School of Mental Health and Neuroscience, Maastricht University, Universiteitssingel 40, Maastricht, 6229 ER, The Netherlands.
J Neuroinflammation. 2013 Jan 24;10:13. doi: 10.1186/1742-2094-10-13.
Hypoxic-ischemic encephalopathy (HIE) is one of the most important causes of brain injury in preterm infants. Preterm HIE is predominantly caused by global hypoxia-ischemia (HI). In contrast, focal ischemia is most common in the adult brain and known to result in cerebral inflammation and activation of the peripheral immune system. These inflammatory responses are considered to play an important role in the adverse outcomes following brain ischemia. In this study, we hypothesize that cerebral and peripheral immune activation is also involved in preterm brain injury after global HI.
Preterm instrumented fetal sheep were exposed to 25 minutes of umbilical cord occlusion (UCO) (n = 8) at 0.7 gestation. Sham-treated animals (n = 8) were used as a control group. Brain sections were stained for ionized calcium binding adaptor molecule 1 (IBA-1) to investigate microglial proliferation and activation. The peripheral immune system was studied by assessment of circulating white blood cell counts, cellular changes of the spleen and influx of peripheral immune cells (MPO-positive neutrophils) into the brain. Pre-oligodendrocytes (preOLs) and myelin basic protein (MBP) were detected to determine white matter injury. Electro-encephalography (EEG) was recorded to assess functional impairment by interburst interval (IBI) length analysis.
Global HI resulted in profound activation and proliferation of microglia in the hippocampus, periventricular and subcortical white matter. In addition, non-preferential mobilization of white blood cells into the circulation was observed within 1 day after global HI and a significant influx of neutrophils into the brain was detected 7 days after the global HI insult. Furthermore, global HI resulted in marked involution of the spleen, which could not be explained by increased splenic apoptosis. In concordance with cerebral inflammation, global HI induced severe brain atrophy, region-specific preOL vulnerability, hypomyelination and persistent suppressed brain function.
Our data provided evidence that global HI in preterm ovine fetuses resulted in profound cerebral inflammation and mobilization of the peripheral innate immune system. These inflammatory responses were paralleled by marked injury and functional loss of the preterm brain. Further understanding of the interplay between preterm brain inflammation and activation of the peripheral immune system following global HI will contribute to the development of future therapeutic interventions in preterm HIE.
缺氧缺血性脑病(HIE)是早产儿脑损伤的最重要原因之一。早产儿 HIE 主要由全脑缺氧缺血(HI)引起。相比之下,局灶性缺血在成人大脑中最为常见,已知会导致大脑炎症和外周免疫系统的激活。这些炎症反应被认为在脑缺血后的不良结局中发挥重要作用。在这项研究中,我们假设在全脑 HI 后,大脑和外周免疫激活也与早产儿脑损伤有关。
对 0.7 胎龄的早产仪器化胎儿羊进行 25 分钟脐带结扎(UCO)(n = 8)。假手术处理的动物(n = 8)作为对照组。用离子钙结合衔接蛋白 1(IBA-1)染色来研究小胶质细胞的增殖和激活,以研究大脑切片。通过评估循环白细胞计数、脾脏的细胞变化以及外周免疫细胞(髓过氧化物酶阳性中性粒细胞)进入大脑的情况来研究外周免疫系统。检测前少突胶质细胞(preOLs)和髓鞘碱性蛋白(MBP)以确定白质损伤。通过脑电(EEG)记录分析脑电(EEG)来评估功能损伤。
全脑 HI 导致海马、脑室周围和皮质下白质中小胶质细胞的强烈激活和增殖。此外,在全脑 HI 后 1 天内观察到白细胞向循环系统的非优先动员,并且在全脑 HI 损伤后 7 天检测到大量中性粒细胞进入大脑。此外,全脑 HI 导致脾脏明显萎缩,而这种情况不能用脾细胞凋亡增加来解释。与大脑炎症一致,全脑 HI 导致严重的脑萎缩、特定区域的 preOL 脆弱性、少突胶质细胞脱髓鞘和持续抑制的脑功能。
我们的数据提供了证据,证明早产羊胎儿的全脑 HI 导致了严重的大脑炎症和外周固有免疫系统的动员。这些炎症反应伴随着早产儿大脑的明显损伤和功能丧失。进一步了解全脑 HI 后早产儿脑炎症与外周免疫激活之间的相互作用,将有助于开发治疗早产儿 HIE 的新疗法。
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