Powles Trevor, Paterson Alexander, McCloskey Eugene, Schein Phil, Scheffler Bobbi, Tidy Alwynne, Ashley Sue, Smith Ian, Ottestad Lars, Kanis John
Parkside Oncology, London, UK.
Breast Cancer Res. 2006;8(2):R13. doi: 10.1186/bcr1384. Epub 2006 Mar 15.
Experimental and clinical data show that the oral bisphosphonate clodronate (Bonefos) can inhibit tumor-induced osteoclastic bone resorption. This randomized, double-blind, placebo-controlled, multicenter trial was designed to determine if the addition of oral clodronate to standard treatment for primary operable breast cancer could reduce the subsequent occurrence of bone metastases and thereby improve overall survival.
1,069 patients with primary operable stage I-III breast cancer were randomized to receive oral clodronate (1,600 mg/day) or placebo for 2 years, in conjunction with standard treatment for primary breast cancer including surgery, radiotherapy, adjuvant chemotherapy, and/or tamoxifen. All patients were assessed for bone metastases at two and five years and additionally when clinically indicated. Survival status was determined as of the close of the study on 30 June 2000 with a median follow up of 5.6 years. The treatment arms were compared using the unstratified log-rank test. Hazard ratios (HRs) with 95% confidence intervals were calculated.
Oral clodronate significantly reduced the risk of bone metastases in all patients over the 5 year study period (51 patients versus 73 patients with placebo; HR = 0.692, P = 0.043); the difference was also statistically significant over the 2 year medication period (19 patients versus 35 patients with placebo; HR = 0.546, P = 0.031). These differences were most pronounced in patients with stage II/III disease (39 patients versus 64 patients with placebo, HR = 0.592, P = 0.009 over 5 years; 16 patients versus 32 patients with placebo, HR= 0.496, P = 0.020 over 2 years). Survival data also favoured the clodronate arm (HR for all patients = 0.768, P = 0.048; HR for stage II/III disease = 0.743, P = 0.041), although this was not significant due to multiple analyses. Oral clodronate was well tolerated, with mild-to-moderate diarrhoea being the most frequently reported adverse event.
These results confirm that oral clodronate will significantly improve the 5 year bone relapse free survival when used as a supplementary adjuvant treatment for patients receiving standard treatment for primary operable breast cancer.
实验和临床数据表明,口服双膦酸盐氯膦酸盐(博宁)可抑制肿瘤诱导的破骨细胞骨吸收。本随机、双盲、安慰剂对照、多中心试验旨在确定在原发性可手术乳腺癌的标准治疗中添加口服氯膦酸盐是否能减少随后骨转移的发生,从而提高总生存率。
1069例原发性I - III期可手术乳腺癌患者被随机分为接受口服氯膦酸盐(1600毫克/天)或安慰剂治疗2年,同时接受原发性乳腺癌的标准治疗,包括手术、放疗、辅助化疗和/或他莫昔芬。所有患者在2年和5年时评估骨转移情况,临床有指征时也进行评估。截至2000年6月30日研究结束时确定生存状态,中位随访时间为5.6年。使用未分层对数秩检验比较治疗组。计算风险比(HR)及95%置信区间。
在5年研究期内,口服氯膦酸盐显著降低了所有患者骨转移的风险(51例患者发生骨转移,安慰剂组为73例;HR = 0.692,P = 0.043);在2年用药期内差异也具有统计学意义(19例患者发生骨转移,安慰剂组为35例;HR = 0.546,P = 0.031)。这些差异在II/III期疾病患者中最为明显(5年时,39例患者发生骨转移,安慰剂组为64例,HR = 0.592,P = 0.009;2年时,16例患者发生骨转移,安慰剂组为32例,HR = 0.496,P = 0.020)。生存数据也有利于氯膦酸盐组(所有患者的HR = 0.768,P = 0.048;II/III期疾病患者的HR = 0.743,P = 0.041),尽管由于多次分析该结果不显著。口服氯膦酸盐耐受性良好,轻度至中度腹泻是最常报告的不良事件。
这些结果证实,口服氯膦酸盐作为接受原发性可手术乳腺癌标准治疗患者的辅助治疗药物,可显著提高5年无骨复发生存率。
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