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Antenatal Betamethasone for Women at Risk for Late Preterm Delivery.对有晚期早产风险的女性使用产前倍他米松。
N Engl J Med. 2016 Apr 7;374(14):1311-20. doi: 10.1056/NEJMoa1516783. Epub 2016 Feb 4.
2
Antenatal Corticosteroids for Reducing Adverse Maternal and Child Outcomes in Special Populations of Women at Risk of Imminent Preterm Birth: A Systematic Review and Meta-Analysis.产前使用皮质类固醇以降低即将早产的高危特殊人群中母婴不良结局的系统评价和荟萃分析
PLoS One. 2016 Feb 3;11(2):e0147604. doi: 10.1371/journal.pone.0147604. eCollection 2016.
3
Repeat doses of prenatal corticosteroids for women at risk of preterm birth for improving neonatal health outcomes.对有早产风险的妇女重复使用产前皮质类固醇以改善新生儿健康结局。
Cochrane Database Syst Rev. 2015 Jul 5;2015(7):CD003935. doi: 10.1002/14651858.CD003935.pub4.
4
A population-based, multifaceted strategy to implement antenatal corticosteroid treatment versus standard care for the reduction of neonatal mortality due to preterm birth in low-income and middle-income countries: the ACT cluster-randomised trial.一项基于人群的、多方面的策略,旨在实施产前皮质类固醇治疗与标准护理,以降低低收入和中等收入国家因早产导致的新生儿死亡率:ACT 整群随机试验。
Lancet. 2015 Feb 14;385(9968):629-639. doi: 10.1016/S0140-6736(14)61651-2. Epub 2014 Oct 15.
5
Extreme caution is needed before scale-up of antenatal corticosteroids to reduce preterm deaths in low-income settings.在低收入地区扩大使用产前皮质类固醇以减少早产死亡之前,需要极其谨慎。
Lancet Glob Health. 2014 Apr;2(4):e191-2. doi: 10.1016/S2214-109X(14)70020-8. Epub 2014 Mar 13.
6
Different corticosteroids and regimens for accelerating fetal lung maturation for women at risk of preterm birth.不同皮质类固醇及方案对早产风险女性加速胎儿肺成熟的作用
Cochrane Database Syst Rev. 2013 Aug 29(8):CD006764. doi: 10.1002/14651858.CD006764.pub3.
7
Dosage regimen of antenatal steroids prior to preterm delivery and effects on maternal and neonatal outcomes.早产前产前类固醇的给药方案及其对孕产妇和新生儿结局的影响。
J Matern Fetal Neonatal Med. 2013 Feb;26(3):237-41. doi: 10.3109/14767058.2012.733758. Epub 2012 Oct 18.
8
A clinical randomized trial on endocervical inflammatory cytokines and betamethasone in prime-gravid pregnant women at risk of preterm labor.一项关于宫颈内炎性细胞因子与倍他米松对有早产风险的初产妇的临床随机试验。
Iran J Immunol. 2012 Sep;9(3):199-207.
9
Antenatal corticosteroids trial in preterm births to increase neonatal survival in developing countries: study protocol.产前皮质类固醇治疗早产儿以提高发展中国家新生儿存活率的试验:研究方案。
Reprod Health. 2012 Sep 19;9:22. doi: 10.1186/1742-4755-9-22.
10
Betamethasone dosing interval: 12 or 24 hours apart? A randomized, noninferiority open trial.倍他米松给药间隔:12 小时还是 24 小时?一项随机、非劣效性开放试验。
Am J Obstet Gynecol. 2012 Mar;206(3):201.e1-11. doi: 10.1016/j.ajog.2012.01.025.

用于加速早产风险女性胎儿肺成熟的产前皮质类固醇。

Antenatal corticosteroids for accelerating fetal lung maturation for women at risk of preterm birth.

作者信息

Roberts Devender, Brown Julie, Medley Nancy, Dalziel Stuart R

机构信息

Obstetrics Directorate, Liverpool Women's NHS Foundation Trust, Crown Street, Liverpool, Merseyside, UK, L8 7SS.

