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晚期乳腺癌的全身治疗

Systemic therapy of advanced breast cancer.

作者信息

Mouridsen H T

机构信息

Department of Oncology, Rigshospitalet, Copenhagen, Denmark.

出版信息

Drugs. 1992;44 Suppl 4:17-28; discussion 66-9. doi: 10.2165/00003495-199200444-00003.

Abstract

Many cytotoxic agents have demonstrated activity in advanced breast cancer, the more active agents being cyclophosphamide and the anthracyclines doxorubicin and epirubicin. Combinations of drugs are generally superior to single agents in terms of response rate, duration of response and survival. The treatment of advanced breast cancer can be continued either until treatment failure, or for a limited time from either initiation of therapy or from the observation of complete response. Although these are issues of significant concern, data from randomised trials are limited, and so the question of optimal treatment duration remains open. Randomised trials comparing regimens that differ by a dose intensity factor of less than 2 have failed to demonstrate significant differences in efficacy between the dose levels. With higher doses, as applied in combination with colony-stimulating factors and bone marrow transplantation, response rates seem to increase, but whether this translates into improved survival has not yet been answered by the results of randomised trials. Approximately 30% of patients respond to endocrine therapy. From the results of randomised trials, which have compared the efficacies and toxicities of different endocrine modalities including combined endocrine therapy, single-agent tamoxifen is generally considered as the preferred first-line treatment, leaving progestins and aromatase inhibitors as alternatives for second-line endocrine therapy in responders. In the majority of trials, chemotherapy combined with endocrine therapy has given improved response rates compared with chemotherapy alone, but the differences have not generally been translated into prolonged survival with combined modalities. This gives rise to the question of the optimal sequence of chemotherapy and endocrine therapy, a subject needing further evaluation in future trials.

摘要

许多细胞毒性药物已在晚期乳腺癌中显示出活性,其中活性较高的药物有环磷酰胺以及蒽环类药物多柔比星和表柔比星。就缓解率、缓解持续时间和生存率而言,联合用药通常优于单一药物。晚期乳腺癌的治疗可以持续到治疗失败,或者从治疗开始或观察到完全缓解起持续一段有限的时间。尽管这些都是备受关注的问题,但随机试验的数据有限,因此最佳治疗持续时间的问题仍未解决。比较剂量强度因子相差小于2的方案的随机试验未能证明不同剂量水平之间在疗效上有显著差异。对于更高剂量,如与集落刺激因子和骨髓移植联合应用时,缓解率似乎会提高,但随机试验结果尚未回答这是否转化为生存率的提高。约30%的患者对内分泌治疗有反应。从比较包括联合内分泌治疗在内的不同内分泌治疗方式的疗效和毒性的随机试验结果来看,单药他莫昔芬通常被视为首选的一线治疗药物,而孕激素和芳香化酶抑制剂则作为有反应者二线内分泌治疗的备选药物。在大多数试验中,与单纯化疗相比,化疗联合内分泌治疗的缓解率有所提高,但联合治疗方式一般并未转化为更长的生存期。这就引发了化疗和内分泌治疗的最佳顺序问题,这一问题需要在未来的试验中进一步评估。

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