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Ann Neurol. 2000 Nov;48(5):713-22.
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Ischemic lesion volumes in acute stroke by diffusion-weighted magnetic resonance imaging correlate with clinical outcome.急性卒中患者通过扩散加权磁共振成像测得的缺血性病变体积与临床预后相关。
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通过扩散加权磁共振成像测量的胞磷胆碱对缺血性病变的影响。胞磷胆碱010研究人员。

Effect of citicoline on ischemic lesions as measured by diffusion-weighted magnetic resonance imaging. Citicoline 010 Investigators.

作者信息

Warach S, Pettigrew L C, Dashe J F, Pullicino P, Lefkowitz D M, Sabounjian L, Harnett K, Schwiderski U, Gammans R

机构信息

National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD 20892-4129, USA.

出版信息

Ann Neurol. 2000 Nov;48(5):713-22.

PMID:11079534
Abstract

We examined the effect of the neuroprotective and neuroreparative agent citicoline on the growth of cerebral ischemic lesions in a double-blind placebo-controlled study involving patients with acute ischemic stroke using diffusion-weighted magnetic resonance imaging (DWI). Patients with acute ischemic stroke symptom onset 24 hours or less before the start of treatment, National Institutes of Health Stroke Scale (NIHSS) scores of 5 or higher, and lesions of 1 to 120 cc in cerebral gray matter by DWI were enrolled. DWI, T2-weighted magnetic resonance imaging (MRI), perfusion-weighted MRI, and magnetic resonance angiography were obtained at baseline, week 1, and week 12. Citicoline (500 mg/day) was administered orally for 6 weeks, and patients were followed for 12 weeks. The primary assessment was progression of ischemic lesion volume from baseline to 12 weeks as measured by MRI. A total of 100 patients entered the study. The primary MRI analysis included 40 placebo-treated patients and 41 citicoline-treated patients with both baseline and week 12 MRI data and failed to demonstrate a significant difference in lesion volume change from baseline to week 12. From baseline to week 12, ischemic lesion volume [all values mean (SE)] expanded by 180% (107) among placebo-treated patients compared with 34% (19) among citicoline-treated patients. In a secondary analysis, lesion volume decreased from week 1 to week 12 by 6.9 cc (2.8) on placebo versus 17.2 cc (2.6) on citicoline. Baseline variables that were predictors of change in lesion size over 12 weeks were the volume of hypoperfusion (strongest association), baseline NIHSS score, lesion volume on DWI, arterial lesion by magnetic resonance angiography, and categorized elapsed time (< or =12 or >12 hours) from stroke onset to first dose. A marked association between lesion volume reduction and improvement of NIHSS score by seven or more points was observed. Significant correlations between lesion volumes and clinical measures were found, replicating values reported in the literature for smaller case series. We observed a reduction in lesion volume growth from baseline to week 12 with citicoline treatment, with a significantly greater reduction in volume from week 1 to week 12 with citicoline. We found a significant inverse relationship between lesion volume change over 12 weeks as measured by MRI and clinical outcome for ischemic stroke. This relationship supports the role of DWI as a surrogate marker of clinically meaningful lesion progression in stroke clinical trials. The hypothesis that citicoline reduces lesion growth and improves clinical outcome will be tested further.

摘要

在一项双盲、安慰剂对照研究中,我们使用扩散加权磁共振成像(DWI),研究了神经保护和神经修复药物胞磷胆碱对急性缺血性中风患者脑缺血性病变发展的影响。纳入的患者为治疗开始前24小时内出现急性缺血性中风症状、美国国立卫生研究院卒中量表(NIHSS)评分≥5分、且DWI显示脑灰质病变体积为1至120立方厘米的患者。在基线、第1周和第12周时进行DWI、T2加权磁共振成像(MRI)、灌注加权MRI和磁共振血管造影检查。胞磷胆碱(500毫克/天)口服给药6周,对患者随访12周。主要评估指标为MRI测量的从基线到12周缺血性病变体积的变化。共有100名患者进入研究。主要MRI分析包括40名接受安慰剂治疗且有基线和第12周MRI数据的患者,以及41名接受胞磷胆碱治疗且有基线和第12周MRI数据的患者,结果未显示从基线到第12周病变体积变化有显著差异。从基线到第12周,接受安慰剂治疗的患者缺血性病变体积[所有值均为平均值(标准误)]增加了180%(107),而接受胞磷胆碱治疗的患者增加了34%(19)。在一项次要分析中,从第1周到第12周,安慰剂组病变体积减少了6.9立方厘米(2.8),胞磷胆碱组减少了17.2立方厘米(2.6)。12周内病变大小变化的预测基线变量包括低灌注体积(关联最强)、基线NIHSS评分、DWI上的病变体积、磁共振血管造影显示的动脉病变,以及从中风发作到首次给药的分类 elapsed time(≤12或>12小时)。观察到病变体积减少与NIHSS评分改善7分或更多之间存在显著关联。发现病变体积与临床指标之间存在显著相关性,这与文献中报道的较小病例系列的值一致。我们观察到胞磷胆碱治疗可使从基线到第12周的病变体积增长减少,且从第1周到第12周胞磷胆碱组的体积减少更为显著。我们发现MRI测量的12周内病变体积变化与缺血性中风的临床结局之间存在显著负相关。这种关系支持DWI作为中风临床试验中有临床意义的病变进展替代标志物的作用。胞磷胆碱减少病变生长并改善临床结局这一假设将进一步得到验证。