Phenotypes of maternal vascular malperfusion placental pathology and adverse pregnancy outcomes: A retrospective cohort study

Author:

Zur Rebecca L.1ORCID,McLaughlin Kelsey1,Aalto Laura2,Jiang Yidi3,Huszti Ella3,Parks W. Tony2,Kingdom John C.1

Affiliation:

1. Maternal–Fetal Medicine Division (Placenta Program), Department of Obstetrics & Gynaecology, Sinai Health System University of Toronto Toronto Ontario Canada

2. Department of Pathology and Laboratory Medicine, Sinai Health System University of Toronto Toronto Ontario Canada

3. Biostatistics Research Unit, University Health Network University of Toronto Toronto Ontario Canada

Abstract

AbstractObjectiveTo identify which components of maternal vascular malperfusion (MVM) pathology are associated with adverse pregnancy outcomes and to investigate the morphological phenotypes of MVM placental pathology and their relationship with distinct clinical presentations of pre‐eclampsia and/or fetal growth restriction (FGR).DesignRetrospective cohort study.SettingTertiary care hospital in Toronto, Canada.PopulationPregnant individuals with low circulating maternal placental growth factor (PlGF) levels (<100 pg/mL) and placental pathology analysis between March 2017 and December 2019.MethodsAssociation between each pathological finding and the outcomes of interest were calculated using the chi‐square test. Cluster analysis and logistic regression was used to identify phenotypic clusters, and their association with adverse pregnancy outcomes. Cluster analysis was performed using the K‐modes unsupervised clustering algorithm.Main outcome measuresPreterm delivery <34+0 weeks of gestation, early onset pre‐eclampsia with delivery <34+0 weeks of gestation, birthweight <10th percentile (small for gestational age, SGA) and stillbirth.ResultsThe diagnostic features of MVM most strongly associated with delivery <34+0 weeks of gestation were: infarction, accelerated villous maturation, distal villous hypoplasia and decidual vasculopathy. Two dominant phenotypic clusters of MVM pathology were identified. The largest cluster (n = 104) was characterised by both reduced placental mass and hypoxic ischaemic injury (infarction and accelerated villous maturation), and was associated with combined pre‐eclampsia and SGA. The second dominant cluster (n = 59) was characterised by infarction and accelerated villous maturation alone, and was associated with pre‐eclampsia and average birthweight for gestational age.ConclusionsPatients with placental MVM disease are at high risk of pre‐eclampsia and FGR, and distinct pathological findings correlate with different clinical phenotypes, suggestive of distinct subtypes of MVM disease.

Publisher

Wiley

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