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Altered fetal growth, placental abnormalities, and stillbirth

BACKGROUND: Worldwide, stillbirth is one of the leading causes of death. Altered fetal growth and placental abnormalities are the strongest and most prevalent known risk factors for stillbirth. The aim of this study was to identify patterns of association between placental abnormalities, fetal growt...

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Autores principales: Bukowski, Radek, Hansen, Nellie I., Pinar, Halit, Willinger, Marian, Reddy, Uma M., Parker, Corette B., Silver, Robert M., Dudley, Donald J., Stoll, Barbara J., Saade, George R., Koch, Matthew A., Hogue, Carol, Varner, Michael W., Conway, Deborah L., Coustan, Donald, Goldenberg, Robert L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5562325/
https://www.ncbi.nlm.nih.gov/pubmed/28820889
http://dx.doi.org/10.1371/journal.pone.0182874
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author Bukowski, Radek
Hansen, Nellie I.
Pinar, Halit
Willinger, Marian
Reddy, Uma M.
Parker, Corette B.
Silver, Robert M.
Dudley, Donald J.
Stoll, Barbara J.
Saade, George R.
Koch, Matthew A.
Hogue, Carol
Varner, Michael W.
Conway, Deborah L.
Coustan, Donald
Goldenberg, Robert L.
author_facet Bukowski, Radek
Hansen, Nellie I.
Pinar, Halit
Willinger, Marian
Reddy, Uma M.
Parker, Corette B.
Silver, Robert M.
Dudley, Donald J.
Stoll, Barbara J.
Saade, George R.
Koch, Matthew A.
Hogue, Carol
Varner, Michael W.
Conway, Deborah L.
Coustan, Donald
Goldenberg, Robert L.
author_sort Bukowski, Radek
collection PubMed
description BACKGROUND: Worldwide, stillbirth is one of the leading causes of death. Altered fetal growth and placental abnormalities are the strongest and most prevalent known risk factors for stillbirth. The aim of this study was to identify patterns of association between placental abnormalities, fetal growth, and stillbirth. METHODS AND FINDINGS: Population-based case-control study of all stillbirths and a representative sample of live births in 59 hospitals in 5 geographic areas in the U.S. Fetal growth abnormalities were categorized as small (<10th percentile) and large (>90th percentile) for gestational age at death (stillbirth) or delivery (live birth) using a published algorithm. Placental examination by perinatal pathologists was performed using a standardized protocol. Data were weighted to account for the sampling design. Among 319 singleton stillbirths and 1119 singleton live births at ≥24 weeks at death or delivery respectively, 25 placental findings were investigated. Fifteen findings were significantly associated with stillbirth. Ten of the 15 were also associated with fetal growth abnormalities (single umbilical artery; velamentous insertion; terminal villous immaturity; retroplacental hematoma; parenchymal infarction; intraparenchymal thrombus; avascular villi; placental edema; placental weight; ratio birth weight/placental weight) while 5 of the 15 associated with stillbirth were not associated with fetal growth abnormalities (acute chorioamnionitis of placental membranes; acute chorioamionitis of chorionic plate; chorionic plate vascular degenerative changes; perivillous, intervillous fibrin, fibrinoid deposition; fetal vascular thrombi in the chorionic plate). Five patterns were observed: placental findings associated with (1) stillbirth but not fetal growth abnormalities; (2) fetal growth abnormalities in stillbirths only; (3) fetal growth abnormalities in live births only; (4) fetal growth abnormalities in stillbirths and live births in a similar manner; (5) a different pattern of fetal growth abnormalities in stillbirths and live births. CONCLUSIONS: The patterns of association between placental abnormalities, fetal growth, and stillbirth provide insights into the mechanism of impaired placental function and stillbirth. They also suggest implications for clinical care, especially for placental findings amenable to prenatal diagnosis using ultrasound that may be associated with term stillbirths.
