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产后使用苯巴比妥预防早产儿脑室内出血

Postnatal phenobarbital for the prevention of intraventricular haemorrhage in preterm infants.

作者信息

Smit Elisa, Odd David, Whitelaw Andrew

机构信息

Neonatal Neuroscience, University of Bristol, St Michaels Hospital, Level D, Southwell Street, Bristol, UK, BS2 8EG.

出版信息

Cochrane Database Syst Rev. 2013 Aug 13;2013(8):CD001691. doi: 10.1002/14651858.CD001691.pub3.

DOI:10.1002/14651858.CD001691.pub3
PMID:23943189
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7061244/
Abstract

BACKGROUND

Intraventricular haemorrhage (IVH) is a major complication of preterm birth. Large haemorrhages are associated with a high risk of disability and hydrocephalus. Instability of blood pressure and cerebral blood flow are postulated as causative factors. Another mechanism may involve reperfusion damage from oxygen free radicals. Phenobarbital has been suggested as a safe treatment that stabilises blood pressure and may protect against free radicals.

OBJECTIVES

To determine the effect of postnatal administration of phenobarbital on the risk of IVH, neurodevelopmental impairment or death in preterm infants.

SEARCH METHODS

We used the search strategy of the Neonatal Collaborative Review Group. The original review author (A Whitelaw) was an active trialist in this area and had personal contact with many groups in this field. He handsearched journals from 1976 (when cranial computed tomography (CT) scanning started) to October 2000; these included: Pediatrics, Journal of Pediatrics, Archives of Disease in Childhood, Pediatric Research, Developmental Medicine and Child Neurology, Acta Paediatrica, European Journal of Pediatrics, Neuropediatrics, New England Journal of Medicine, Lancet and British Medical Journal. We searched the National Library of Medicine (USA) database (via PubMed) and the Cochrane Central Register of Controlled Trials (CENTRAL, 2012, Issue 10) through to 31 October 2012. We did not limit the searches to the English language, as long as the article included an English abstract. We read identified articles in the original language or translated.

SELECTION CRITERIA

We included randomised or quasi-randomised controlled trials in which phenobarbital was given to preterm infants identified as being at risk of IVH because of gestational age below 34 weeks, birthweight below 1500 g or respiratory failure. Adequate determination of IVH by ultrasound or CT was also required.

DATA COLLECTION AND ANALYSIS

In addition to details of patient selection and control of bias, we extracted the details of the administration of phenobarbital. We searched for the following endpoints: IVH (with grading), posthaemorrhagic ventricular dilation or hydrocephalus, neurodevelopmental impairment and death. In addition, we searched for possible adverse effects of phenobarbitone, for example hypotension, mechanical ventilation, pneumothorax, hypercapnia and acidosis.

MAIN RESULTS

We included 12 controlled trials that recruited 982 infants. There was heterogeneity between trials for the outcome IVH, with three trials finding a significant decrease in IVH and one trial finding an increase in IVH in the group receiving phenobarbital. Meta-analysis showed no difference between the phenobarbital-treated group and the control group in either all IVH (typical risk ratio (RR) 0.91; 95% CI 0.77 to 1.08), severe IVH (typical RR 0.77; 95% CI 0.58 to 1.04), posthaemorrhagic ventricular dilation (typical RR 0.89; 95% CI 0.38 to 2.08), severe neurodevelopmental impairment (typical RR 1.44; 95% CI 0.41 to 5.04) or death before hospital discharge (typical RR 0.88; 95% CI 0.64 to 1.21). There was a consistent trend in the trials towards increased use of mechanical ventilation in the phenobarbital-treated group, which was supported by the meta-analysis (typical RR 1.18; 95% CI 1.06 to 1.32; typical risk difference 0.129; 95% CI 0.04 to 0.21), but there was no significant difference in pneumothorax, acidosis or hypercapnia.

AUTHORS' CONCLUSIONS: Postnatal administration of phenobarbital cannot be recommended as prophylaxis to prevent IVH in preterm infants and is associated with an increased need for mechanical ventilation.

摘要

背景

脑室内出血(IVH)是早产的主要并发症。大量出血与高致残风险和脑积水相关。血压和脑血流不稳定被认为是致病因素。另一种机制可能涉及氧自由基的再灌注损伤。苯巴比妥被认为是一种安全的治疗方法,可稳定血压并可能抵御自由基。

目的

确定出生后给予苯巴比妥对早产儿发生IVH、神经发育障碍或死亡风险的影响。

检索方法

我们采用了新生儿协作审查组的检索策略。原始综述作者(A·惠特洛)是该领域的活跃试验者,与该领域的许多团队有个人联系。他手工检索了1976年(头颅计算机断层扫描(CT)扫描开始时)至2000年10月的期刊;这些期刊包括:《儿科学》《儿科学杂志》《儿童疾病档案》《儿科研究》《发育医学与儿童神经病学》《儿科学报》《欧洲儿科学杂志》《神经儿科学》《新英格兰医学杂志》《柳叶刀》和《英国医学杂志》。我们检索了美国国立医学图书馆数据库(通过PubMed)以及截至2012年10月31日的Cochrane对照试验中心注册库(CENTRAL,2012年第10期)。我们不将检索限于英语,只要文章包含英文摘要即可。我们阅读了以原文或翻译形式识别出的文章。

入选标准

我们纳入了随机或半随机对照试验,试验中因胎龄低于34周、出生体重低于1500克或呼吸衰竭而被确定有IVH风险的早产儿接受了苯巴比妥治疗。还需要通过超声或CT充分确定IVH。

数据收集与分析

除了患者选择和偏倚控制的细节外,我们提取了苯巴比妥给药的细节。我们搜索了以下终点:IVH(分级)、出血后脑室扩张或脑积水、神经发育障碍和死亡。此外,我们搜索了苯巴比妥可能的不良反应,例如低血压、机械通气、气胸、高碳酸血症和酸中毒。

主要结果

我们纳入了12项对照试验,共招募了982名婴儿。IVH结局在各试验之间存在异质性,三项试验发现接受苯巴比妥治疗的组中IVH显著减少,一项试验发现该组中IVH增加。荟萃分析显示,苯巴比妥治疗组与对照组在所有IVH(典型风险比(RR)0.91;95%置信区间0.77至1.08)、重度IVH(典型RR 0.77;95%置信区间0.58至1.04)、出血后脑室扩张(典型RR 0.89;95%置信区间0.38至2.08)、重度神经发育障碍(典型RR 1.44;95%置信区间0.41至5.04)或出院前死亡(典型RR 0.88;95%置信区间0.64至1.21)方面均无差异。在试验中,苯巴比妥治疗组使用机械通气的趋势一致增加,荟萃分析支持这一点(典型RR 1.18;95%置信区间1.06至1.32;典型风险差值0.129;95%置信区间0.04至0.21),但气胸、酸中毒或高碳酸血症方面无显著差异。

作者结论

出生后给予苯巴比妥不能作为预防早产儿IVH的药物推荐,并且与机械通气需求增加相关。

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