Liggins Institute, The University of Auckland, Park Rd, Grafton, Auckland, New Zealand, 1142.

出版信息

Cochrane Database Syst Rev. 2017 Mar 21;3(3):CD004454. doi: 10.1002/14651858.CD004454.pub3.

DOI:10.1002/14651858.CD004454.pub3
PMID:28321847
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6464568/
Abstract

BACKGROUND

Respiratory morbidity including respiratory distress syndrome (RDS) is a serious complication of preterm birth and the primary cause of early neonatal mortality and disability. While researching the effects of the steroid dexamethasone on premature parturition in fetal sheep in 1969, Liggins found that there was some inflation of the lungs of lambs born at gestations at which the lungs would be expected to be airless. Liggins and Howie published the first randomised controlled trial in humans in 1972 and many others followed.

OBJECTIVES

To assess the effects of administering a course of corticosteroids to the mother prior to anticipated preterm birth on fetal and neonatal morbidity and mortality, maternal mortality and morbidity, and on the child in later life.

SEARCH METHODS

We searched Cochrane Pregnancy and Childbirth's Trials Register (17 February 2016) and reference lists of retrieved studies.

SELECTION CRITERIA

We considered all randomised controlled comparisons of antenatal corticosteroid administration (betamethasone, dexamethasone, or hydrocortisone) with placebo, or with no treatment, given to women with a singleton or multiple pregnancy, prior to anticipated preterm delivery (elective, or following spontaneous labour), regardless of other co-morbidity, for inclusion in this review. Most women in this review received a single course of steroids; however, nine of the included trials allowed for women to have weekly repeats.

DATA COLLECTION AND ANALYSIS

Two review authors independently assessed trials for inclusion and risk of bias, extracted data and checked them for accuracy. The quality of the evidence was assessed using the GRADE approach.

MAIN RESULTS

This update includes 30 studies (7774 women and 8158 infants). Most studies are of low or unclear risk for most bias domains. An assessment of high risk usually meant a trial had potential for performance bias due to lack of blinding. Two trials had low risks of bias for all risk of bias domains.Treatment with antenatal corticosteroids (compared with placebo or no treatment) is associated with a reduction in the most serious adverse outcomes related to prematurity, including: perinatal death (average risk ratio (RR) 0.72, 95% confidence interval (CI) 0.58 to 0.89; participants = 6729; studies = 15; Tau² = 0.05, I² = 34%; moderate-quality); neonatal death (RR 0.69, 95% CI 0.59 to 0.81; participants = 7188; studies = 22), RDS (average RR 0.66, 95% CI 0.56 to 0.77; participants = 7764; studies = 28; Tau² = 0.06, I² = 48%; moderate-quality); moderate/severe RDS (average RR 0.59, 95% CI 0.38 to 0.91; participants = 1686; studies = 6; Tau² = 0.14, I² = 52%); intraventricular haemorrhage (IVH) (average RR 0.55, 95% CI 0.40 to 0.76; participants = 6093; studies = 16; Tau² = 0.10, I² = 33%; moderate-quality), necrotising enterocolitis (RR 0.50, 95% CI 0.32 to 0.78; participants = 4702; studies = 10); need for mechanical ventilation (RR 0.68, 95% CI 0.56 to 0.84; participants = 1368; studies = 9); and systemic infections in the first 48 hours of life (RR 0.60, 95% CI 0.41 to 0.88; participants = 1753; studies = 8).There was no obvious benefit for: chronic lung disease (average RR 0.86, 95% CI 0.42 to 1.79; participants = 818; studies = 6; Tau² = 0.38 I² = 65%); mean birthweight (g) (MD -18.47, 95% CI -40.83 to 3.90; participants = 6182; studies = 16; moderate-quality); death in childhood (RR 0.68, 95% CI 0.36 to 1.27; participants = 1010; studies = 4); neurodevelopment delay in childhood (RR 0.64, 95% CI 0.14 to 2.98; participants = 82; studies = 1); or death into adulthood (RR 1.00, 95% CI 0.56 to 1.81; participants = 988; studies = 1).Treatment with antenatal corticosteroids does not increase the risk of chorioamnionitis (RR 0.83, 95% CI 0.66 to 1.06; participants = 5546; studies = 15; moderate-quality evidence) or endometritis (RR 1.20, 95% CI 0.87 to 1.63; participants = 4030; studies = 10; Tau² = 0.11, I² = 28%; moderate-quality). No increased risk in maternal death was observed. However, the data on maternal death is based on data from a single trial with two deaths; four other trials reporting maternal death had zero events (participants = 3392; studies = 5; moderate-quality).There is no definitive evidence to suggest that antenatal corticosteroids work differently in any pre-specified subgroups (singleton versus multiple pregnancy; membrane status; presence of hypertension) or for different study protocols (type of corticosteroid; single course or weekly repeats).GRADE outcomes were downgraded to moderate-quality. Downgrading decisions (for perinatal death, RDS, IVH, and mean birthweight) were due to limitations in study design or concerns regarding precision (chorioamnionitis, endometritis). Maternal death was downgraded for imprecision due to few events.

