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上皮性卵巢癌的挽救性化疗

Salvage chemotherapy for epithelial ovarian carcinoma.

作者信息

Christian M C, Trimble E L

机构信息

Cancer Therapy Evaluation Program, National Cancer Institute, Bethesda, Maryland 20892.

出版信息

Gynecol Oncol. 1994 Dec;55(3 Pt 2):S143-50. doi: 10.1006/gyno.1994.1354.

Abstract

Advanced epithelial ovarian cancer is a highly chemosensitive solid tumor with response rates of 70-80% to first-line chemotherapy, including a high proportion of complete responses. The majority of patients, however, eventually relapse and ultimately die of chemoresistant disease. Response rates to salvage agents are modest, and duration of response is relatively short. Important new agents have been identified in the salvage setting, however, and all patients with ovarian cancer recurring or persisting after front-line therapy should be encouraged to enroll in clinical trials. Phase II trials should include multiple adequately sized cohorts, for patients with platinum-sensitive disease and those with platinum-refractory disease. In addition, patients should be stratified by treatment-free interval. An effort should be made to report standard response endpoints, such as median duration of response, median time to progression, and median survival. Retreatment with a platinum-containing compound is appropriate in patients with platinum-sensitive disease. Trials of high-dose chemotherapy with hematologic support may be most appropriate for patients with minimal disease following first-line therapy, but are unlikely to benefit patients with platinum-resistant or bulky disease. Paclitaxel should figure prominently in consideration of salvage therapy for patients with platinum-resistant disease. Responses to other single agents or combination chemotherapy have been modest and generally of short duration. Efforts at hormonal therapy have been disappointing. Promising new agents include topoisomerase I inhibitors, such as topotecan, 9-aminocamptothecin, irinotecan (CPT-11), and pyrazoloacridine. Therapies focusing on novel molecular targets include antiangiogenesis agents, antimetastatic agents, and signal transduction inhibitors. Immunotherapy, including radioimmunotherapy, immunotoxins, and direct antitumor effects of monoclonal antibodies, may be useful. Greater understanding of the molecular pathology of ovarian cancer may help us develop more rational and effective treatment.

摘要

晚期上皮性卵巢癌是一种对化疗高度敏感的实体瘤,一线化疗的缓解率为70%-80%,其中完全缓解的比例很高。然而,大多数患者最终会复发,并最终死于化疗耐药性疾病。挽救性治疗药物的缓解率一般,且缓解持续时间相对较短。不过,在挽救性治疗方面已发现了重要的新型药物,所有一线治疗后复发或病情持续的卵巢癌患者都应被鼓励参加临床试验。II期试验应包括多个规模足够大的队列,分别针对铂敏感疾病患者和铂耐药疾病患者。此外,患者应按无治疗间期进行分层。应努力报告标准的缓解终点,如缓解持续时间中位数、疾病进展时间中位数和总生存中位数。铂敏感疾病患者再次使用含铂化合物进行治疗是合适的。对于一线治疗后疾病轻微的患者,进行有血液学支持的大剂量化疗试验可能最为合适,但对铂耐药或肿瘤体积较大的患者不太可能有益。对于铂耐药疾病患者,在考虑挽救性治疗时应重点考虑紫杉醇。对其他单药或联合化疗的反应一般,且持续时间通常较短。激素治疗的效果令人失望。有前景的新型药物包括拓扑异构酶I抑制剂,如拓扑替康、9-氨基喜树碱、伊立替康(CPT-11)和吡唑并吖啶。针对新型分子靶点的治疗方法包括抗血管生成药物、抗转移药物和信号转导抑制剂。免疫治疗,包括放射免疫治疗、免疫毒素和单克隆抗体的直接抗肿瘤作用,可能会有帮助。对卵巢癌分子病理学的更深入了解可能有助于我们开发更合理、有效的治疗方法。

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