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尝试使用剂量强化的环磷酰胺、依托泊苷和粒细胞集落刺激因子治疗恶性星形细胞瘤。

Attempted dose intensified cyclophosphamide, etoposide, and granulocyte colony-stimulating factor for treatment of malignant astrocytoma.

作者信息

Newton H B, Newton C L

机构信息

Department of Neurology, Ohio State University, Columbus, USA.

出版信息

J Neurooncol. 1995;24(3):285-92. doi: 10.1007/BF01052845.

DOI:10.1007/BF01052845
PMID:7595759
Abstract

Patients with malignant astrocytoma continue to respond poorly to chemotherapy and have a dismal prognosis. Cyclophosphamide (CTX) and etoposide demonstrate activity against malignant astrocytoma at standard dosages, with bone marrow suppression as the limiting toxicity. In order to allow dose intensification, minimize leukopenia, and improve efficacy granulocyte colony-stimulating factor (G-CSF) was used in combination with CTX and etoposide. The protocol consisted of CTX (2 mg/m2/d, days 1, 2), etoposide (200-300 mg/m2/d, days 1-3), and G-CSF (5-10 micrograms/d subcutaneously, days 4-18), every 4 weeks. Nine evaluable patients (7 glioblastoma multiforme, 2 anaplastic astrocytoma) were treated, ranging in age from 26-67 (mean 41). One of 9 patients responded (11%) with a partial response (13+ months), 3 had stable disease (33%; 8, 5, 2.5 months), and 5 had progressive disease (3, 2.5, 2, 1.5, 1 months). The median time to progression for responders was 6.5 months, while overall it was 2.5 months. Overall median survival was only 7.0 months. Toxicity was frequent and severe, typically delaying treatment cycles. The most common complications were severe myeolosuppression (9), sepsis (8), rash (6), urinary infection (5), and anorexia (5). Treatment delays caused by infections and other complications occurred often, abrogating the intended dose intensification. The received dose intensity (DI) for CTX was 400-425 mg/m2/week (relative DI 0.41), while for etoposide it was 75 mg/m2/week (relative DI 0.42). In summary, as used in this protocol, dose intensive chemotherapy with CTX, etoposide, and G-CSF does not improve efficacy over standard regimens and results in excessive toxicity.

摘要

恶性星形细胞瘤患者对化疗的反应仍然很差,预后不佳。环磷酰胺(CTX)和依托泊苷在标准剂量下对恶性星形细胞瘤有活性,骨髓抑制是其限制毒性。为了实现剂量强化、减少白细胞减少并提高疗效,将粒细胞集落刺激因子(G-CSF)与CTX和依托泊苷联合使用。方案包括CTX(2mg/m²/天,第1、2天)、依托泊苷(200 - 300mg/m²/天,第1 - 3天)和G-CSF(5 - 10微克/天皮下注射,第4 - 18天),每4周重复一次。治疗了9例可评估患者(7例多形性胶质母细胞瘤,2例间变性星形细胞瘤),年龄在26 - 67岁之间(平均41岁)。9例患者中有1例有反应(11%),为部分缓解(13 + 个月),3例病情稳定(33%;8、5、2.5个月),5例病情进展(3、2.5、2、1.5、1个月)。有反应者的中位进展时间为6.5个月,总体为2.5个月。总体中位生存期仅为7.0个月。毒性频繁且严重,通常会延迟治疗周期。最常见的并发症是严重骨髓抑制(9例)、败血症(8例)、皮疹(6例)、泌尿系统感染(5例)和厌食(5例)。由感染和其他并发症导致的治疗延迟经常发生,破坏了预期的剂量强化。CTX的实际剂量强度(DI)为400 - 425mg/m²/周(相对DI 0.41),依托泊苷为75mg/m²/周(相对DI 0.42)。总之,在本方案中使用时,CTX、依托泊苷和G-CSF的剂量密集化疗与标准方案相比并未提高疗效,且导致过度毒性。

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