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首页> 外文期刊>Stroke: A Journal of Cerebral Circulation >AMPA antagonist ZK200775 in patients with acute ischemic stroke: possible glial cell toxicity detected by monitoring of S-100B serum levels.
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AMPA antagonist ZK200775 in patients with acute ischemic stroke: possible glial cell toxicity detected by monitoring of S-100B serum levels.

机译:AMPA拮抗剂ZK200775在急性缺血性中风患者中:通过监测S-100B血清水平检测出可能的神经胶质细胞毒性。

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BACKGROUND AND PURPOSE: S-100B and neuron-specific enolase (NSE) serum concentrations can be used as peripheral markers of glial cell and neuronal damage, respectively. We investigated these markers in a clinical trial with the alpha-amino-3-hydroxy-5-methyl-4-isoxazole propionate (AMPA) antagonist ZK200775 in acute ischemic stroke patients. METHODS: In a multicenter, double-blind, randomized, placebo-controlled phase 2 trial, 61 ischemic stroke patients were treated with either placebo or active drug in a dose-finding design. Twenty-five patients received placebo, 12 patients received a total dose of 262.5 mg in 48 hours (dose group 1), and 13 patients received a total dose of 525 mg in 48 hours (dose group 2). Eleven patients received a total dose of 105 mg over a period of 6 hours (dose group 3; reduction of total dose and infusion time because of adverse events in group 2). Serum concentrations of S-100B and NSE were analyzed with the use of a monoclonal sandwich immunoluminometric assay. Neurological outcome was assessed with the National Institutes of Health Stroke Scale (NIHSS). RESULTS: In group 2 there was a significant transient worsening in the mean NIHSS score 48 hours after the start of treatment. The mean increase was 11 points. This was due to reduction of consciousness (stupor and coma) in 8 of 13 patients. Neurological deterioration in group 2 was associated with a higher increase of S-100B concentrations, but not of NSE concentrations, than in the placebo group. The trial was stopped prematurely for safety reasons. CONCLUSIONS: The AMPA antagonist ZK200775 transiently worsened the neurological condition in patients with acute ischemic stroke. Our results suggest that in addition to neuronal dysfunction, glial cell toxicity may have occurred. It may be useful to introduce monitoring of serum markers of brain damage in phase 2 trials with glutamate receptor antagonists.
机译:背景与目的:S-100B和神经元特异性烯醇化酶(NSE)血清浓度分别可用作神经胶质细胞和神经元损伤的外周标志物。我们在急性缺血性中风患者中使用丙酸α-氨基-3-羟基-5-羟基-5-甲基-4-异恶唑(AMPA)拮抗剂ZK200775的临床试验研究了这些标志物。方法:在一项多中心,双盲,随机,安慰剂对照的2期临床试验中,以剂量查找设计方式对61例缺血性中风患者进行了安慰剂或活性药物治疗。 25名患者接受了安慰剂,12名患者在48小时内接受了262.5 mg的总剂量(剂量组1),13名患者在48小时内接受了525 mg的总剂量(剂量组2)。 11名患者在6小时内接受了105 mg的总剂量(剂量组3;由于组2中的不良事件,减少了总剂量和输注时间)。使用单克隆三明治免疫荧光测定法分析血清S-100B和NSE的浓度。神经学结果用美国国立卫生研究院卒中量表(NIHSS)进行评估。结果:在第2组中,开始治疗后48小时NIHSS平均评分出现明显的暂时性恶化。平均增加11点。这是由于13例患者中有8例意识(木僵和昏迷)减少。与安慰剂组相比,第2组的神经功能恶化与S-100B浓度升高有关,而与NSE浓度升高无关。出于安全原因,该试验被提前终止。结论:AMPA拮抗剂ZK200775暂时使急性缺血性中风患者的神经系统状况恶化。我们的结果表明,除了神经元功能障碍外,神经胶质细胞毒性可能已经发生。在使用谷氨酸受体拮抗剂的2期试验中引入对脑损伤血清标志物的监测可能是有用的。

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