Lees K R, Barer D, Ford G A, Hacke W, Kostulas V, Sharma A K, Odergren T
University Department of Medicine and Therapeutics, Western Infirmary, Glasgow, UK.
Stroke. 2003 Feb;34(2):482-7. doi: 10.1161/01.str.0000053032.14223.81.
NXY-059 is a nitrone-based free radical-trapping agent in development for acute stroke. In patients with acute stroke, NXY-059 is well tolerated at concentrations known to be associated with neuroprotection in animal models of transient cerebral ischemia; however, higher target concentrations appear necessary on the basis of animal models of permanent ischemia.
This was a randomized, double-blind, placebo-controlled, parallel-group, dose-escalation, multicenter study that evaluated safety, tolerability, and plasma concentrations of 2 NXY-059 dosing regimens within 24 hours of acute stroke. NXY-059 was administered as either 915 mg over 1 hour followed by 420 mg/h for 71 hours or 1820 mg for 1 hour followed by 844 mg/h for 71 hours; plasma concentrations were monitored. Neurological and functional outcomes were recorded for up to 30 days.
One hundred thirty-five patients were recruited, of whom 134 received study treatment and completed assessments (844 mg/h, n=39; 420 mg/h, n=48; placebo, n=47). Mean age was 69 years (range, 34 to 92 years), and baseline National Institutes of Health Stroke Scale score was 8.5 (SD, 6.6). Serious adverse events occurred in 3, 17, and 13 patients, respectively, with deaths in 0, 4, and 3 patients and treatment discontinuations because of adverse events in 0, 1, and 3 patients. Good outcome, defined by modified Rankin Scale score of 0 or 1, was seen in 53%, 29% and 40%, respectively. No safety concern was identified in analysis of body temperature, blood pressure, or other laboratory parameters. The unbound plasma concentration at steady state was 260+/-79 micromol/L, exceeding the target of 200 micromol/L in the high-dose group.
NXY-059 was well tolerated in patients with an acute stroke at and above concentrations shown to be neuroprotective in an animal model when initiated 4 hours after onset of permanent focal ischemia.
NXY - 059是一种正在研发用于急性卒中的基于硝酮的自由基捕获剂。在急性卒中患者中,NXY - 059在已知与短暂性脑缺血动物模型中的神经保护作用相关的浓度下耐受性良好;然而,基于永久性缺血动物模型,似乎需要更高的目标浓度。
这是一项随机、双盲、安慰剂对照、平行组、剂量递增的多中心研究,评估急性卒中24小时内两种NXY - 059给药方案的安全性、耐受性和血浆浓度。NXY - 059的给药方式为:1小时内给予915 mg,随后71小时以420 mg/h的速度给药;或1小时内给予1820 mg,随后71小时以844 mg/h的速度给药;监测血浆浓度。记录长达30天的神经和功能结局。
招募了135名患者,其中134名接受了研究治疗并完成了评估(844 mg/h组,n = 39;420 mg/h组,n = 48;安慰剂组,n = 47)。平均年龄为69岁(范围34至92岁),基线美国国立卫生研究院卒中量表评分为8.5(标准差6.6)。分别有3、17和13名患者发生严重不良事件,分别有0、4和3名患者死亡,分别有0、1和3名患者因不良事件而停药。改良Rankin量表评分为0或1所定义的良好结局分别在53%、29%和40%的患者中出现。在体温、血压或其他实验室参数分析中未发现安全问题。高剂量组稳态下的游离血浆浓度为260±79 μmol/L,超过了200 μmol/L的目标值。
在永久性局灶性缺血发作4小时后开始使用时,NXY - 059在急性卒中患者中,在达到及高于动物模型中显示具有神经保护作用的浓度时耐受性良好。
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