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Prognostic value of somatosensory evoked potentials, neuron-specific enolase, and S100 for short-term outcome in ischemic stroke

机译:体感诱发电位,神经元特异性烯醇化酶和S100对缺血性卒中短期预后的预后价值

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Haupt WF, Chopan G, Sobesky J, Liu WC, Dohmen C. Prognostic value of somatosensory evoked potentials, neuron-specific enolase, and S100 for short-term outcome in ischemic stroke. / Neurophysiol 115: 1273-1278, 2016. First published December 23, 2015; doi:10.1152/jn.01012.2015.—To predict short-term outcome in acute ischemic stroke, we analyzed somatosensory evoked potentials (SEP) and biochemical parameters [neuron-specific enolase (NSE) and S100 protein] in a prospective study with serial measurement. In 31 patients with 1st middle cerebral artery infarction, serum NSE and S100 protein were measured daily between days 1 and 6 poststroke. The N20 and N70 components of the SEP (SEP20 and SEP70) were determined on days 1 and 6. SEP and biochemical markers in stroke patients were compared with a control group. Short-term outcome was assessed by the modified Rankin Scale (mRS) at days 7-10 and was dichotomized between good (mRS 0-2) and poor (mRS >3) outcome. Specificity and positive predictive value (PPV) were high at day 1 for SEP (SEP20: 100% for both; SEP70: 93 and 88%, respectively) compared with lower values for NSE (67 and 50%) and S100 (23 and 57%). In contrast, S100 showed the highest sensitivity at day 1 with 77% compared with a relatively low sensitivity of NSE (31%) and SEP (SEP20: 35%, SEP70: 47%). The biochemical markers showed an improving sensitivity over time with best values (>90%) between days 3 and 4 at the expense of a lower specificity. Specificity and PPV of SEP on day 6 was still 100% with sensitivity increasing up to 53% (SEP20) and 60% (SEP70). SEP could early differentiate between good and poor outcome and reliably predict poor outcome. Since biochemical markers and SEP complement each other in the prognosis of stroke, a combined application of these markers seems promising.
机译:Haupt WF,Chopan G,Sobesky J,Liu WC,DohmenC。躯体感觉诱发电位,神经元特异性烯醇化酶和S100对缺血性卒中的短期预后的预后价值。 / Neurophysiol 115:1273-1278,2016年。2015年12月23日首次发布; doi:10.1152 / jn.01012.2015。—为了预测急性缺血性卒中的短期预后,我们在一项前瞻性研究中通过系列测量分析了体感诱发电位(SEP)和生化参数[神经特异性烯醇化酶(NSE)和S100蛋白]。 。在31例第一脑中动脉梗死患者中,卒中后第1天至第6天每天测量血清NSE和S100蛋白。在第1天和第6天确定SEP的N20和N70成分(SEP20和SEP70)。将中风患者的SEP和生化标志物与对照组进行比较。短期结果在7-10天通过改良的Rankin量表(mRS)进行评估,并分为好(mRS 0-2)和差(mRS> 3)结果。 SEP在第1天的特异性和阳性预测值(PPV)高(SEP20:两者均为100%; SEP70:分别为93和88%),而NSE(67和50%)和S100则较低(23和57) %)。相反,S100在第1天显示出最高的敏感性,为77%,而NSE和SEP的敏感性相对较低(SEP20:35%,SEP70:47%)。生化标记物随着时间的推移显示出提高的敏感性,在第3天到第4天之间具有最佳值(> 90%),但特异性较低。第6天SEP的特异性和PPV仍为100%,敏感性增加到53%(SEP20)和60%(SEP70)。 SEP可以及早区分好结果和差结果,并可靠地预测差的结果。由于生化标志物和SEP在中风的预后方面互为补充,因此这些标志物的联合应用似乎很有希望。

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