McGuire W P, Blessing J A, Bookman M A, Lentz S S, Dunton C J
Department of Medicine, University of Mississippi School of Medicine, Jackson, MS, USA.
J Clin Oncol. 2000 Mar;18(5):1062-7. doi: 10.1200/JCO.2000.18.5.1062.
Topotecan is known to be active in recurrent ovarian cancer, but most prior studies have focused on platinum-resistant or refractory populations. This study was undertaken to define the response rate and progression-free interval in platinum-sensitive patients.
Patients with recurrent ovarian cancer after one or two prior chemotherapy regimens and in whom the interval between prior platinum therapy and the initiation of protocol therapy was greater than 6 months were treated with topotecan 1.5 mg/m(2) intravenously over 30 minutes daily for 5 days, with this cycle repeated every 21 days.
Forty-eight patients were entered onto the study; 47 were assessable for toxicity and 46 for response. The response rate was 33% (two complete responses and 13 partial responses), with a median response duration of 11.2 months. Hematologic toxicity predominated but was manageable in most patients with frequent incorporation of cytokines and RBC and platelet transfusions. Fatigue was reported in 15 patients and resulted in the discontinuation of therapy in five responding patients.
Topotecan is an active drug in platinum-sensitive ovarian cancer, with significant but manageable hematologic toxicity. Fatigue is also a common problem that may be dose-limiting in some patients.
已知拓扑替康对复发性卵巢癌有效,但既往大多数研究集中于铂耐药或难治人群。本研究旨在确定铂敏感患者的缓解率和无进展生存期。
接受过一或两个既往化疗方案且既往铂类治疗与方案治疗开始间隔大于6个月的复发性卵巢癌患者,接受拓扑替康1.5mg/m²静脉滴注,30分钟内滴完,每日1次,共5天,每21天重复此周期。
48例患者进入研究;47例可评估毒性,46例可评估疗效。缓解率为33%(2例完全缓解和13例部分缓解),中位缓解持续时间为11.2个月。血液学毒性为主,但多数患者通过频繁应用细胞因子及红细胞和血小板输注可控制。15例患者报告有疲劳,5例缓解患者因疲劳导致治疗中断。
拓扑替康对铂敏感的卵巢癌是一种有效药物,有显著但可控制的血液学毒性。疲劳也是一个常见问题,在某些患者中可能是剂量限制性的。
