Barrington Keith J, Finer Neil
Department of Pediatrics, CHU Ste-Justine, 3175 Cote Ste Catherine, Montreal, Quebec, Canada, H3T 1C5.
Cochrane Database Syst Rev. 2010 Dec 8(12):CD000509. doi: 10.1002/14651858.CD000509.pub4.
Inhaled nitric oxide (iNO) is effective in term infants with hypoxic respiratory failure. The pathophysiology of respiratory failure and the potential risks of iNO differ substantially in preterm infants, necessitating study in this population.
To determine the effect of treatment with iNO on death, bronchopulmonary dysplasia (BPD), intraventricular hemorrhage (IVH), and neurodevelopmental disability in preterm newborn infants with respiratory disease.
Standard methods of the Cochrane Neonatal Review Group were used. MEDLINE, EMBASE, Healthstar and the Cochrane Central Register of Controlled Trials (The Cochrane Library) were searched covering the years from 1985 to 2010. In addition, the abstracts of the Pediatric Academic Societies were also searched.
Randomized and quasi-randomized studies in preterm infants with respiratory disease that compared the effects of iNO gas to control, with or without placebo were eligible.
Standard methods of the Cochrane Neonatal Review Group were used.
Fourteen randomized controlled trials of inhaled nitric oxide therapy in preterm infants were found. The trials have been grouped post hoc into three categories depending on entry criteria; entry in the first three days of life based on oxygenation criteria, routine use in preterm babies with pulmonary disease, and later enrolment based on an increased risk of BPD. No overall analyses were performed.Nine trials of early rescue treatment of infants based on oxygenation criteria demonstrated no significant effect of iNO on mortality or BPD. Three studies with routine use of iNO in infants with pulmonary disease also demonstrated no significant reduction in death or BPD [typical RR 0.93 (95% CI 0.86 to 1.01)] although this small effect approached significance. Later treatment with iNO based on the risk of BPD (two trials) demonstrated no significant benefit for this outcome in analyses which are possible using summary data.There is no clear effect of iNO on the frequency of all grades of IVH or of severe IVH. Early rescue treatment was associated with a non-significant 20% increase in severe IVH.No effect on the incidence of neurodevelopmental impairment was found.
AUTHORS' CONCLUSIONS: iNO as rescue therapy for the very ill preterm infant does not appear to be effective. Early routine use of iNO in preterm infants with respiratory disease does not affect serious brain injury or improve survival without BPD. Later use of iNO to prevent BPD might be effective, but requires further study.
吸入一氧化氮(iNO)对足月低氧性呼吸衰竭婴儿有效。呼吸衰竭的病理生理学及iNO的潜在风险在早产儿中差异很大,因此有必要在该人群中进行研究。
确定iNO治疗对患有呼吸系统疾病的早产新生儿死亡、支气管肺发育不良(BPD)、脑室内出血(IVH)及神经发育障碍的影响。
采用Cochrane新生儿回顾组的标准方法。检索了MEDLINE、EMBASE、Healthstar及Cochrane对照试验中心注册库(Cochrane图书馆),涵盖1985年至2010年的文献。此外,还检索了儿科学术协会的摘要。
符合条件的研究为对患有呼吸系统疾病的早产儿进行的随机和半随机研究,比较了iNO气体与对照(有或无安慰剂)的效果。
采用Cochrane新生儿回顾组的标准方法。
共发现14项关于早产儿吸入一氧化氮治疗的随机对照试验。根据纳入标准,这些试验事后被分为三类:根据氧合标准在出生后前三天纳入、对患有肺部疾病的早产儿常规使用、基于BPD风险增加的后期纳入。未进行总体分析。9项基于氧合标准对婴儿进行早期抢救治疗的试验表明,iNO对死亡率或BPD无显著影响。3项对患有肺部疾病的婴儿常规使用iNO的研究也表明,死亡或BPD没有显著降低[典型相对危险度0.93(95%可信区间0.86至1.01)],尽管这种微小影响接近显著水平。基于BPD风险的后期iNO治疗(两项试验)在使用汇总数据进行的分析中,未显示出对该结果有显著益处。iNO对所有级别IVH或重度IVH的发生率没有明显影响。早期抢救治疗与重度IVH增加20%但无统计学意义相关。未发现对神经发育障碍发生率有影响。
iNO作为病情极重的早产儿的抢救治疗似乎无效。对患有呼吸系统疾病的早产儿早期常规使用iNO不会影响严重脑损伤,也不会提高无BPD的生存率。后期使用iNO预防BPD可能有效,但需要进一步研究。
