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宫内炎症、新生儿败血症与慢性肺病:一项为期13年的医院队列研究。

Intrauterine inflammation, neonatal sepsis, and chronic lung disease: a 13-year hospital cohort study.

作者信息

Lahra Monica M, Beeby Philip J, Jeffery Heather E

机构信息

Royal Prince Alfred Hospital, Department of Neonatal Medicine, Missenden Road, Camperdown, New South Wales 2050, Australia.

出版信息

Pediatrics. 2009 May;123(5):1314-9. doi: 10.1542/peds.2008-0656.

Abstract

UNLABELLED

OBJECTIVE To determine the impact of intrauterine inflammation of maternal (chorioamnionitis) and fetal (umbilical vasculitis) origin and neonatal sepsis on the development of neonatal chronic lung disease in preterm infants.

METHODS

This study was conducted at Royal Prince Alfred Hospital in Sydney, Australia. All infants born at <30 weeks' gestation, admitted to the NICU, and surviving to 36 weeks' corrected gestation during 1992-2004 were eligible. Infants with major congenital abnormalities and those without placental examination were excluded. Antenatal and perinatal data extracted from hospital databases were correlated with the independent, central neonatal database and diagnostic laboratory reports. Neonatal sepsis was categorized according to blood culture isolates into 3 groups: coagulase-negative staphylococci, other bacteria, and Candida species.

RESULTS

There were 798 eligible infants born during the study period, and 761 (95.4%) had placental examination. The mean gestational age was 27.4 +/- 1.5 weeks. Antenatal maternal steroids were given to 94.4%. Regression analysis showed that chorioamnionitis with umbilical vasculitis and increasing gestation were associated with reduced odds of chronic lung disease. Chorioamnionitis without umbilical vasculitis showed a trend to reduced odds of chronic lung disease. Birth weight at <3rd percentile and neonatal sepsis were associated with increased odds of chronic lung disease.

CONCLUSIONS

A fetal inflammatory response is protective for chronic lung disease. Neonatal sepsis is strongly associated with chronic lung disease, and the infecting organism is important. Coagulase-negative staphylococcal infection confers a risk for chronic lung disease similar to that of other bacteremias. Candidemia confers the greatest risk of chronic lung disease.

摘要

未标注

目的 确定源于母体(绒毛膜羊膜炎)和胎儿(脐血管炎)的宫内炎症以及新生儿败血症对早产儿慢性肺病发展的影响。

方法

本研究在澳大利亚悉尼的皇家阿尔弗雷德王子医院进行。纳入所有在1992年至2004年期间孕30周前出生、入住新生儿重症监护病房且存活至矫正孕周36周的婴儿。排除有重大先天性异常的婴儿以及未进行胎盘检查的婴儿。从医院数据库提取的产前和围产期数据与独立的中央新生儿数据库及诊断实验室报告进行关联。根据血培养分离菌将新生儿败血症分为3组:凝固酶阴性葡萄球菌、其他细菌和念珠菌属。

结果

研究期间有798名符合条件的婴儿出生,其中761名(95.4%)进行了胎盘检查。平均孕周为27.4±1.5周。94.4%的产妇接受了产前类固醇治疗。回归分析显示,伴有脐血管炎的绒毛膜羊膜炎以及孕周增加与慢性肺病发生几率降低相关。不伴有脐血管炎的绒毛膜羊膜炎显示出慢性肺病发生几率降低的趋势。出生体重低于第3百分位数和新生儿败血症与慢性肺病发生几率增加相关。

结论

胎儿炎症反应对慢性肺病具有保护作用。新生儿败血症与慢性肺病密切相关,感染病原体很重要。凝固酶阴性葡萄球菌感染导致慢性肺病的风险与其他菌血症相似。念珠菌血症导致慢性肺病的风险最大。

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