Continuous infusion of interleukin-2 and cyclophosphamide as treatment of advanced cancers: a National Biotherapy Study Group Trial.

Molecular biotherapy Pub Date : 1991-06-01

R K Oldham, J Stark, N M Barth, B Hoogstraten, C H Brown, T O'Connor, S Dupere, R Birch

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Abstract

We have evaluated the effect of Interleukin-2 [IL-2] after Cyclophosphamide (C) chemotherapy in 41 patients with metastatic cancer. IL-2 was given as a continuous infusion priming cycle 36 hours after C at 1 gm/m2 intravenously. In 39 evaluable patients, there were no complete remissions [CR], 2 partial remissions [PR], and 1 had a minor response [MR]. Stable disease for 30 days was seen in 16 patients whereas 20 progressed. The durations of partial and minor responses were brief, ranging from 1-6 months. Grade 3-4 neutropenia was seen in 41%. This was more severe than seen with IL-2 alone or IL-2 combined with lower doses of C. The marrow suppression was due to the chemotherapy. This combination of IL-2 and C appears to be reasonably well tolerated by patients, but toxicity is greater and the response rate is no better than results achieved by IL-2 alone. Responses of 26 patients with renal cancer appear to be inferior to our historical data using IL-2/LAK cells without C. Immune monitoring demonstrated changes expected with C chemotherapy (i.e., a non-selective decline in immune function). C induced no further differences in IL-2 induced changes in immune function.

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持续输注白介素-2和环磷酰胺治疗晚期癌症:一项国家生物治疗研究组试验。

我们评估了41例转移性癌症患者在环磷酰胺(C)化疗后白细胞介素-2 (IL-2)的作用。IL-2以1 gm/m2静脉滴注，在C后36小时连续灌注启动周期。在39例可评估的患者中，没有完全缓解[CR]， 2例部分缓解[PR]， 1例轻微缓解[MR]。16例病情稳定30天，20例病情进展。部分和轻微反应的持续时间很短，从1-6个月不等。41%为3-4级中性粒细胞减少。这比单独使用IL-2或IL-2与低剂量c联合使用更为严重。骨髓抑制是由于化疗。这种IL-2和C的联合治疗似乎对患者的耐受性相当好，但毒性更大，而且反应率并不比单独使用IL-2的结果好。26例肾癌患者的反应似乎不如我们使用IL-2/LAK细胞而不使用C的历史数据。免疫监测显示C化疗预期的变化(即免疫功能的非选择性下降)。C对IL-2诱导的免疫功能变化无进一步影响。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Molecular biotherapy

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