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Serial measurement of S100B and NSE in pediatric traumatic brain injury

机译:小儿创伤性脑损伤S100B和NSE的串行测量

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PurposeIncreased serum biomakers, such as S100 calcium-binding protein B (S100B) and neuron-specific enolase (NSE), are associated with traumatic brain injury (TBI). The purpose of this study is to investigate the serum levels of S100B and NSE in pediatric TBI patients and to predict a clinical outcome.MethodsPeripheral venous blood was collected within 6h of injury and at 1week to measure S100B and NSE. The serum S100B and NSE levels were measured using commercially available enzyme-linked immunosorbent assay kits. The authors divided participants into two groups at admission: a favorable group (patients with Glasgow Coma Scale [GCS] scores of 10-15) and an unfavorable group (patients with GCS scores of less than 9). Both S100B and NSE levels were compared between the two groups at the time of admission and 1week later.ResultsTen pediatric patients were enrolled (5 in the favorable group, 5 in the unfavorable group). The median serum S100B level of 134.21pg/ml (range, 51.00-789.65pg/ml) in patients with TBI at admission dropped to 41.49pg/ml (range, 25.65-260.93pg/ml) after 1week, with significant differences between the traumatic event and 1week later (p=0.007). The median serum NSE level of 14.76ng/ml (range, 6.48-21.23ng/ml) in patients with TBI at admission was higher than that after 1week (4.96ng/ml, range, 3.01-31.21ng/ml), with significant differences (p=0.015). A significant difference was observed in S100B after 1week between patients in the favorable and unfavorable groups (p=0.047). One patient whose serum S100B and NSE levels were elevated 1week after TBI eventually died.ConclusionsElevated serum S100B and NSE levels in pediatric TBI patients decreased 1week after traumatic events. The serum S100B level 1week after TBI was related to the severity of brain damage. These results indicated that serum S100B and NSE might play a role in predicting the prognosis and monitoring ongoing brain injury in pediatric TBI patients.
机译:有目的性的血清生物制剂,例如S100钙结合蛋白B(S100B)和神经元特异性烯醇酶(NSE)与创伤性脑损伤(TBI)有关。本研究的目的是研究儿科TBI患者S100B和NSE的血清水平,并预测临床结果。在损伤6小时内收集脑周围静脉血,以测量S100B和NSE。使用市售的酶联免疫吸附试剂盒测量血清S100B和NSE水平。作者将参与者分为两组入院:一个有利的群体(Glasgow Coma患者缩放了10-15分)和不利的群体(GCS得分少于9)。在入院时间和1周后的两组之间比较了S100B和NSE水平。评估了儿科患者(在有利的群体中的5周内,在不利的群体中的5周)。 TBI患者的134.21pg / ml(范围,51.00-789.65pg / ml)中的中位血清S100b水平为13.49pg / ml(范围,范围,25.65-260.93pg / ml),差异创伤事件和1周后(P = 0.007)。在入院的TBI患者中,14.76ng / ml(范围,6.48-21.23ng / ml)的中位血清NSE水平高于1周(4.96ng / ml,范围,3.01-31.21ng / ml),具有重要意义差异(p = 0.015)。在患者在有利和不利的群体之间的1week之后,在S100B中观察到显着差异(p = 0.047)。在TBI最终死亡后,一名患者血清S100B和NSE水平升高了1周升高了1周。小儿TBI患者的血清S100B和NSE水平在创伤事件发生后减少1周。 TBI后血清S100B级别1周与脑损伤的严重程度有关。这些结果表明,S100B和NSE血清S100B和NSE可能在预测预后和监测儿科TBI患者的持续脑损伤方面发挥作用。

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