Department of Molecular and Developmental Medicine, General Hospital "Santa Maria alle Scotte", University of Siena, Italy.
Department of Pediatrics, University of Florida, Gainesville, FL, USA.
Cytokine. 2018 Nov;111:119-124. doi: 10.1016/j.cyto.2018.08.011. Epub 2018 Aug 22.
Inflammation is a crucial but understudied mechanism of neuronal injury after hypoxia-ischemia. The aim was to identify a panel of cytokines involved in brain injury in neonates with hypoxic ischemic encephalopathy (HIE).
Ten newborns with HIE undergoing to therapeutic hypothermia (TH, HIE Group) and 8 healthy newborns (CTRL Group) were enrolled. For the HIE group, 5 samples were collected: between 0 and 6 h of life (time 1), 12 h (time 2), 24 h (time 3), 48 h (time 4) and 96 h of life (time 5). For the CTRL group, one sample was collected. A panel of 48 inflammatory cytokines was determined in all samples. Data were analyzed using multivariate statistical analysis (Principal component analysis, PCA) RESULTS: 17 cytokines, among 48 analyzed, were found to be significantly different, initially, between the CTRL and HIE groups: 12 with reported pro-inflammatory effects and 5 with reported anti-inflammatory effects. In the HIE group cytokines showed a decreasing trend during the TH and at the end of treatment comparable to the CTRL group. IL-18 did demonstrate a slight increase at time 3 during HT but decreased steadily at sampling times, 4 and 5.
Our data demonstrates that many pathways of the inflammatory cascade are activated following hypoxic-ischemic injury. This information will increase our understanding of changes in cytokines over time in neonates with HIE undergoing TH.
炎症是缺氧缺血后神经元损伤的一个关键但研究不足的机制。本研究旨在确定一组参与新生儿缺氧缺血性脑病(HIE)脑损伤的细胞因子。
纳入 10 名接受治疗性低温(TH)的 HIE 新生儿(HIE 组)和 8 名健康新生儿(CTRL 组)。HIE 组采集 5 个时间点的样本:出生后 0-6 小时(时间 1)、12 小时(时间 2)、24 小时(时间 3)、48 小时(时间 4)和 96 小时(时间 5)。CTRL 组采集 1 个时间点的样本。在所有样本中测定了 48 种炎症细胞因子的表达。使用多元统计分析(主成分分析,PCA)对数据进行分析。
在所分析的 48 种细胞因子中,有 17 种在 CTRL 组和 HIE 组之间最初存在显著差异:12 种具有已知的促炎作用,5 种具有抗炎作用。在 HIE 组中,在 TH 期间和治疗结束时,细胞因子呈下降趋势,与 CTRL 组相似。IL-18 在 HT 期间时间 3 时略有增加,但在采样时间 4 和 5 时逐渐下降。
我们的数据表明,许多炎症级联途径在缺氧缺血性损伤后被激活。这些信息将增加我们对接受 TH 的 HIE 新生儿细胞因子随时间变化的理解。
