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儿童严重创伤性脑损伤后血清泛素 C 末端水解酶-L1 和 145 kDa αII-血影蛋白降解产物的时间反应曲线

Temporal response profiles of serum ubiquitin C-terminal hydrolase-L1 and the 145-kDa alpha II-spectrin breakdown product after severe traumatic brain injury in children.

作者信息

Metzger Ryan R, Sheng Xiaoming, Niedzwecki Christian M, Bennett Kimberly S, Morita Denise C, Zielinski Brandon, Schober Michelle E

机构信息

1Division of Pediatric Surgery.

2Department of Pediatrics.

出版信息

J Neurosurg Pediatr. 2018 Oct;22(4):369-374. doi: 10.3171/2018.4.PEDS17593. Epub 2018 Jun 29.

Abstract

OBJECTIVE

Traumatic brain injury (TBI) is the leading cause of acquired disability among children. Brain injury biomarkers may serve as useful diagnostic and prognostic indicators for TBI. Levels of ubiquitin C-terminal hydrolase-L1 (UCH-L1) and the 145-kDa alpha II-spectrin breakdown product (SBDP-145) correlate with outcome in adults after severe TBI. The authors conducted a pilot study of these biomarkers in children after severe TBI to inform future research exploring their utility in this population.

METHODS

The levels of UCH-L1 and SBDP-145 were measured in serum, and UCH-L1 in CSF from pediatric patients after severe TBI over 5 days after injury. Both biomarkers were also measured in age-matched control serum and CSF.

RESULTS

Adequate numbers of samples were obtained in serum, but not CSF, to assess biomarker temporal response profiles. Using patients with samples from all time points, UCH-L1 levels increased rapidly and transiently, peaking at 12 hours after injury. SBDP-145 levels showed a more gradual and sustained response, peaking at 48 hours. The median serum UCH-L1 concentration was greater in patients with TBI than in controls (median [IQR] = 361 [187, 1330] vs 147 [50, 241] pg/ml, respectively; p < 0.001). Receiver operating characteristic (ROC) analysis revealed an AUC of 0.77. Similarly, serum SBDP-145 was greater in children with TBI than in controls (median [IQR] = 172 [124, 257] vs 69 [40, 99] pg/ml, respectively; p < 0.001), with an ROC AUC of 0.85. When only time points of peak levels were used for ROC analysis, the discriminability of each serum biomarker increased (AUC for UCH-L1 at 12 hours = 1.0 and for SBDP-145 at 48 hours = 0.91). Serum and CSF UCH-L1 levels correlated well in patients with TBI (r = 0.70, p < 0.001).

CONCLUSIONS

Findings from this exploratory study reveal robust increases of UCH-L1 and SBDP-145 in serum and UCH-L1 in CSF obtained from children after severe TBI. In addition, important temporal profile differences were found between these biomarkers that can help guide optimal time point selection for future investigations of their potential to characterize injury or predict outcomes after pediatric TBI.

摘要

目的

创伤性脑损伤(TBI)是儿童后天性残疾的主要原因。脑损伤生物标志物可能是TBI有用的诊断和预后指标。泛素C末端水解酶-L1(UCH-L1)和145 kDaαII-血影蛋白降解产物(SBDP-145)的水平与重度TBI成年患者的预后相关。作者对重度TBI患儿的这些生物标志物进行了一项初步研究,以为未来探索其在该人群中的效用的研究提供信息。

方法

在伤后5天内测定了重度TBI患儿血清中UCH-L1和SBDP-145的水平,以及脑脊液中UCH-L1的水平。还在年龄匹配的对照血清和脑脊液中测量了这两种生物标志物。

结果

获得了足够数量的血清样本,但脑脊液样本不足,无法评估生物标志物的时间反应谱。对所有时间点都有样本的患者进行分析,UCH-L1水平迅速短暂升高,在伤后12小时达到峰值。SBDP-145水平显示出更缓慢和持续的反应,在48小时达到峰值。TBI患者血清UCH-L1浓度中位数高于对照组(中位数[四分位间距]分别为361[187,1330]与147[50,241]pg/ml;p<0.001)。受试者工作特征(ROC)分析显示曲线下面积(AUC)为0.77。同样,TBI患儿血清SBDP-145高于对照组(中位数[四分位间距]分别为172[124,257]与69[40,99]pg/ml;p<0.001),ROC AUC为0.85。当仅将峰值水平的时间点用于ROC分析时,每种血清生物标志物的辨别能力增加(UCH-L1在12小时时的AUC = 1.0,SBDP-145在48小时时的AUC = 0.91)。TBI患者血清和脑脊液UCH-L1水平相关性良好(r = 0.70,p<0.001)。

结论

这项探索性研究的结果显示,重度TBI患儿血清中UCH-L1和SBDP-145以及脑脊液中UCH-L1显著升高。此外,这些生物标志物之间存在重要的时间谱差异,这有助于指导未来研究中最佳时间点的选择,以研究它们在儿童TBI后表征损伤或预测预后的潜力。

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