Sarcoma Center, Departments of Medical Oncology, Surgical Oncology and Pathology, West German Cancer Center, University Hospital Essen, University Duisburg-Essen, D-45122 Essen, Germany.
Int J Oncol. 2013 Jul;43(1):23-8. doi: 10.3892/ijo.2013.1928. Epub 2013 May 2.
Trabectedin has mostly been studied in metastatic leiomyosarcoma and liposarcomas. Only limited data are available in other sarcoma subtypes, heavily pretreated and elderly patients. We retrospectively analyzed 101 consecutive sarcoma patients treated with trabectedin at our center. We recorded progression-free survival (PFS), clinical benefit rate (CBR, defined as complete or partial response or stable disease for at least 6 weeks) and toxicity. Covariates were sarcoma subtype, age and pretreatment. On average, trabectedin was administered for 2nd relapse/progression (range 1st to 12th line). A median of 2 cycles and a dose of 1.5 mg/m2 (range 1-21 cycles; 1.3-1.5 mg/m2) was administered. The median PFS under treatment with trabectedin was 2.1 months in the overall population. Different clinical outcomes were observed with respect to sarcoma subtypes: in patients with L-sarcoma [defined as leiosarcoma and liposarcoma (n=25)] the CBR was 55%. Notably, long lasting remissions were even observed in 7th-line treatment. In contrast, the majority of patients with non-L-sarcomas quickly progressed (median PFS 1.6 months). Nevertheless, a CBR of 34% was achieved, including long-lasting disease stabilization in subtypes such as rhabdomyosarcoma. Patients treated with trabectedin at 1st or 2nd line (n=16) achieved an improved PFS (median 5.7 months, range) and a CBR of 59%. No differences in terms of toxicity or efficacy were observed between patients older than 65 years (n=23) and younger patients (n=78). In this non-trial setting, port-associated complications were more frequent (14%) with trabectedin compared to other continuous infusion protocols administered at our outpatient therapy center. The majority of patients with relapsing L-sarcomas and a substantial fraction of patients with non-L-sarcomas derive a clinically meaningful benefit from trabectedin. Outpatient treatment is well tolerated also in elderly and heavily pretreated patients. Port-associated complications were observed at an unusually high rate. This suggests a drug-specific local toxicity that merits further investigation.
曲贝替定主要在转移性平滑肌肉瘤和脂肪肉瘤中进行了研究。在其他肉瘤亚型、经过大量预处理和老年患者中,仅有有限的数据可用。我们回顾性分析了在我们中心接受曲贝替定治疗的 101 例连续肉瘤患者。我们记录了无进展生存期(PFS)、临床获益率(CBR,定义为完全或部分缓解或稳定疾病至少 6 周)和毒性。协变量为肉瘤亚型、年龄和预处理。平均而言,曲贝替定用于第 2 次复发/进展(范围第 1 至 12 线)。中位数为 2 个周期,剂量为 1.5mg/m2(范围 1-21 个周期;1.3-1.5mg/m2)。总体人群中接受曲贝替定治疗的中位 PFS 为 2.1 个月。根据肉瘤亚型观察到不同的临床结果:在 L-肉瘤患者中[定义为 leiiosarcoma 和 liposarcoma(n=25)],CBR 为 55%。值得注意的是,甚至在第 7 线治疗中也观察到了持久的缓解。相比之下,大多数非 L-肉瘤患者很快进展(中位 PFS 1.6 个月)。然而,仍达到了 34%的 CBR,包括横纹肌肉瘤等亚型的持久疾病稳定。在第 1 或 2 线接受曲贝替定治疗的患者(n=16),PFS 得到改善(中位 5.7 个月,范围),CBR 为 59%。在 65 岁以上的患者(n=23)和年轻患者(n=78)之间,在毒性或疗效方面没有差异。在这种非试验环境中,与我们门诊治疗中心给予的其他连续输注方案相比,曲贝替定更常发生与端口相关的并发症(14%)。大多数复发性 L-肉瘤患者和相当一部分非 L-肉瘤患者从曲贝替定中获得了有临床意义的益处。门诊治疗在老年和大量预处理患者中也耐受良好。观察到与端口相关的并发症发生率异常高。这表明存在药物特异性局部毒性,值得进一步研究。
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