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spelling pubmed-55623252017-08-25 Altered fetal growth, placental abnormalities, and stillbirth Bukowski, Radek Hansen, Nellie I. Pinar, Halit Willinger, Marian Reddy, Uma M. Parker, Corette B. Silver, Robert M. Dudley, Donald J. Stoll, Barbara J. Saade, George R. Koch, Matthew A. Hogue, Carol Varner, Michael W. Conway, Deborah L. Coustan, Donald Goldenberg, Robert L. PLoS One Research Article BACKGROUND: Worldwide, stillbirth is one of the leading causes of death. Altered fetal growth and placental abnormalities are the strongest and most prevalent known risk factors for stillbirth. The aim of this study was to identify patterns of association between placental abnormalities, fetal growth, and stillbirth. METHODS AND FINDINGS: Population-based case-control study of all stillbirths and a representative sample of live births in 59 hospitals in 5 geographic areas in the U.S. Fetal growth abnormalities were categorized as small (<10th percentile) and large (>90th percentile) for gestational age at death (stillbirth) or delivery (live birth) using a published algorithm. Placental examination by perinatal pathologists was performed using a standardized protocol. Data were weighted to account for the sampling design. Among 319 singleton stillbirths and 1119 singleton live births at ≥24 weeks at death or delivery respectively, 25 placental findings were investigated. Fifteen findings were significantly associated with stillbirth. Ten of the 15 were also associated with fetal growth abnormalities (single umbilical artery; velamentous insertion; terminal villous immaturity; retroplacental hematoma; parenchymal infarction; intraparenchymal thrombus; avascular villi; placental edema; placental weight; ratio birth weight/placental weight) while 5 of the 15 associated with stillbirth were not associated with fetal growth abnormalities (acute chorioamnionitis of placental membranes; acute chorioamionitis of chorionic plate; chorionic plate vascular degenerative changes; perivillous, intervillous fibrin, fibrinoid deposition; fetal vascular thrombi in the chorionic plate). Five patterns were observed: placental findings associated with (1) stillbirth but not fetal growth abnormalities; (2) fetal growth abnormalities in stillbirths only; (3) fetal growth abnormalities in live births only; (4) fetal growth abnormalities in stillbirths and live births in a similar manner; (5) a different pattern of fetal growth abnormalities in stillbirths and live births. CONCLUSIONS: The patterns of association between placental abnormalities, fetal growth, and stillbirth provide insights into the mechanism of impaired placental function and stillbirth. They also suggest implications for clinical care, especially for placental findings amenable to prenatal diagnosis using ultrasound that may be associated with term stillbirths. Public Library of Science 2017-08-18 /pmc/articles/PMC5562325/ /pubmed/28820889 http://dx.doi.org/10.1371/journal.pone.0182874 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 (https://creativecommons.org/publicdomain/zero/1.0/) public domain dedication.
spellingShingle Research Article
Bukowski, Radek
Hansen, Nellie I.
Pinar, Halit
Willinger, Marian
Reddy, Uma M.
Parker, Corette B.
Silver, Robert M.
Dudley, Donald J.
Stoll, Barbara J.
Saade, George R.
Koch, Matthew A.
Hogue, Carol
Varner, Michael W.
Conway, Deborah L.
Coustan, Donald
Goldenberg, Robert L.
Altered fetal growth, placental abnormalities, and stillbirth
title Altered fetal growth, placental abnormalities, and stillbirth
title_full Altered fetal growth, placental abnormalities, and stillbirth
title_fullStr Altered fetal growth, placental abnormalities, and stillbirth
title_full_unstemmed Altered fetal growth, placental abnormalities, and stillbirth
title_short Altered fetal growth, placental abnormalities, and stillbirth
title_sort altered fetal growth, placental abnormalities, and stillbirth
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5562325/
https://www.ncbi.nlm.nih.gov/pubmed/28820889
http://dx.doi.org/10.1371/journal.pone.0182874
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