AUTHORS' CONCLUSIONS: Evidence from this update supports the continued use of a single course of antenatal corticosteroids to accelerate fetal lung maturation in women at risk of preterm birth. A single course of antenatal corticosteroids could be considered routine for preterm delivery. It is important to note that most of the evidence comes from high income countries and hospital settings; therefore, the results may not be applicable to low-resource settings with high rates of infections.There is little need for further trials of a single course of antenatal corticosteroids versus placebo in singleton pregnancies in higher income countries and hospital settings. However, data are sparse in lower income settings. There are also few data regarding risks and benefits of antenatal corticosteroids in multiple pregnancies and other high-risk obstetric groups. Further information is also required concerning the optimal dose-to-delivery interval, and the optimal corticosteroid to use.We encourage authors of previous studies to provide further information, which may answer any remaining questions about the use of antenatal corticosteroids in such pregnancies without the need for further randomised controlled trials. Individual patient data meta-analysis from published trials is likely to answer some of the evidence gaps. Follow-up studies into childhood and adulthood, particularly in the late preterm gestation and repeat courses groups, are needed. We have not examined the possible harmful effects of antenatal corticosteroids in low-resource settings in this review. It would be particularly relevant to explore this finding in adequately powered prospective trials.

摘要

背景

包括呼吸窘迫综合征(RDS)在内的呼吸道疾病是早产的严重并发症,也是早期新生儿死亡和残疾的主要原因。1969年,利金斯在研究类固醇地塞米松对胎羊早产的影响时发现,在预期肺部无空气的孕周出生的羔羊肺部有一定程度的充气。利金斯和豪伊于1972年发表了第一项人类随机对照试验,随后还有许多其他试验。

目的

评估在预期早产前给母亲使用一个疗程的皮质类固醇对胎儿和新生儿发病率及死亡率、母亲死亡率和发病率以及儿童后期生活的影响。

检索方法

我们检索了Cochrane妊娠与分娩试验注册库(2016年2月17日)以及检索到的研究的参考文献列表。

选择标准

我们纳入了所有将产前皮质类固醇(倍他米松、地塞米松或氢化可的松)与安慰剂或不治疗进行随机对照比较的研究,这些研究针对的是单胎或多胎妊娠的妇女,在预期早产(选择性早产或自然分娩后)前进行,无论是否存在其他合并症。本综述中的大多数妇女接受了一个疗程的类固醇治疗;然而,纳入的9项试验允许妇女每周重复用药。

