Shiihara Takashi, Miyake Taeko, Izumi Sakiko, Watanabe Mio, Kamayachi Keiko, Kodama Kazuhiko, Nabetani Makoto, Ikemiyagi Masako, Yamaguchi Yoshio, Sawaura Noriko
Department of Neurology, Gunma Children's Medical Center, Shibukawa, Gunma 377-8577, Japan.
Pediatr Int. 2012 Feb;54(1):52-5. doi: 10.1111/j.1442-200X.2011.03454.x. Epub 2011 Oct 30.
Acute encephalopathy with biphasic seizures and late reduced diffusion (AESD) is characterized clinically by biphasic seizures and late magnetic resonance imaging abnormalities, such as reduced subcortical diffusion from day 3 onwards, often accompanied with some neurological sequelae. In the early stages of the disease, AESD closely resembles its far more prevalent and relatively benign counterpart, febrile seizure (FS).
We measured and compared the serum or cerebrospinal fluid (CSF) levels of S100B, neuron-specific enolase (NSE), and total tau protein in 43 patients with FS and 18 patients with AESD, at any point during the disease. To assess early diagnostic validity, we compared these biomarkers in 43 FS and eight AESD patients, with whom the day 0-2 samples were available. We used the receiver-operator characteristic curve to evaluate the diagnostic values of these markers.
The levels of all biomarkers were significantly higher in AESD than FS patients. When only day 0-2 samples from AESD patients were used, the levels of all the measured biomarkers, except serum NSE, were still significantly higher in patients with AESD than in FS, suggesting that AESD could damage astrocytes, neurons, and axons, even in the early stages of the disease. According to the receiver-operator characteristic curve analyses, CSF S100B (cut-off value, 100 pg/mL) and CSF total tau protein (cut-off value, 100 pg/mL) were better predictors of AESD than other biomarkers.
The combination of CSF S100B and CSF total tau protein resulted in a positive predictive value of AESD 83.3%, which could be helpful for early diagnosis, facilitating early therapeutic interventions.
伴有双相性癫痫发作和晚期弥散受限的急性脑病(AESD)的临床特征为双相性癫痫发作和晚期磁共振成像异常,例如从第3天起皮质下弥散受限,常伴有一些神经后遗症。在疾病的早期阶段,AESD与更为常见且相对良性的热性惊厥(FS)极为相似。
我们在疾病的任何阶段测量并比较了43例FS患者和18例AESD患者的血清或脑脊液(CSF)中S100B、神经元特异性烯醇化酶(NSE)和总tau蛋白的水平。为评估早期诊断的有效性,我们比较了43例FS患者和8例AESD患者(可获取第0 - 2天样本)的这些生物标志物。我们使用受试者工作特征曲线来评估这些标志物的诊断价值。
AESD患者所有生物标志物的水平均显著高于FS患者。仅使用AESD患者第0 - 2天的样本时,除血清NSE外,所有测量的生物标志物在AESD患者中的水平仍显著高于FS患者,这表明即使在疾病的早期阶段,AESD也会损害星形胶质细胞、神经元和轴突。根据受试者工作特征曲线分析,脑脊液S100B(临界值,100 pg/mL)和脑脊液总tau蛋白(临界值,100 pg/mL)比其他生物标志物更能预测AESD。
脑脊液S100B和脑脊液总tau蛋白的联合检测对AESD的阳性预测值为83.3%,这有助于早期诊断,促进早期治疗干预。
