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口服双膦酸盐作为可手术乳腺癌的辅助治疗

Oral bisphosphonates as adjuvant therapy for operable breast cancer.

作者信息

Powles Trevor, McCroskey Eugene, Paterson Alexander

机构信息

Parkside Oncology Clinic, London, and University of Sheffield, United Kingdom.

出版信息

Clin Cancer Res. 2006 Oct 15;12(20 Pt 2):6301s-6304s. doi: 10.1158/1078-0432.CCR-06-1211.

Abstract

Bone is the most common site of metastatic spread from primary operable breast cancer, causing pain, fractures, and hypercalcemia. This spread depends on the release of osteolytic substances by the cancer cells, which activate osteoclasts to cause bone resorption. The osteoclasts also release growth factors that can act back on the cancer cells to activate growth. This vicious circle thereby facilitates the growth of metastases in bone, thus making this a preferential site for relapse. Agents, such as the bisphosphonates, which block osteoclast function, have been shown to reduce the progression of established bone metastases. The oral bisphosphonate clodronate (1,600 mg/d) is effective for treatment of patients with bone metastases. When used as adjuvant therapy, given to patients with operable breast cancer for 2 years, clodronate has been reported to significantly reduce the risk of bone metastases during the 2-year study period [19 clodronate patients versus 35 placebo patients; hazard ratio (HR), 0.546; P=0.03] and 5-year study period (51 clodronate patients versus 73 placebo patients; HR, 0.692; P=0.04) with a significant reduction in mortality (HR, 0.768; P=0.048). This benefit, together with the low toxicity and safety of clodronate, supports its use as additional adjuvant therapy for patients with primary breast cancer. Further, similarly designed trials are under way to establish the optimal duration of therapy, the efficacy in stage I disease, and the relative potential of other bisphosphonates, particularly the more powerful aminobisphosphonates, such as ibandronate and zoledronate.

摘要

骨是原发性可手术乳腺癌转移扩散最常见的部位,会引起疼痛、骨折和高钙血症。这种扩散取决于癌细胞释放的溶骨物质,这些物质激活破骨细胞导致骨吸收。破骨细胞还释放生长因子,这些因子可作用于癌细胞以激活其生长。这种恶性循环从而促进了骨转移瘤的生长,因此使骨成为复发的优先部位。已证明,诸如双膦酸盐之类的药物可阻断破骨细胞功能,从而减少已形成的骨转移的进展。口服双膦酸盐氯膦酸盐(1600毫克/天)对骨转移患者的治疗有效。当用作辅助治疗,给予可手术乳腺癌患者2年时,据报道氯膦酸盐在2年研究期内(19例氯膦酸盐患者对35例安慰剂患者;风险比[HR],0.546;P = 0.03)和5年研究期内(51例氯膦酸盐患者对73例安慰剂患者;HR,0.692;P = 0.04)可显著降低骨转移风险,且死亡率显著降低(HR,0.768;P = 0.048)。这种益处,连同氯膦酸盐的低毒性和安全性,支持将其用作原发性乳腺癌患者的额外辅助治疗。此外,正在进行类似设计的试验,以确定最佳治疗持续时间、I期疾病的疗效以及其他双膦酸盐,特别是更强效的氨基双膦酸盐,如伊班膦酸盐和唑来膦酸盐的相对潜力。

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