新生儿白质损伤的“多重打击”模型:慢性胎盘炎症、急性胎儿炎症和产后炎症事件的累积作用
A "multi-hit" model of neonatal white matter injury: cumulative contributions of chronic placental inflammation, acute fetal inflammation and postnatal inflammatory events.
作者信息
Korzeniewski Steven J, Romero Roberto, Cortez Josepf, Pappas Athina, Schwartz Alyse G, Kim Chong Jai, Kim Jung-Sun, Kim Yeon Mee, Yoon Bo Hyun, Chaiworapongsa Tinnakorn, Hassan Sonia S
出版信息
J Perinat Med. 2014 Nov;42(6):731-43. doi: 10.1515/jpm-2014-0250.
OBJECTIVE
We sought to determine whether cumulative evidence of perinatal inflammation was associated with increased risk in a "multi-hit" model of neonatal white matter injury (WMI).
METHODS
This retrospective cohort study included very preterm (gestational ages at delivery <32 weeks) live-born singleton neonates delivered at Hutzel Women's Hospital, Detroit, MI, from 2006 to 2011. Four pathologists blinded to clinical diagnoses and outcomes performed histological examinations according to standardized protocols. Neurosonography was obtained per routine clinical care. The primary indicator of WMI was ventriculomegaly (VE). Neonatal inflammation-initiating illnesses included bacteremia, surgical necrotizing enterocolitis, other infections, and those requiring mechanical ventilation.
RESULTS
A total of 425 live-born singleton neonates delivered before the 32nd week of gestation were included. Newborns delivered of pregnancies affected by chronic chorioamnionitis who had histologic evidence of an acute fetal inflammatory response were at increased risk of VE, unlike those without funisitis, relative to referent newborns without either condition, adjusting for gestational age [odds ratio (OR) 4.7; 95% confidence interval (CI) 1.4-15.8 vs. OR 1.3; 95% CI 0.7-2.6]. Similarly, newborns with funisitis who developed neonatal inflammation-initiating illness were at increased risk of VE, unlike those who did not develop such illness, compared to the referent group without either condition [OR 3.6 (95% CI 1.5-8.3) vs. OR 1.7 (95% CI 0.5-5.5)]. The greater the number of these three types of inflammation documented, the higher the risk of VE (P<0.0001).
CONCLUSION
Chronic placental inflammation, acute fetal inflammation, and neonatal inflammation-initiating illness seem to interact in contributing risk information and/or directly damaging the developing brain of newborns delivered very preterm.
目的
我们试图确定围产期炎症的累积证据是否与新生儿白质损伤(WMI)“多重打击”模型中的风险增加相关。
方法
这项回顾性队列研究纳入了2006年至2011年在密歇根州底特律市胡茨尔妇女医院出生的极早产(分娩时孕周<32周)单胎活产新生儿。四位对临床诊断和结局不知情的病理学家按照标准化方案进行组织学检查。根据常规临床护理进行神经超声检查。WMI的主要指标是脑室扩大(VE)。引发新生儿炎症的疾病包括菌血症、外科坏死性小肠结肠炎、其他感染以及需要机械通气的疾病。
结果
共纳入425例孕周在32周前出生的单胎活产新生儿。与无脐带炎且无上述两种情况的参照新生儿相比,患有慢性绒毛膜羊膜炎且有急性胎儿炎症反应组织学证据的孕妇所分娩的新生儿发生VE的风险增加,校正孕周后[比值比(OR)4.7;95%置信区间(CI)1.4 - 15.8,相比之下OR 1.3;95% CI 0.7 - 2.6]。同样,与未发生此类疾病的新生儿相比,患有脐带炎且发生引发新生儿炎症疾病的新生儿发生VE的风险增加,与无上述两种情况的参照组相比[OR 3.6(95% CI 1.5 - 8.3),相比之下OR 1.7(95% CI 0.5 - 5.5)]。记录到的这三种炎症类型的数量越多,VE风险越高(P<0.0001)。
结论
慢性胎盘炎症、急性胎儿炎症和引发新生儿炎症的疾病似乎相互作用,共同增加风险信息和/或直接损害极早产新生儿正在发育的大脑。
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