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. 2016 Nov;101(6):F513-F519.
doi: 10.1136/archdischild-2015-308518. Epub 2016 Mar 23.

Fetal inflammation associated with minimal acute morbidity in moderate/late preterm infants

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Fetal inflammation associated with minimal acute morbidity in moderate/late preterm infants

Tate Gisslen et al. Arch Dis Child Fetal Neonatal Ed. 2016 Nov.

Abstract

Objective: To determine whether exposure to acute chorioamnionitis and fetal inflammation caused short-term adverse outcomes.

Design: This is a prospective observational study: subjects were mothers delivering at 32-36 weeks gestation and their preterm infants at a large urban tertiary level III perinatal unit (N=477 infants). Placentae and fetal membranes were scored for acute histological chorioamnionitis based on the Redline criteria. Fetal inflammation was characterised by histological diagnosis of funisitis (umbilical cord inflammation), increased cord blood cytokines measured by ELISA, and activation of the inflammatory cells infiltrating the placenta and fetal membranes measured by immunohistology. Maternal and infant data were collected.

Results: Twenty-four per cent of 32-36-week infants were exposed to histological chorioamnionitis and 6.9% had funisitis. Immunostaining for leucocyte subsets showed selective infiltration of the placenta and fetal membranes with activated neutrophils and macrophages with chorioamnionitis. Interleukin (IL) 6, IL-8 and granulocyte colony-stimulating factor were selectively increased in the cord blood of preterm infants with funisitis. Compared with infants without chorioamnionitis, funisitis was associated with increased ventilation support during resuscitation (43.8% vs 15.4%) and more respiratory distress syndrome postnatally (27.3% vs 10.2%) in univariate analysis. However, these associations disappeared after adjusting for prematurity.

Conclusions: Despite fetal exposure to funisitis, increased cord blood cytokines and activated placental inflammatory cells, we could not demonstrate neonatal morbidity specifically attributable to fetal inflammation after adjusting for gestational age in moderate and late preterm infants.

Keywords: Fetal Medicine; Immunology; Neonatology; Resuscitation.

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Conflict of interest statement

Competing interests: None declared.

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