Hoskins P, Eisenhauer E, Vergote I, Dubuc-Lissoir J, Fisher B, Grimshaw R, Oza A, Plante M, Stuart G, Vermorken J
British Columbia Cancer Agency, Vancouver Clinic, Vancouver, British Columbia, Canada.
J Clin Oncol. 2000 Dec 15;18(24):4038-44. doi: 10.1200/JCO.2000.18.24.4038.
Despite the improved results in advanced ovarian cancer achieved with the addition of paclitaxel to frontline therapy, there remains room for improvement. One approach is to add new agents such as topotecan. Because myelosuppression limits the delivery of topotecan with paclitaxel/cisplatin in a three-drug combination, we explored giving sequential couplets of cisplatin/topotecan followed by paclitaxel/cisplatin.
Forty-four patients with residual epithelial ovarian carcinoma after primary surgery were studied. Cisplatin 50 mg/m(2) on day 1 and topotecan 0.75 mg/m(2) on days 1 through 5 were administered at 21-day intervals for four cycles, followed by interval debulking surgery (if optimal debulking was not achieved with primary surgery), and then paclitaxel 135 mg/m(2) over 24 hours on day 1 and cisplatin 75 mg/m(2) on day 2 at 21-day intervals for four cycles.
Such sequential couplets are feasible. Myelotoxicity was the major toxic effect, but it was of short duration. The granulocyte nadir with topotecan/cisplatin occurred late (median, day 18), so retreatment on day 21 was not always possible. There was no unexpected nonhematologic toxicity. The regimen was active in this group of patients who had undergone largely suboptimal debulking surgery. In 34 patients with clinically measurable disease, the overall response rate was 78%, and 30 (77%) of the 39 patients with elevated CA 125 levels at baseline had normalization of CA 125 levels by the end of therapy.
Sequential couplets of cisplatin/topotecan followed by paclitaxel/cisplatin are feasible. The efficacy data in this suboptimal group of patients has encouraged us to proceed with a randomized study based on this approach.
尽管在一线治疗中添加紫杉醇后晚期卵巢癌的治疗效果有所改善,但仍有改进空间。一种方法是添加新的药物,如拓扑替康。由于骨髓抑制限制了拓扑替康与紫杉醇/顺铂三联用药的给药剂量,我们探索了顺铂/拓扑替康序贯双联给药,随后给予紫杉醇/顺铂的方案。
对44例初次手术后有残留上皮性卵巢癌的患者进行了研究。第1天给予顺铂50mg/m²,第1至5天给予拓扑替康0.75mg/m²,每21天为一个周期,共进行4个周期,之后进行间隔减瘤手术(如果初次手术未达到最佳减瘤效果),然后第1天24小时内给予紫杉醇135mg/m²,第2天给予顺铂75mg/m²,每21天为一个周期,共进行4个周期。
这种序贯双联给药方案是可行的。骨髓毒性是主要的毒性反应,但持续时间较短。拓扑替康/顺铂治疗后的粒细胞最低点出现较晚(中位时间为第18天),因此并非总是能够在第21天进行再次治疗。未出现意外的非血液学毒性。该方案对这组大部分减瘤效果欠佳的患者有效。在34例有临床可测量病灶的患者中,总缓解率为78%,基线时CA 125水平升高的39例患者中,有30例(77%)在治疗结束时CA 125水平恢复正常。
顺铂/拓扑替康序贯双联给药,随后给予紫杉醇/顺铂是可行的。该次优组患者的疗效数据鼓励我们基于此方法开展一项随机研究。
