在转移性乳腺癌化疗方案中添加药物。
Addition of drug/s to a chemotherapy regimen for metastatic breast cancer.
作者信息
Butters Daria J, Ghersi Davina, Wilcken Nicholas, Kirk Steven J, Mallon Peter T
机构信息
PAREXEL International Ltd, The Quays,, 101-105 Oxford Road,, Uxbridge, Middlesex, UK, UB8 1LZ.
出版信息
Cochrane Database Syst Rev. 2010 Nov 10;2010(11):CD003368. doi: 10.1002/14651858.CD003368.pub3.
BACKGROUND
The addition of a chemotherapy drug or drugs to an established regimen is one method used to increase the dose and intensity of treatment for metastatic breast cancer.
OBJECTIVES
To assess the effects of adding one or more chemotherapy drugs to an established regimen in women with metastatic breast cancer.
SEARCH STRATEGY
We searched the Cochrane Breast Cancer Group's Specialised Register (to August 2009) using the codes for "advanced breast cancer" and "chemotherapy". This review is an update of the original Cochrane Review (Issue 3, 2006).
SELECTION CRITERIA
Randomised trials with a first line regimen of at least two chemotherapy drugs compared to the same regimen plus the addition of one or more chemotherapy drugs in women with metastatic breast cancer.
DATA COLLECTION AND ANALYSIS
Two authors extracted data independently from published trials. We derived hazard ratios (HR) from time-to-event outcomes where possible, and used a fixed-effect model for meta-analysis. We analysed response rates as dichotomous variables and extracted toxicity data where available.
MAIN RESULTS
We identified 17 trials reporting on 22 treatment comparisons (2674 patients randomised). Fifteen trials (20 treatment comparisons) reported results for tumour response and 11 trials (14 treatment comparisons) published time-to-event data for overall survival. There were 1532 deaths in 2116 women randomised to trials of the addition of a drug to the regimen and control (the regimen alone). There was no detectable difference in overall survival between these patients, with an overall HR of 0.96 (95% confidence interval (CI) 0.87 to 1.07, P = 0.47) and no significant heterogeneity. We found no difference in time to progression between these regimens, with an overall HR of 0.93 (95% CI 0.81 to 1.07, P = 0.31) and no significant heterogeneity. Addition of a drug to the regimen was favourably associated with overall tumour response rates (odds ratio 1.21, 95% CI 1.01 to 1.44, P = 0.04) although we observed significant heterogeneity for this outcome across the trials. Where measured, acute toxicities such as alopecia, nausea and vomiting and leucopenia were more common with the addition of a drug.
AUTHORS' CONCLUSIONS: The addition of one or more drugs to the regimen shows a statistically significant advantage for tumour response in women with metastatic breast cancer but the results suggest no difference in survival time or time to progression. The positive effect on tumour response was also associated with increased toxicity.
背景
在既定治疗方案中添加一种或多种化疗药物是用于增加转移性乳腺癌治疗剂量和强度的一种方法。
目的
评估在既定治疗方案中添加一种或多种化疗药物对转移性乳腺癌女性患者的影响。
检索策略
我们使用“晚期乳腺癌”和“化疗”的代码检索了Cochrane乳腺癌小组专业注册库(截至2009年8月)。本综述是原始Cochrane综述(2006年第3期)的更新。
选择标准
转移性乳腺癌女性患者中,将至少两种化疗药物的一线治疗方案与相同方案加一种或多种化疗药物进行比较的随机试验。
数据收集与分析
两位作者独立从已发表的试验中提取数据。我们尽可能从事件发生时间结局中得出风险比(HR),并使用固定效应模型进行荟萃分析。我们将缓解率作为二分变量进行分析,并在可获得的情况下提取毒性数据。
主要结果
我们确定了17项试验,报告了22项治疗比较(2674例患者随机分组)。15项试验(20项治疗比较)报告了肿瘤反应结果,11项试验(14项治疗比较)发表了总生存的事件发生时间数据。在2116名随机分组接受在方案中加药试验和对照(仅方案)的女性中,有1532例死亡。这些患者的总生存无明显差异,总体HR为0.96(95%置信区间(CI)0.87至1.07,P = 0.47),且无显著异质性。我们发现这些方案在疾病进展时间上无差异,总体HR为0.93(95%CI 0.81至1.07,P = 0.31),且无显著异质性。在方案中加药与总体肿瘤缓解率呈有利关联(优势比1.21,95%CI 1.01至1.44,P = 0.04),尽管我们观察到各试验在该结局上存在显著异质性。在有测量的情况下,脱发、恶心、呕吐和白细胞减少等急性毒性在加药时更常见。
作者结论
在方案中添加一种或多种药物对转移性乳腺癌女性患者的肿瘤反应显示出统计学上的显著优势,但结果表明在生存时间或疾病进展时间上无差异。对肿瘤反应的积极影响也与毒性增加有关。
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