.
J Clin Oncol. 2007 May 20;25(15):2006-11. doi: 10.1200/JCO.2006.09.4482. Epub 2007 Apr 23.
Controversy exists regarding estrogen (ER) and progesterone (PgR) receptor expression on efficacy of adjuvant endocrine therapy. In the ATAC (Arimidex, Tamoxifen, Alone or in Combination) trial, the benefit of anastrozole over tamoxifen was substantially greater in ER+/PgR-than ER+/PgR+ tumors. In BIG 1-98 (Breast International Group), the benefits of letrozole over tamoxifen were the same in ER+ tumors irrespective of PgR. MA.17 randomized postmenopausal women after 5 years of tamoxifen, to letrozole or placebo. We present outcomes according to tumor receptor status.
Disease-free survival (DFS) and other outcomes were assessed in subgroups by ER and PgR status using Cox's proportional hazards model, adjusting for nodal status and prior adjuvant chemotherapy.
The DFS hazard ratio (HR) for letrozole versus placebo in ER+/PgR+ tumors (N = 3,809) was 0.49 (95% CI, 0.36 to 0.67) versus 1.21 (95% CI, 0.63 to 2.34) in ER+/PgR-tumors (n = 636). ER+/PgR+ letrozole patients experienced significant benefit in distant DFS (DDFS; HR = 0.53; 95% CI, 0.35 to 0.80) and overall survival (OS; HR = 0.58; 95% CI, 0.37 to 0.90). A statistically significant difference in treatment effect between ER+/PgR+ and ER+/PgR-subgroups for DFS was observed (P = .02), but not for DDFS (P = .06) or OS (P = .09).
These results suggest greater benefit for letrozole in DFS, DDFS, and OS in patients with ER+/PgR+ tumors, implying greater activity of letrozole in tumors with a functional ER. However, because this is a subset analysis and receptors were not measured centrally, we caution against using these results for clinical decision making.
关于雌激素(ER)和孕激素(PgR)受体表达对辅助内分泌治疗疗效的影响存在争议。在ATAC(阿那曲唑、他莫昔芬,单独或联合使用)试验中,阿那曲唑相对于他莫昔芬的获益在ER + /PgR - 肿瘤中比在ER + /PgR + 肿瘤中显著更大。在BIG 1 - 98(国际乳腺癌研究组)试验中,来曲唑相对于他莫昔芬的获益在ER + 肿瘤中与PgR状态无关。MA.17试验将接受5年他莫昔芬治疗后的绝经后女性随机分为来曲唑组或安慰剂组。我们根据肿瘤受体状态呈现结果。
使用Cox比例风险模型,根据ER和PgR状态在亚组中评估无病生存期(DFS)和其他结果,并对淋巴结状态和先前的辅助化疗进行校正。
在ER + /PgR + 肿瘤(N = 3,809)中,来曲唑相对于安慰剂的DFS风险比(HR)为0.49(95%CI,0.36至0.67),而在ER + /PgR - 肿瘤(n = 636)中为1.21(95%CI,0.63至2.34)。ER + /PgR + 的来曲唑治疗患者在远处无病生存期(DDFS;HR = 0.53;95%CI,0.35至0.80)和总生存期(OS;HR = 0.58;95%CI,0.37至0.90)方面有显著获益。观察到ER + /PgR + 和ER + /PgR - 亚组之间在DFS的治疗效果上有统计学显著差异(P = 0.02),但在DDFS(P = 0.06)或OS(P = 0.09)方面没有。
这些结果表明,来曲唑对ER + /PgR + 肿瘤患者的DFS﹑DDFS和OS有更大益处,这意味着来曲唑在具有功能性ER的肿瘤中活性更高。然而,由于这是一项亚组分析且受体并非集中测量,我们谨慎建议不要将这些结果用于临床决策。
