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首页> 外文期刊>Amyotrophic lateral sclerosis eofficial publication of the World Federation of Neurology Research Group on Motor Neuron Diseases >Neurophysiological index as a biomarker for ALS progression: Validity of mixed effects models
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Neurophysiological index as a biomarker for ALS progression: Validity of mixed effects models

机译:神经生理指标作为ALS进展的生物标志物:混合效应模型的有效性

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摘要

Our objective was to evaluate the neurophysiological index (NI) as a biomarker for amyotrophic lateral sclerosis (ALS) and to assess the validity of linear mixed effects models for describing longitudinal changes. Functional assessment and nerve conduction studies were undertaken in 58 ALS patients. Neurophysiological data were collected on four occasions over 12 weeks (baseline, weeks 4, 8 and 12). The NI was calculated for the abductor digiti minimi and ulnar nerve at the wrist. NI declined at a rate of 0.04 per week (S.E. 0.006, p < 0.0001). Patients with bulbar-onset disease had 0.88 greater NI than patients with upper limb-onset disease over the follow-up period (S.E. 0.39, p = 0.03). There were no differences in the rates of decline among patients with different disease phenotypes. Rates of change in NI and functional impairment were weakly correlated (Spearman's p = 0.29, p = 0.03). Linear mixed effects models were appropriate for detailing the longitudinal changes in NI. The present findings support incorporation of NI as an outcome measure for ALS clinical trials conducted over short time periods.
机译:我们的目标是评估神经生理指标(NI)作为肌萎缩性侧索硬化(ALS)的生物标记,并评估用于描述纵向变化的线性混合效应模型的有效性。在58例ALS患者中进行了功能评估和神经传导研究。在12周内(基线,第4、8和12周)四次收集神经生理学数据。计算NI为手腕外展指最小和尺神经。 NI每周下降0.04(S.E. 0.006,p <0.0001)。在随访期内,延髓性疾病患者的NI比上肢性疾病患者高0.88(S.E. 0.39,p = 0.03)。在具有不同疾病表型的患者中,下降率没有差异。 NI的变化率与功能障碍的相关性很弱(Spearman's p = 0.29,p = 0.03)。线性混合效应模型适合于详细描述NI的纵向变化。本研究结果支持将NI作为短期内进行的ALS临床试验的一项结局指标。

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