Lee JoonHo, Romero Roberto, Lee Kyung A, Kim Eun Na, Korzeniewski Steven J, Chaemsaithong Piya, Yoon Bo Hyun
Department of Obstetrics and Gynecology, Seoul National University College of Medicine, Seoul, Republic of Korea.
Perinatology Research Branch, Eunice Kennedy Shriver National Institute of Child Health and Human Development/National Institutes of Health/US Department of Health and Human Services, Bethesda, MD, and Detroit, MI; Department of Obstetrics and Gynecology, University of Michigan, Ann Arbor, MI; Department of Epidemiology and Biostatistics, Michigan State University, East Lansing, MI; Center for Molecular Medicine and Genetics, Wayne State University, Detroit, MI.
Am J Obstet Gynecol. 2016 Mar;214(3):366.e1-9. doi: 10.1016/j.ajog.2015.10.009. Epub 2015 Oct 17.
Meconium aspiration syndrome (MAS) is a leading cause of morbidity and mortality in term infants. Meconium-stained amniotic fluid (MSAF) occurs in approximately 1 of every 7 pregnancies, but only 5% of neonates exposed to MSAF develop MAS. Why some infants exposed to meconium develop MAS while others do not is a fundamental question. Patients with MSAF have a higher frequency of intraamniotic inflammation/infection than those with clear fluid. We propose that fetal systemic inflammation is a risk factor for the development of MAS in patients with MSAF.
We sought to investigate whether intraamniotic inflammation and funisitis, the histopathologic landmark of a fetal inflammatory response, predispose to MAS.
A prospective cohort study was conducted from 1995 through 2009. Amniotic fluid (AF) samples (n = 1281) were collected at the time of cesarean delivery from women who delivered singleton newborns at term (gestational age ≥38 weeks). Intraamniotic inflammation was diagnosed if the AF concentration of matrix metalloproteinase-8 was >23 ng/mL. Funisitis was diagnosed by histologic examination if inflammation was present in the umbilical cord.
The prevalence of MSAF was 9.2% (118/1281), and 10.2% (12/118) of neonates exposed to MSAF developed MAS. There were no significant differences in the median gestational age or umbilical cord arterial pH at birth between neonates who developed MAS and those who did not (each P > .1). Mothers whose newborns developed MAS had a higher median of AF matrix metalloproteinase-8 (456.8 vs 157.2 ng/mL, P < .05). Newborns exposed to intraamniotic inflammation had a higher rate of MAS than those who were not exposed to intraamniotic inflammation [13.0% (10/77) vs 0% (0/32), P = .03], as did those exposed to funisitis [31.3% (5/16) vs 7.3% (6/82); relative risk, 4.3; 95% confidence interval, 1.5-12.3]. Among the 89 newborns for whom both AF and placental histology were available, MAS was more common in patients with both intraamniotic inflammation and funisitis than in those without intraamniotic inflammation and funisitis [28.6% (4/14) vs 0% (0/28), P = .009], while the rate of MAS did not show a significant difference between patients with intraamniotic inflammation alone (without funisitis) and those without intraamniotic inflammation and funisitis [10.9% (5/46) vs 0% (0/28)].
The combination of intraamniotic inflammation with fetal systemic inflammation is an important antecedent of MAS. This concept has implications for the understanding of the mechanisms of disease responsible for MAS and for the development of prognostic models and therapeutic interventions for this disorder.
胎粪吸入综合征(MAS)是足月儿发病和死亡的主要原因。约每7例妊娠中就有1例出现胎粪污染羊水(MSAF),但暴露于MSAF的新生儿中只有5%会发生MAS。为什么有些暴露于胎粪的婴儿会发生MAS而其他婴儿不会,这是一个根本性问题。与羊水清澈的患者相比,MSAF患者羊膜腔内炎症/感染的发生率更高。我们提出胎儿全身性炎症是MSAF患者发生MAS的一个危险因素。
我们试图研究羊膜腔内炎症和脐带炎(胎儿炎症反应的组织病理学标志)是否易导致MAS。
1995年至2009年进行了一项前瞻性队列研究。在剖宫产时,从足月(孕周≥38周)分娩单胎新生儿的妇女中收集羊水(AF)样本(n = 1281)。如果羊水基质金属蛋白酶-8浓度>23 ng/mL,则诊断为羊膜腔内炎症。如果脐带存在炎症,则通过组织学检查诊断为脐带炎。
MSAF的发生率为9.2%(118/1281),暴露于MSAF的新生儿中有10.2%(12/118)发生MAS。发生MAS的新生儿与未发生MAS的新生儿在出生时的中位孕周或脐动脉pH值方面无显著差异(P均>.1)。新生儿发生MAS的母亲,其羊水基质金属蛋白酶-8的中位数较高(456.8 vs 157.2 ng/mL,P <.05)。暴露于羊膜腔内炎症的新生儿发生MAS的比例高于未暴露于羊膜腔内炎症的新生儿[13.0%(10/77)vs 0%(0/32),P =.03],暴露于脐带炎的新生儿也是如此[31.3%(5/16)vs 7.3%(6/82);相对危险度,4.3;95%置信区间,1.5 - 12.3]。在89例同时有羊水和胎盘组织学检查结果的新生儿中,同时有羊膜腔内炎症和脐带炎的患者发生MAS比没有羊膜腔内炎症和脐带炎的患者更常见[28.6%(4/14)vs 0%(0/28),P =.009],而单纯有羊膜腔内炎症(无脐带炎)的患者与没有羊膜腔内炎症和脐带炎的患者之间MAS发生率无显著差异[10.9%(5/46)vs 0%(0/28)]。
羊膜腔内炎症与胎儿全身性炎症的联合是MAS的重要先兆。这一概念对于理解导致MAS的疾病机制以及该疾病预后模型和治疗干预措施的开发具有重要意义。