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新生儿脑病的预后神经生物标志物。

Prognostic Neurobiomarkers in Neonatal Encephalopathy.

机构信息

The Department of Physiology, University of Auckland, Auckland, New Zealand.

出版信息

Dev Neurosci. 2022;44(4-5):331-343. doi: 10.1159/000522617. Epub 2022 Feb 15.

DOI:10.1159/000522617
PMID:35168240
Abstract

Therapeutic hypothermia (TH) is now a standard treatment for infants with moderate-to-severe neonatal encephalopathy (NE), and improves brain damage on neuroimaging and neurodevelopmental outcomes. Critically, for effective neuroprotection, hypothermia should be started within 6 h from birth. There is compelling evidence to suggest that a proportion of infants with mild NE have material risk of developing brain damage and poor outcomes. This cohort is increasingly being offered TH, despite lack of trial evidence for its benefit. In current practice, infants need to be diagnosed within 6 h of birth for therapeutic treatment, compared to retrospective NE grading in the pre-hypothermia era. This presents challenges as NE is a dynamic brain disorder that can worsen or resolve over time. Neurological symptoms of NE can be difficult to discern in the first few hours after birth, and confounded by analgesics and anesthetic treatment. Using current enrolment criteria, a significant number of infants with NE that would benefit from hypothermia are not treated, and vice versa, some infants receive hypothermia when its benefit will be limited. Better biomarkers are needed to further improve management and treatment of these neonates. In the present review, we examine the latest research, and highlight a central limitation of most current biomarkers: that their predictive value is consistently greatest after most neuroprotective therapies are no longer effective.

摘要

治疗性低温(therapeutic hypothermia,TH)现在是中重度新生儿脑病(neonatal encephalopathy,NE)患儿的标准治疗方法,可改善神经影像学和神经发育结局的脑损伤。关键是,为了实现有效的神经保护,低温治疗应在出生后 6 小时内开始。有强有力的证据表明,一部分轻度 NE 患儿有发生脑损伤和不良结局的实质性风险。尽管缺乏其获益的临床试验证据,但这部分患儿越来越多地接受了低温治疗。在目前的实践中,与低温前的回顾性 NE 分级相比,需要在出生后 6 小时内对患儿进行诊断,以进行治疗性治疗。这带来了挑战,因为 NE 是一种动态的脑疾病,随着时间的推移可能会恶化或缓解。NE 的神经症状在出生后最初几个小时可能难以识别,并且会受到镇痛和麻醉治疗的干扰。根据目前的入组标准,有相当数量的 NE 患儿本应接受低温治疗,但未得到治疗,反之亦然,一些患儿接受了低温治疗,但获益有限。需要更好的生物标志物来进一步改善这些新生儿的管理和治疗。在本综述中,我们检查了最新的研究,并强调了大多数当前生物标志物的一个核心局限性:它们的预测价值在大多数神经保护治疗不再有效的情况下,始终是最大的。

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