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新生儿缺血性癫痫发作后睡眠功能障碍的差异与 qEEG 确定的新生儿损伤时龄有关,这在小鼠模型中得到了证实。

Sleep dysfunction following neonatal ischemic seizures are differential by neonatal age of insult as determined by qEEG in a mouse model.

机构信息

Department of Neuroscience, Hugo Moser Research Institute at Kennedy Krieger, Johns Hopkins University, Baltimore, MD 21205, USA.

Department of Biomedical Engineering, Johns Hopkins University, Baltimore, MD 21205, USA.

出版信息

Neurobiol Dis. 2018 Aug;116:1-12. doi: 10.1016/j.nbd.2018.04.012. Epub 2018 Apr 21.

Abstract

Neonatal seizures associated with hypoxic-ischemic encephalopathy (HIE) pose a challenge in their acute clinical management and are often followed by long-term neurological consequences. We used a newly characterized CD-1 mouse model of neonatal ischemic seizures associated with age-dependent (P7 vs. P10) seizure severity and phenobarbital efficacy (i.e.; PB-resistant vs. PB-efficacious respectively) following unilateral carotid ligation. The long-term consequences following untreated neonatal seizures in P7 vs. P10 ligated pups were investigated using neurobehavioral testing, 24 h v- quantitative EEG -EMG (qEEG, qEMG), and western blot analyses in adult mice. Significant hyperactivity emerged in a small sub-set of mice in both age-groups associated with a failure to habituate during open-field (OF) testing. 24 h continuous qEEGs detected significantly altered sleep architecture due to long-wake cycles in both age-groups. Delta power (0.5-4 Hz) quantification during slow-wave-sleep (SWS) revealed significant SWS compensation in P10 ligates following periods of increased sleep pressure which the P7 ligate group failed to show. Theta/beta ratios deemed as negative correlation markers of attentional control were significantly higher only in the P10 ligates. These results indicate that neonatal age-dependent differences in the characteristics of ischemic neonatal seizures in CD-1 pups differentially modulate long-term outcomes, when evaluated with v-qEEG/EMG as adults.

摘要

与缺氧缺血性脑病 (HIE) 相关的新生儿癫痫发作在急性临床管理中带来了挑战,并且常常伴有长期的神经后果。我们使用了一种新的 CD-1 幼鼠模型,该模型与年龄依赖性(P7 与 P10)的癫痫发作严重程度以及苯巴比妥的疗效相关(即分别为苯巴比妥耐药和苯巴比妥有效),随后进行单侧颈总动脉结扎。在 P7 与 P10 结扎幼鼠中,我们使用神经行为测试、24 小时 v-定量脑电图-肌电图 (qEEG、qEMG) 和成年小鼠的 Western blot 分析来研究未经治疗的新生儿癫痫发作后的长期后果。在两个年龄组中,一小部分幼鼠都出现了明显的多动症状,与旷场 (OF) 测试中的习惯化失败有关。24 小时连续 qEEG 检测到由于两个年龄组中长醒周期而导致的睡眠结构发生了明显改变。在慢波睡眠 (SWS) 期间对δ功率 (0.5-4 Hz) 进行量化,发现 P10 结扎组在睡眠压力增加期间表现出显著的 SWS 补偿,而 P7 结扎组则没有表现出这种情况。被认为是注意力控制负相关标记物的θ/β 比值仅在 P10 结扎组中显著升高。这些结果表明,在 CD-1 幼鼠中,与缺氧缺血性相关的新生儿癫痫发作的特征在新生儿期存在年龄依赖性差异,当以 v-qEEG/EMG 作为成人评估时,这些差异会对长期结果产生不同的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fd34/5995660/b9dfa77bcb0f/nihms962157f1.jpg

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