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全身性产后皮质类固醇、支气管肺发育不良与无脑瘫生存情况

Systemic Postnatal Corticosteroids, Bronchopulmonary Dysplasia, and Survival Free of Cerebral Palsy.

作者信息

Doyle Lex W, Mainzer Rheanna, Cheong Jeanie L Y

机构信息

Departments of Obstetrics, Gynaecology, and Newborn Health, the Royal Women's Hospital, University of Melbourne, Parkville, Victoria, Australia.

Newborn Research, the Royal Women's Hospital, Parkville, Victoria, Australia.

出版信息

JAMA Pediatr. 2025 Jan 1;179(1):65-72. doi: 10.1001/jamapediatrics.2024.4575.

Abstract

IMPORTANCE

Systemic postnatal corticosteroids have been shown to reduce rates of bronchopulmonary dysplasia (BPD) in infants born preterm, but both corticosteroids and BPD are associated with cerebral palsy.

OBJECTIVE

To describe how the association between systemic postnatal corticosteroids and survival free of cerebral palsy varies with the risk of BPD in infants born preterm, and if the association differs between dexamethasone and hydrocortisone, or with age at starting treatment.

DESIGN, SETTING, AND PARTICIPANTS: This comparative effectiveness research used weighted meta-regression analysis of eligible randomized clinical trials (RCTs) of systemic postnatal corticosteroids reported from June 1989 through March 2022 that included rates of all of BPD, mortality, and cerebral palsy in neonatal intensive care units in 10 countries. Infants born preterm at risk of BPD were included. Data were analyzed from April and July 2024.

INTERVENTIONS

Systemic dexamethasone or hydrocortisone.

MAIN OUTCOMES AND MEASURES

Type and timing of corticosteroid, control group rate of BPD, and risk difference in survival free of cerebral palsy between corticosteroid and control arms.

RESULTS

Twenty-six RCTs with data on 3700 randomized infants were eligible; 18 (69%) investigated dexamethasone and 8 (31%) hydrocortisone; 12 (46%) started treatment in the first week after birth. There was evidence for a differential association of the type of corticosteroid with the effect of systemic dexamethasone on survival free of cerebral palsy and the risk of BPD in control groups (interaction coefficient, 0.54; 95% CI, 0.25-0.82; P = .001). For dexamethasone, for every 10-percentage point increase in the risk of BPD, the risk difference for survival free of cerebral palsy increased by 3.74% (95% CI, 1.54 to 5.93; P = .002). Dexamethasone was associated with improved survival free of cerebral palsy at a risk of BPD greater than 70%. Conversely, dexamethasone was associated with harm at a risk of BPD less than 30%. There was some evidence for a negative association with hydrocortisone, with possible benefit with risk of BPD less than 30%. There was no strong evidence for a differential effect of timing among those treated with dexamethasone (interaction coefficient, 0.13; 95% CI, -0.04 to 0.30; P = .14).

CONCLUSIONS AND RELEVANCE

The findings suggest that dexamethasone (compared with control) was associated with improved rates of survival free of cerebral palsy in infants at high risk of BPD but should be avoided in those at low risk. A role for hydrocortisone is uncertain.

摘要

重要性

已表明全身应用产后皮质类固醇可降低早产儿支气管肺发育不良(BPD)的发生率,但皮质类固醇和BPD均与脑瘫有关。

目的

描述全身应用产后皮质类固醇与无脑瘫存活之间的关联如何随早产儿BPD风险而变化,以及地塞米松和氢化可的松之间的关联是否不同,或与开始治疗时的年龄是否有关。

设计、设置和参与者:这项比较有效性研究对1989年6月至2022年3月报告的全身应用产后皮质类固醇的合格随机临床试验(RCT)进行加权荟萃回归分析,这些试验包括10个国家新生儿重症监护病房中所有BPD、死亡率和脑瘫的发生率。纳入有BPD风险的早产儿。于2024年4月和7月进行数据分析。

干预措施

全身应用地塞米松或氢化可的松。

主要结局和指标

皮质类固醇的类型和时间、对照组BPD发生率以及皮质类固醇组与对照组无脑瘫存活的风险差异。

结果

26项RCT符合条件,涉及3700名随机分组的婴儿;18项(69%)研究地塞米松,8项(31%)研究氢化可的松;12项(46%)在出生后第一周开始治疗。有证据表明皮质类固醇类型与全身应用地塞米松对无脑瘫存活的影响以及对照组BPD风险之间存在差异关联(交互系数为0.54;95%CI为0.25 - 0.82;P = 0.001)。对于地塞米松,BPD风险每增加10个百分点,无脑瘫存活的风险差异增加3.74%(95%CI为1.54至5.93;P = 0.002)。当BPD风险大于70%时,地塞米松与无脑瘫存活改善相关。相反,当BPD风险小于30%时,地塞米松与危害相关。有一些证据表明氢化可的松存在负相关,当BPD风险小于30%时可能有益。对于接受地塞米松治疗的患者,开始治疗时间的差异效应没有有力证据(交互系数为0.13;95%CI为 - 0.04至0.30;P = 0.14)。

结论和相关性

研究结果表明,地塞米松(与对照组相比)与BPD高风险婴儿无脑瘫存活率提高相关,但低风险婴儿应避免使用。氢化可的松的作用尚不确定。

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