Placental findings in singleton stillbirths

Halit Pinar; Robert L Goldenberg; Matthew A Koch; Josefine Heim-Hall; Hal K Hawkins; Bahig Shehata; Carlos Abramowsky; Corette B Parker; Donald J Dudley; Robert M Silver; Barbara Stoll; Marshall Carpenter; George Saade; Janet Moore; Deborah Conway; Michael W Varner; Carol J R Hogue; Donald R Coustan; Elena Sbrana; Vanessa Thorsten; Marian Willinger; Uma M Reddy

doi:10.1097/AOG.0000000000000100

Placental findings in singleton stillbirths

Obstet Gynecol. 2014 Feb;123(2 Pt 1):325-336. doi: 10.1097/AOG.0000000000000100.

Affiliation

¹ The Warren Alpert Medical School of Brown University, Providence, Rhode Island; Columbia University School of Medicine, New York, New York; RTI International, Durham, North Carolina; the University of Texas Health Science Center at San Antonio, San Antonio, and the University of Texas Medical Branch, Galveston, Texas; Emory University, Atlanta, Georgia; the University of Utah School of Medicine, Salt Lake City, Utah; Tufts University Medical Center, Boston, Masachusetts; and the Eunice Kennedy Shriver National Institute of Child Health and Human Development, Bethesda, Maryland. For a list of members in the Eunice Kennedy Shriver National Institute of Child Health and Human Development Stillbirth Collaborative Research Network, see the Appendix online at http://links.lww.com/AOG/A465.

Abstract

Objective: To compare placental lesions for stillbirth cases and live birth controls in a population-based study.

Methods: Pathologic examinations were performed on placentas from singleton pregnancies using a standard protocol. Data were analyzed overall and within gestational age groups at delivery.

Results: Placentas from 518 stillbirths and 1,200 live births were studied. Single umbilical artery was present in 7.7% of stillbirths and 1.7% of live births, velamentous cord insertion was present in 5% of stillbirths and 1.1% of live births, diffuse terminal villous immaturity was present in 10.3% of stillbirths and 2.3% of live births, inflammation (eg, acute chorioamnionitis of placental membranes) was present in 30.4% of stillbirths and 12% of live births, vascular degenerative changes in chorionic plate were present in 55.7% of stillbirths and 0.5% of live births, retroplacental hematoma was present in 23.8% of stillbirths and 4.2% of live births, intraparenchymal thrombi was present in 19.7% of stillbirths and 13.3% of live births, parenchymal infarction was present in 10.9% of stillbirths and 4.4% of live births, fibrin deposition was present in 9.2% of stillbirths and 1.5% of live births, fetal vascular thrombi was present in 23% of stillbirths and 7% of live births, avascular villi was present in 7.6% of stillbirths and 2.0% of live births, and hydrops was present in 6.4% of stillbirths and 1.0% of live births. Among stillbirths, inflammation and retroplacental hematoma were more common in placentas from early deliveries, whereas thrombotic lesions were more common in later gestation. Inflammatory lesions were especially common in early live births.

Conclusions: Placental lesions were highly associated with stillbirth compared with live births. All lesions associated with stillbirth were found in live births but often with variations by gestational age at delivery. Knowledge of lesion prevalence within gestational age groups in both stillbirths and live birth controls contributes to an understanding of the association between placental abnormality and stillbirth.

Level of evidence: II.

Publication types

Comparative Study
Research Support, N.I.H., Extramural

MeSH terms

Adult
Chorioamnionitis / pathology
Chorionic Villi / pathology
Female
Fetal Death / pathology
Gestational Age
Humans
Live Birth
Placenta / abnormalities
Placenta / pathology*
Placenta Diseases / pathology*
Pregnancy
Pregnancy Complications / pathology
Single Umbilical Artery / pathology
Stillbirth*

Placental findings in singleton stillbirths

Authors

Affiliation

Abstract

Publication types

MeSH terms

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