Sleep architecture in neonatal and infantile onset epilepsies in the first six months of life: A scoping review

癫痫 睡眠(系统调用) 睡眠架构 儿科 遗传建筑学 心理学 脑电图 睡眠剥夺 医学 神经科学 认知 多导睡眠图 人口 操作系统 环境卫生 数量性状位点 计算机科学
作者
Sangeeta Jethwa,Ronit M. Pressler,Didem Kaya,Alexandre N. Datta
出处
期刊:European Journal of Paediatric Neurology [Elsevier BV]
卷期号:41: 99-108
标识
DOI:10.1016/j.ejpn.2022.11.004
摘要

Epilepsy occurs in approximately 80 per 100,000 infants in the first year of life, ranging in severity from self-limited and likely to spontaneously resolve, to severe developmental and epileptic encephalopathies. Sleep plays a key role in early brain development and the reciprocal relationship between sleep and seizures is not yet fully understood, particularly in young children. We conducted a Scoping Review to synthesise current knowledge of sleep architecture in neonates and infants with epilepsy.Peer-reviewed publications from 2005 to 2022 describing sleep architecture in infants up to six months of age with unprovoked seizures were included. The analysis set was derived from EMBASE, Web of Science and PubMED using key terms "sleep, epilepsy and infant" and related descriptors. Inclusion criteria were prospectively described in a Scoping Review protocol. Sleep architecture was assessed as macro- and micro-structural elements.21 publications were included in the qualitative analysis. In self-limited familial and genetic epilepsy, sleep macrostructure was generally preserved. In DEEs and in epileptic encephalopathies of genetic or structural aetiology, sleep architecture was significantly disrupted.Early identification of infants with epilepsy is important to ensure early and effective treatment. In the DEE spectrum, sleep architecture is significantly impacted, and abnormal sleep architecture may be associated with compromised developmental outcome. Further research is needed to identify the sequence of events in abnormal brain development, epilepsy and sleep disruption and potentially help to predict the course of epilepsy towards a self-limited epilepsy versus a DEE.
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