数据收集与分析

两位综述作者独立评估试验是否纳入及偏倚风险,提取数据并检查其准确性。使用GRADE方法评估证据质量。

主要结果

本次更新纳入30项研究(7774名妇女和8158名婴儿)。大多数研究在大多数偏倚领域的风险较低或不明确。高风险评估通常意味着试验因缺乏盲法而存在执行偏倚的可能性。两项试验在所有偏倚风险领域的偏倚风险较低。产前使用皮质类固醇治疗(与安慰剂或不治疗相比)与早产相关的最严重不良结局的减少有关,包括:围产期死亡(平均风险比(RR)0.72,95%置信区间(CI)0.58至0.89;参与者 = 6729;研究 = 15;Tau² = 0.05,I² = 34%;中等质量);新生儿死亡(RR 0.69,95%CI 0.59至0.81;参与者 = 7188;研究 = 22),RDS(平均RR 0.66,95%CI 0.56至0.77;参与者 = 7764;研究 = 28;Tau² = 0.06,I² = 48%;中等质量);中度/重度RDS(平均RR 0.59,95%CI 0.38至0.91;参与者 = 1686;研究 = 6;Tau² = 0.14,I² = 52%);脑室内出血(IVH)(平均RR 0.55,95%CI 0.40至0.76;参与者 = 6093;研究 = 16;Tau² = 0.10,I² = 33%;中等质量),坏死性小肠结肠炎(RR 0.50,95%CI 0.32至0.78;参与者 = 4702;研究 = 10);需要机械通气(RR 0.68,95%CI 0.56至0.84;参与者 = 1368;研究 = 9);以及出生后48小时内的全身感染(RR 0.60,95%CI 0.41至0.88;参与者 = 1753;研究 = 8)。对于以下情况没有明显益处:慢性肺病(平均RR 0.86,95%CI 0.42至1.79;参与者 = 818;研究 = 6;Tau² = 0.38,I² = 65%);平均出生体重(克)(MD -18.47,95%CI -40.83至3.90;参与者 = 6182;研究 = 16;中等质量);儿童期死亡(RR 0.68,95%CI 0.36至1.27;参与者 = 1010;研究 = 4);儿童期神经发育延迟(RR 0.64,95%CI 0.14至2.98;参与者 = 82;研究 = 1);或成年期死亡(RR = 1.00,95%CI 0.56至1.81;参与者 = 988;研究 = 1)。产前使用皮质类固醇治疗不会增加绒毛膜羊膜炎(RR 0.83,95%CI 0.66至1.06;参与者 = 5546;研究 = 15;中等质量证据)或子宫内膜炎(RR 1.20,95%CI 0.87至1.63;参与者 = 4030;研究 = 10;Tau² = 0.11,I² = 28%;中等质量)的风险。未观察到母亲死亡风险增加。然而,关于母亲死亡的数据基于一项有两例死亡的单一试验的数据;其他四项报告母亲死亡的试验事件数为零(参与者 = 3392;研究 = 5;中等质量)。没有确凿证据表明产前皮质类固醇在任何预先指定的亚组(单胎与多胎妊娠;胎膜状况;是否存在高血压)或不同的研究方案(皮质类固醇类型;单疗程或每周重复)中有不同的作用。GRADE结局被降级为中等质量。降级决定(针对围产期死亡、RDS、IVH和平均出生体重)是由于研究设计的局限性或对精确性的担忧(绒毛膜羊膜炎、子宫内膜炎)。母亲死亡因事件数少而被降级为精确性不足。

作者结论

本次更新的证据支持继续使用一个疗程的产前皮质类固醇来加速有早产风险妇女的胎儿肺成熟。一个疗程的产前皮质类固醇可被视为早产分娩的常规治疗。需要注意的是,大多数证据来自高收入国家和医院环境;因此,结果可能不适用于感染率高的资源匮乏地区。在高收入国家和医院环境中,单胎妊娠中进一步比较一个疗程的产前皮质类固醇与安慰剂的试验几乎没有必要。然而,低收入地区的数据稀少。关于产前皮质类固醇在多胎妊娠和其他高危产科群体中的风险和益处的数据也很少。还需要关于最佳给药至分娩间隔以及最佳皮质类固醇使用的进一步信息。我们鼓励以前研究的作者提供更多信息,这可能无需进一步的随机对照试验就能回答关于此类妊娠中使用产前皮质类固醇的任何剩余问题。对已发表试验的个体患者数据进行荟萃分析可能会回答一些证据空白。需要对儿童期和成年期进行随访研究,特别是在晚期早产和重复疗程组中。在本综述中,我们未研究产前皮质类固醇在资源匮乏地区可能的有害影响。在有足够样本量的前瞻性试验中探索这一发现将尤为相关。