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首页> 外文期刊>Neurology: Official Journal of the American Academy of Neurology >Multiple biomarkers covering distinct pathways for predicting outcomes after ischemic stroke
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Multiple biomarkers covering distinct pathways for predicting outcomes after ischemic stroke

机译:多个生物标志物覆盖不同的途径缺血性中风后预测结果

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Objective To study the prognostic significance of multiple novel biomarkers in combination after ischemic stroke. Methods We derived data from the China Antihypertensive Trial in Acute Ischemic Stroke, and 12 informative biomarkers were measured. The primary outcome was the combination of death and major disability (modified Rankin Scale score >= 3) at 3 months after ischemic stroke, and secondary outcomes included major disability, death, and vascular events. Results In 3,405 participants, 866 participants (25.4%) experienced major disability or died within 3 months. In multivariable analyses, elevated high-sensitive C-reactive protein, complement C3, matrix metalloproteinase-9, hepatocyte growth factor, and antiphosphatidylserine antibodies were individually associated with the primary outcome. Participants with a larger number of elevated biomarkers had increased risk of all study outcomes. The adjusted odds ratios (95% confidence intervals) of participants with 5 elevated biomarkers were 3.88 (2.05-7.36) for the primary outcome, 2.81 (1.49-5.33) for major disability, 5.67 (1.09-29.52) for death, and 4.00 (1.22-13.14) for vascular events, compared to those with no elevated biomarkers. Simultaneously adding these 5 biomarkers to the basic model with traditional risk factors led to substantial reclassification for the combined outcome (net reclassification improvement 28.5%, p < 0.001; integrated discrimination improvement 2.2%, p < 0.001) and vascular events (net reclassification improvement 37.0%, p = 0.001; integrated discrimination improvement 0.8%, p = 0.001). Conclusion We observed a clear gradient relationship between the numbers of elevated novel biomarkers and risk of major disability, mortality, and vascular events. Incorporation of a combination of multiple biomarkers observed substantially improved the risk stratification for adverse outcomes in ischemic stroke patients.
机译:摘要目的研究的预后意义之后结合多种新颖的生物标志物缺血性中风。中国在急性缺血性降压试验中风和12的生物标记测量。死亡和重大残疾的兰金(修改量表得分> = 3)在脑缺血后3个月中风和次要结果包括专业残疾、死亡和血管事件。866年3405名参与者,参与者(25.4%)经历了重大残疾或死亡在3个月。高灵敏度c反应蛋白、补体C3、矩阵metalloproteinase-9,肝细胞生长因素,antiphosphatidylserine抗体分别与主吗结果。生物标志物升高的风险增加了研究的结果。置信区间)的参与者5生物标志物升高3.88 (2.05 - -7.36)主要结果,2.81 (1.49 - -5.33)为死亡,残疾,5.67(1.09 - -29.52)和4.00为血管事件(1.22 - -13.14),相比那些没有生物标志物升高。将这5个生物标记添加到基本模型传统的风险因素导致实质性的重新分类为合并后的结果(净重新分类提高28.5%,p < 0.001;集成歧视改善2.2%,p <0.001)和血管事件(净重新分类提高37.0%,p = 0.001;歧视改善0.8%,p = 0.001)。结论我们观察到一个明显的梯度升高的数量之间的关系新型生物标志物和风险的主要障碍,死亡率,和血管事件。结合多个生物标志物大大提高了危险分层对缺血性中风患者的不良结果。

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