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强的松对六甲蜜胺治疗多发性骨髓瘤有效性的作用。

Contribution of prednisone to the effectiveness of hexamethylmelamine in multiple myeloma.

作者信息

Oken M M, Lenhard R E, Tsiatis A A, Glick J H, Silverstein M N

出版信息

Cancer Treat Rep. 1987 Sep;71(9):807-11.

PMID:3113729
Abstract

The Eastern Cooperative Oncology Group evaluated hexamethylmelamine in 89 patients with advanced refractory or relapsing multiple myeloma. Hexamethylmelamine was initially used as a single agent administered orally at 200 mg/m2/day for the first 3 weeks of each 4-week cycle. When this regimen proved to be ineffective, it was modified first by increasing the dose of hexamethylmelamine to 280 mg/m2/day and subsequently by adding prednisone at 75 mg for the first 7 days of each 28-day cycle. None of the 39 patients receiving hexamethylmelamine without prednisone had an objective response, while two patients had minimal objective improvement (25%-50% decrease in M protein with symptomatic improvement). Only 14% of these patients had objective or symptomatic response or both. In contrast, patients treated with hexamethylmelamine plus prednisone had a 22% objective response rate, with another 14% showing lesser degrees of objective improvement. Fifty-one percent of the patients treated with this regimen had either objective or symptomatic improvement or both. Severe (grade 3) toxicity was seen in nearly two-thirds of the patients on the higher-dose hexamethylmelamine regimens compared with 37% of the patients receiving low-dose hexamethylmelamine; however, in most instances this represented rapidly reversible cytopenias. Because all but one of the patients responding to hexamethylmelamine plus prednisone had experienced previous treatment failure on regimens containing prednisone in similar dose and schedules, it is unlikely that the responses are due to prednisone alone. Instead, this study suggests that the activity of hexamethylmelamine in multiple myeloma is dependent on the concomitant administration of prednisone and that the combination regimen appears to be synergistic.

摘要

东部肿瘤协作组对89例晚期难治性或复发性多发性骨髓瘤患者使用六甲蜜胺进行了评估。六甲蜜胺最初作为单一药物,在每4周周期的前3周口服,剂量为200mg/m²/天。当该方案被证明无效时,首先将六甲蜜胺剂量增加至280mg/m²/天进行调整,随后在每28天周期的前7天加用75mg泼尼松。39例接受六甲蜜胺但未使用泼尼松的患者均无客观缓解,而2例患者有轻微客观改善(M蛋白降低25%-50%且症状改善)。这些患者中只有14%有客观或症状缓解或两者皆有。相比之下,接受六甲蜜胺加泼尼松治疗的患者客观缓解率为22%,另有14%有程度较轻的客观改善。接受该方案治疗的患者中有51%有客观或症状改善或两者皆有。与接受低剂量六甲蜜胺治疗的患者的37%相比,近三分之二接受高剂量六甲蜜胺方案治疗的患者出现了严重(3级)毒性;然而,在大多数情况下,这表现为迅速可逆的血细胞减少。由于除1例患者外,所有对六甲蜜胺加泼尼松有反应的患者之前在含类似剂量和给药方案泼尼松的方案治疗中均失败,因此这些反应不太可能仅归因于泼尼松。相反,这项研究表明六甲蜜胺在多发性骨髓瘤中的活性依赖于泼尼松的联合使用,且联合方案似乎具有协同作用。

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