来曲唑辅助治疗患者中塞来昔布和低剂量阿司匹林对结局的影响:CCTG MA.27.
Effects of Celecoxib and Low-dose Aspirin on Outcomes in Adjuvant Aromatase Inhibitor-Treated Patients: CCTG MA.27.
机构信息
Center for Oncology, Hematology and Palliative Care, Wilhelminen Hospital, Vienna, Austria.
Mater Misericordiae University Hospital, Dublin, Ireland.
出版信息
J Natl Cancer Inst. 2018 Sep 1;110(9):1003-1008. doi: 10.1093/jnci/djy017.
BACKGROUND
Celecoxib and low-dose aspirin might decrease risk of breast cancer recurrence.
METHODS
In the Canadian Cancer Trials Group MA.27, postmenopausal hormone receptor-positive breast cancer patients were randomly assigned (2 × 2) to adjuvant exemestane or anastrozole, and celecoxib or placebo. Low-dose aspirin of 81 mg or less was a stratification factor. Due to concerns about cardiac toxicity, celecoxib use was stopped in December 2004, while stratification by aspirin use was removed through protocol amendment. We examined the effects of celecoxib and low-dose aspirin on event-free survival (EFS), defined as time from random assignment to time of locoregional or distant disease recurrence, new primary breast cancer, or death from any cause; distant disease-free survival (DDFS); and overall survival (OS). All statistical tests were two-sided.
RESULTS
Random assignment to celecoxib (n = 811, 50.0%) or placebo (n = 811, 50.0%) was discontinued after 18 months (n = 1622). At a median of 4.1 years' follow-up, among 1622 patients, 186 (11.5%) patients had an EFS event: 80 (4.9%) had distant relapse, and 125 (7.7%) died from any cause. Celecoxib did not statistically significantly impact EFS, DDFS, or OS in univariate analysis (respectively, P = .92, P = .55, and P = .56) or multivariable analysis (respectively, P = .74, P = .60, and P = .76). Low-dose aspirin use (aspirin users n = 476, 21.5%; non-aspirin users n = 1733, 78.5%) was associated in univariate analyses with worse EFS (hazard ratio [HR] = 1.48, 95% confidence interval [CI] = 1.12 to 1.96, P = 0.006) and worse OS (HR = 1.87, 95% CI = 1.35 to 2.61, P < .001). After adjusting for baseline characteristics and treatment arm, aspirin use showed no statistical association with EFS (P = .08) and DDFS (P = .82), but was associated with statistically worse OS (HR = 1.67, 95% CI = 1.13 to 2.49, P = .01).
CONCLUSION
Random assignment to short-term (≤18 months) celecoxib as well as use of low-dose aspirin showed no effect on DDFS and EFS in multivariable analysis. Low-dose aspirin increased "all-cause" mortality, presumably because of higher preexisting cardiovascular risks.
背景
塞来昔布和低剂量阿司匹林可能降低乳腺癌复发的风险。
方法
在加拿大癌症临床试验组 MA.27 中,绝经后激素受体阳性乳腺癌患者被随机分配(2×2)接受辅助依西美坦或阿那曲唑,以及塞来昔布或安慰剂。低剂量阿司匹林(81 毫克或以下)是分层因素。由于对心脏毒性的担忧,塞来昔布的使用于 2004 年 12 月停止,而通过方案修正案取消了阿司匹林使用的分层。我们研究了塞来昔布和低剂量阿司匹林对无事件生存(EFS)的影响,EFS 定义为从随机分组到局部或远处疾病复发、新原发性乳腺癌或任何原因死亡的时间;远处无病生存(DDFS);以及总生存(OS)。所有统计检验均为双侧。
结果
随机分配至塞来昔布(n=811,50.0%)或安慰剂(n=811,50.0%)的患者在 18 个月后(n=1622)停止治疗。在中位数为 4.1 年的随访中,在 1622 例患者中,有 186 例(11.5%)发生 EFS 事件:80 例(4.9%)发生远处复发,125 例(7.7%)死于任何原因。在单变量分析(分别为 P=0.92、P=0.55 和 P=0.56)或多变量分析(分别为 P=0.74、P=0.60 和 P=0.76)中,塞来昔布对 EFS、DFS 和 OS 均无统计学显著影响。低剂量阿司匹林的使用(阿司匹林使用者 n=476,21.5%;非阿司匹林使用者 n=1733,78.5%)在单变量分析中与 EFS 较差相关(风险比 [HR] = 1.48,95%置信区间 [CI] = 1.12 至 1.96,P=0.006)和 OS 较差(HR = 1.87,95% CI = 1.35 至 2.61,P<0.001)。在调整基线特征和治疗臂后,阿司匹林的使用与 EFS(P=0.08)和 DDFS(P=0.82)无统计学关联,但与较差的 OS 有统计学关联(HR = 1.67,95% CI = 1.13 至 2.49,P=0.01)。
结论
在多变量分析中,短期(≤18 个月)塞来昔布的随机分配以及低剂量阿司匹林的使用均对 DDFS 和 EFS 无影响。低剂量阿司匹林增加了“全因”死亡率,可能是因为存在较高的预先存在的心血管风险。
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