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Brain‐derived circulating endothelial cells in peripheral blood of newborn infants with seizures: a potential biomarker for cerebrovascular injury

机译:癫痫发作新生婴儿外周血中脑源性循环内皮细胞:脑血管损伤的潜在生物标志物

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AbstractNeonatal seizures have been associated with cerebrovascular endothelial injury and neurological disabilities. In a piglet model, the long-term loss of endothelial regulation of cerebral blood flow coincides with the surge of brain-derived circulating endothelial cells (BCECs) in blood. We hypothesized that BCECs could serve as a noninvasive biomarker of cerebrovascular injury in neonates with seizures. In a prospective pilot feasibility study, we enrolled newborn infants with confirmed diagnoses of perinatal asphyxia and intraventricular hemorrhage (IVH); both are commonly associated with seizures. Infants without clinical evidence of cerebrovascular injuries were representative of the control group. BCECs were detected in the CD45-negative fraction of peripheral blood mononuclear cells by coexpression of CD31 (common endothelial antigen) and GLUT1 (blood-brain barrier antigen) via automated flow cytometry method. In Infants with asphyxia (n = 12) and those with IVH grade III/IV (n = 5), the BCEC levels were 9.9 ± 0.9% and 19.0 ± 2.0%, respectively. These levels were significantly higher than the control group (n = 27), 0.9 ± 0.2%, P  0.001. BCECs in infants with cerebrovascular insults with documented clinical seizures (n = 10; 16.8 ± 1.3%) were significantly higher than infants with cerebrovascular insults with subclinical or no seizures (n = 7; 9.5 ± 1.2%); P  0.001. BCEC levels decreased with seizure control. BCECs levels were elevated in infants with seizures caused by severe IVH and perinatal asphyxia. We suggest that monitoring BCEC levels in peripheral blood can potentially offer a biological marker that reflects cerebrovascular insult and recovery. Further studies with a larger number of patients are required to support these findings.
机译:摘要新生儿癫痫发作与脑血管内皮损伤和神经功能障碍有关。在仔猪模型中,脑血管的内皮调节的长期丧失与血液中脑源性循环内皮细胞(BCEC)的激增相吻合。我们假设BCECs可以作为癫痫发作新生儿脑血管损伤的非侵入性生物标志物。在一项前瞻性试点可行性研究中,我们纳入了确诊为围生期窒息和脑室内出血(IVH)的新生儿。两者通常与癫痫发作有关。没有脑血管损伤临床证据的婴儿是对照组的代表。通过自动流式细胞术方法共表达CD31(常见的内皮抗原)和GLUT1(血脑屏障抗原),在外周血单核细胞的CD45阴性级分中检测到BCEC。窒息婴儿(n = 12)和IVH III / IV级婴儿(n = 5)的BCEC水平分别为9.9±0.9%和19.0±2.0%。这些水平显着高于对照组(n = 27),0.9±0.2%,P <0.001。有临床癫痫发作记录的脑血管损伤婴儿的BCEC(n = 10; 16.8±1.3%)显着高于具有亚临床或无癫痫发作的脑血管损伤的婴儿(n = 7; 9.5±1.2%); P <0.001。随着癫痫发作控制,BCEC水平降低。严重IVH和围产期窒息引起癫痫发作的婴儿的BCECs水平升高。我们建议监测外周血中的BCEC水平可以潜在地提供反映脑血管损伤和恢复的生物学标记。为了支持这些发现,需要对更多患者进行进一步研究。

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