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儿童创伤后癫痫的急性生理学预测。

Acute physiologic prediction of pediatric post-traumatic epilepsy.

机构信息

Barrow Neurological Institute at Phoenix Children's Hospital, 1919 E. Thomas Road, Ambulatory Building, 3rd Floor, Phoenix, AZ 85016, USA.

Phoenix Children's Hospital, Department of Radiology, 1919 E. Thomas Road, Ambulatory Building, 3rd Floor, Phoenix, AZ 85016, USA.

出版信息

Epilepsy Res. 2022 Jul;183:106935. doi: 10.1016/j.eplepsyres.2022.106935. Epub 2022 Apr 27.

Abstract

OBJECTIVE

Post-traumatic epilepsy (PTE) is a known complication of traumatic brain injury (TBI). Limited physiologic biomarkers have been investigated in relation to pediatric PTE. Our aim is to identify clinical, physiologic and neuroimaging biomarkers predictive of pediatric PTE arising during the acute care phase after injury.

METHODS

We performed a retrospective analysis from a prospectively collected clinical database of pediatric patients who underwent multimodality neurologic monitoring that included continuous electroencephalography and intracranial pressure (ICP) monitoring. Biomarkers included hemodynamic vital signs, model-based indices of cerebrovascular pressure reactivity (CVPR) and autonomic function (AF), electroencephalographic abnormalities, and neuroimaging abnormalities on the initial CT scan on day of imaging. Our primary outcome, PTE, was classified as the presence of unprovoked seizures 2 months post-injury or the continued need for antiseizure medications at 12-month post-injury. We utilized univariate logistic regression to identify biomarkers associated with PTE.

RESULTS

61 surviving patients were included in this study, among which 10 (16.4%) developed PTE. We identified that PTE was associated with increased ICP (odds ratio [OR] 1.25, 95% confidence interval [CI] 1.02-1.52), increased pressure reactivity indices (92.53, 2.84->999.99), increased wavelet pressure reactivity indices (121.76, 2.84->999.99), increased CT Marshall scores (1.76, 1.13-2.74), decreased HRsd (0.54, 0.33-0.87) and the presence of epileptiform discharges (8.06, 1.85-35.17), and abnormal sleep spindles (4.88, 1.18-20.00). Whereas early post-traumatic seizures within the first 7 days post-injury were associated with PTE development (7.58, 1.81-39.68), this association was significant for such seizures occurring between 24 and 168 h post-injury (21.47, 4.18-110.38), and not for seizures occurring within 24 h post-injury. Among patients experiencing early post-traumatic seizures, increased time with seizures on surface electroencephalography was associated with PTE development (7.28, 2.05-73.14). We also identified that development of PTE was associated with worsened functional outcomes identified by increased Glasgow Outcome Scale - Extended Pediatric (GOSE-PEDs) scores (3.18, 1.68-8.01).

CONCLUSION

Pediatric PTE development is associated with increased ICP, impaired CVPR, low heart rate variability, worsened neuroimaging findings, and electroencephalographic abnormalities identified during intensive care. Further studies are needed to investigate strategies to mitigate pediatric PTE development.

摘要

目的

创伤性脑损伤(TBI)后发生的外伤性癫痫(PTE)是已知的并发症。已经研究了有限的生理生物标志物与儿科 PTE 相关。我们的目的是确定与损伤后急性护理阶段发生的儿科 PTE 相关的临床、生理和神经影像学生物标志物。

方法

我们对接受包括连续脑电图和颅内压(ICP)监测在内的多模态神经监测的儿科患者进行了前瞻性收集的临床数据库的回顾性分析。生物标志物包括血流动力学生命体征、基于模型的脑血管压力反应性(CVPR)和自主功能(AF)指数、脑电图异常以及初始 CT 扫描上的神经影像学异常成像当天。我们的主要结局是 PTE,定义为损伤后 2 个月内出现无诱因发作或损伤后 12 个月时仍需要抗癫痫药物。我们利用单变量逻辑回归来确定与 PTE 相关的生物标志物。

结果

本研究纳入了 61 名存活患者,其中 10 名(16.4%)发生了 PTE。我们发现 PTE 与 ICP 升高(比值比 [OR] 1.25,95%置信区间 [CI] 1.02-1.52)、压力反应性指数升高(92.53,2.84->999.99)、小波压力反应性指数升高(121.76,2.84->999.99)、CT Marshall 评分升高(1.76,1.13-2.74)、HRsd 降低(0.54,0.33-0.87)和出现癫痫样放电(8.06,1.85-35.17)以及异常睡眠纺锤波(4.88,1.18-20.00)有关。而损伤后前 7 天内出现的早期创伤性发作与 PTE 发展相关(7.58,1.81-39.68),但这种关联仅在损伤后 24 至 168 小时之间出现的发作中显著(21.47,4.18-110.38),而在损伤后 24 小时内出现的发作中则不显著。在经历早期创伤性发作的患者中,表面脑电图上癫痫发作时间的增加与 PTE 发展相关(7.28,2.05-73.14)。我们还发现,格拉斯哥结局量表-扩展儿科(GOSE-PEDs)评分升高(3.18,1.68-8.01)与 PTE 发展有关。

结论

儿科 PTE 的发展与 ICP 升高、CVPR 受损、心率变异性降低、神经影像学发现恶化以及重症监护期间出现的脑电图异常有关。需要进一步研究以探讨减轻儿科 PTE 发展的策略。

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