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Sequential Dose-Dense Doxorubicin and Ifosfamide in AdvancedSoft-Tissue Sarcoma Patients in an Out-Patient-Basis Schedule

机译:序贯剂量密集的阿霉素和异环磷酰胺在门诊患者基础上的高级软组织肉瘤患者中的应用

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Aims. This phase II study explored activity/safety of front-line dose-dense chemotherapy in high-grade STS (soft tissue sarcoma) patients and tested ezrin as prognostic factor. Patients and Methods. The protocol consisted of three cycles of doxorubicin (DOXO) 30 mg/m2 on days 1-3 every 2 weeks, followed by three cycles of ifosfamide (IFO) 2.5 g/m2 two hours a day on days 1-5 every 3 weeks, with GCSF support. Ezrin was assessed immunohistochemically. Results. Twenty patients, 13 metastatic and 7 locally advanced, were enrolled. Median age was 39 years (25-60). Median dose intensities were 42 mg/m2/week and 3.6 g/m2/week for DOXO and IFO, respectively. Grade 3/4 toxicities occurred in 18 patients. Response rate was 15% (3 of 20) by RECIST. Patients younger than 45 years with locally advanced disease and synovial histology presented longer survival. A trend towards longer survival was observed among ezrin-positive patients. Conclusions. This dose-dense schedule should not be routinely used due to its high frequency of toxic events; however, a sequential strategy with DOXO and IFO may benefit selected patients and should be further explored with lower doses. The role of ezrin as a prognostic marker should be confirmed in a larger group of patients.
机译:目的这项II期研究探讨了在高级STS(软组织肉瘤)患者中进行一线剂量密集化疗的活性/安全性,并测试了ezrin作为预后因素。患者和方法。该方案包括每2周1-3天进行3个周期的阿霉素(DOXO)30 mg / m2的三个周期,然后每3周1-5天在每天2小时进行三个周期的异环磷酰胺(IFO)2.5 g / m2的三个周期,具有GCSF支持。用免疫组织化学法评估Ezrin。结果。入选20例患者,其中13例转移,7例局部晚期。中位年龄为39岁(25-60)。 DOXO和IFO的中位剂量强度分别为42 mg / m2 /周和3.6 g / m2 /周。 18名患者发生3/4级毒性。 RECIST的回复率为15%(20之3)。年龄小于45岁且患有局部晚期疾病和滑膜组织学的患者生存期更长。在ezrin阳性患者中观察到了更长的生存趋势。结论由于这种中毒事件的发生频率很高,因此不应常规使用这种剂量密集的时间表。但是,采用DOXO和IFO的序贯策略可能会使选定的患者受益,应该以更低的剂量进一步探索。 ezrin作为预后标志物的作用应在更多患者中得到证实。

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