isophosphamide (NSC-109724)的I期临床试验。

Cancer chemotherapy reports Pub Date : 1975-07-01
M H Cohen, P J Creaven, F Tejada, H H Hansen, F Muggia, A Mittelman, O S Selawry
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引用次数: 0

摘要

异磷酰胺的初步临床I期试验已进行,剂量水平为200-10,000 mg/m2的体表面积,采用单剂量,每3周一次的时间表。低于2900 mg/m2的异磷酰胺剂量水平未见明显毒性。在高剂量下,恶心和呕吐几乎是普遍的。在剂量为3800-7000 mg/m2的20例患者中,有12例出现血液学毒性,表现为白细胞减少。未见患者血小板减少至100,000血小板/mm3。剂量为3800 ~ 10000 mg/m2的23例患者中有15例出现出血性膀胱炎的膀胱毒性。n -乙酰- l-半胱氨酸(1%溶液,2000 ml/d)膀胱冲洗可完全预防出血性膀胱炎。在14名接受异磷酰胺剂量为5000-7000 mg/m2的患者中,只有两名患者的血尿素氮升高至30 mg/dl,在很大程度上防止了肾毒性。另一个副作用是17例患者中有7例在剂量为5000-10,000 mg/m2时中枢神经系统毒性。对于II期试验,建议剂量为5000mg /m2,同时要注意患者的水合状态,并了解膀胱冲洗对于预防和/或改善膀胱毒性可能是必要的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Phase I clinical trial of isophosphamide (NSC-109724).

An initial clinical phase I trial of isophosphamide has been carried out at dose levels of 200-10,000 mg/m2 of body surface area using a single-dose, every-3-week schedule. Significant toxicity was not seen at isophosphamide dose levels less than 2900 mg/m2. At higher doses, nausea and vomiting was nearly universal. Hematologic toxicity manifested by leukopenia occurred in 12 of 20 patients treated with doses of 3800-7000 mg/m2. Thrombocytopenia to 100,000 platelets/mm3 was not seen in any patient. Urinary bladder toxicity manifested by hemorrhagic cystitis was seen in 15 of 23 patients treated with doses of 3800-10,000 mg/m2. Hemorrhagic cystitis could be completely prevented by bladder irrigation with N-acetyl-L-cysteine (1% solution, 2000 ml/day). With careful attention to hydration, renal toxicity was largely prevented with blood urea nitrogen elevations to 30 mg/dl in only two of 14 patients receiving isophosphamide doses of 5000-7000 mg/m2. Another side effect was central nervous system toxicity in seven of 17 patients at doses of 5000-10,000 mg/m2. For phase II trials a dose of 5000 mg/m2 is recommended, with careful attention to the state of hydration in the patient and with the knowledge that bladder irrigation may be necessary for the prevention and/or amelioration of bladder toxicity.

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