麻环素治疗转移性肾细胞癌的生物学及治疗效果。

Molecular biotherapy Pub Date : 1992-06-01
A Schomburg, T Menzel, M Hadam, S Duensing, A Körfer, H Kirchner, H Poliwoda, J Atzpodien
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引用次数: 0

摘要

众所周知,恶氮磷[如环磷酰胺和4-氢过氧环磷酰胺(mafosfamide)]是有效的免疫抑制剂。在适当的条件下,它们也可以增强免疫反应。免疫调节是化疗耐药肿瘤治疗的重大突破。因此,我们评估了低至中剂量(100- 1000mg /m2)给药16例患者的临床和实验室后遗症。治疗4周后,1名患者完全缓解,8名患者病情稳定,7名患者无反应。临床和实验室毒性轻微且完全可逆,所有患者对治疗耐受良好。循环外周血单个核细胞的表型细胞表面抗原分析显示CD4/CD8比值的不一致改变,CD8+细胞的初始消耗和随后反弹,CD20+细胞的增加,以及以CD16和CD56阳性为特征的自然杀伤样细胞的mafosfamide剂量依赖性调节。细胞介导的对K562靶细胞的细胞毒性在治疗后1天达到峰值,在接受300 mg/m2的mafosfamide的患者中最为明显,而对Daudi靶细胞的细胞毒性基本不变,这与自然杀伤活性的增加一致,而没有增加淋巴因子激活的杀伤。我们的结论是,低至中剂量给药可以具有良好的安全性和耐受性;免疫表型分析和细胞毒性试验显示,在接受低剂量麻黄酰胺治疗的患者中发生了最明显的改变。这些观察结果支持使用甲基环磷酰胺来增强抗肿瘤免疫反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Biologic and therapeutic efficacy of mafosfamide in patients with metastatic renal cell carcinoma.

It is well known that oxazaphosphorines [e.g., cyclophosphamide and 4-hydroperoxycyclophosphamide (mafosfamide)] are potent immunosuppressive agents. Under the proper conditions, they can potentiate immune responses as well. Immunomodulation represents a major breakthrough in the management of chemotherapy-resistant tumors. Thus, we evaluated the clinical and laboratory sequelae of low to intermediate doses (100-1000 mg/m2) of mafosfamide administered to 16 patients. Four weeks after therapy, one patient had a complete remission, eight patients presented with stable disease, and seven patients did not respond. Clinical and laboratory toxicity was mild and totally reversible, and therapy was well tolerated in all patients. Analyses of phenotypic cell surface antigens on circulating peripheral blood mononuclear cells showed inconsistent alterations of the CD4/CD8 ratio, initial depletion with later rebound of CD8+ cells, increase of CD20+ cells, and a mafosfamide dose-dependent regulation of natural killer-like cells as characterized by CD16 and CD56 positivity. Cell-mediated cytotoxicity against K562 target cells peaked 1 day after therapy and was most pronounced in patients who had received 300 mg/m2 mafosfamide, whereas cytotoxicity against Daudi targets was essentially unchanged, consistent with an increase in natural killing activity without augmentation of lymphokine activated killing. We conclude that mafosfamide administration at low to intermediate doses can be performed with good safety and tolerance; immunophenotypic analyses and cytotoxicity assays showed most pronounced alterations in patients receiving low doses of mafosfamide. These observations support the use of mafosfamide in the attempt to augment antitumor immune responses.

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