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大剂量全身应用阿糖胞苷的中枢神经系统毒性

Central nervous system toxicity of high-dose systemic cytosine arabinoside.

作者信息

Lazarus H M, Herzig R H, Herzig G P, Phillips G L, Roessmann U, Fishman D J

出版信息

Cancer. 1981 Dec 15;48(12):2577-82. doi: 10.1002/1097-0142(19811215)48:12<2577::aid-cncr2820481207>3.0.co;2-z.

Abstract

Forty-nine adult patients with acute leukemia in relapse, refractory to conventional therapy, were studied. Increasing quantities of i.v. bolus high-dose cytosine arabinoside (cytarabine) were administered using the following schedules: 3 g/m2 every 12 hrs for 4-16 consecutive doses, or 4.5 g/m2 every 12 hrs for 12 consecutive doses. Patients ages ranged 16-76 year (median: 38). Thirty-seven patients had previously received either induction or maintainance therapy with conventional doses of cytarabine. Cerebral or cerebellar dysfunction attributable to cytarabine was observed in eight patients and appeared 6-8 days (mean: 6.6) after the first dose and lasted 3-7 days (mean: 4.7). None of 12 patients receiving up to 24 g/m2 total dose of 48 g/m2 developed reversible neurologic dysfunction. Four of six patients receiving 54 g/m2 developed CNS toxicity (irreversible in two cases), a significantly greater incidence compared to toxicity in patients receiving less than or equal to 48 g/m2 total dose (P less than 0.01). CNS toxicity was dose-related since patients treated for 12 consecutive doses of 4.5 g/m2 had significantly greater CNS toxicity than 12 consecutive doses at 3 g/m2 (P less than 0.04). Systemic cytarabine doses less than 54 g/m2 can be administered with minimal CNS side-effects.

摘要

对49例急性白血病复发且对传统治疗无效的成年患者进行了研究。采用以下方案静脉推注递增剂量的大剂量阿糖胞苷:每12小时3g/m²,连续4 - 16剂;或每12小时4.5g/m²,连续12剂。患者年龄在16 - 76岁之间(中位数:38岁)。37例患者此前曾接受过传统剂量阿糖胞苷的诱导或维持治疗。8例患者出现了与阿糖胞苷相关的大脑或小脑功能障碍,在首剂后6 - 8天(平均:6.6天)出现,持续3 - 7天(平均:4.7天)。接受总剂量达24g/m²(共48g/m²)的12例患者中,无一例出现可逆性神经功能障碍。接受54g/m²的6例患者中有4例出现中枢神经系统毒性(2例不可逆),与接受总剂量小于或等于48g/m²的患者相比,发生率显著更高(P<0.01)。中枢神经系统毒性与剂量相关,因为连续12剂4.5g/m²治疗的患者中枢神经系统毒性明显高于连续12剂3g/m²治疗的患者(P<0.04)。全身阿糖胞苷剂量小于54g/m²时,可产生最小的中枢神经系统副作用。

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