Placental vascular alterations are associated with early neurodevelopmental and pulmonary impairment in the rabbit fetal growth restriction model

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作者
Ignacio Valenzuela
David Basurto
Yannick Regin
Andre Gie
Lennart van der Veeken
Simen Vergote
Emma Muñoz-Moreno
Bartosz Leszczynski
Birger Tielemans
Greetje Vande Velde
Jan Deprest
Johannes van der Merwe
机构
[1] KU Leuven,Department of Development and Regeneration, Cluster Woman and Child, Group Biomedical Sciences
[2] Stellenbosch University and Tygerberg Hospital,Department of Paediatrics and Child Health, Faculty of Medicine and Health Sciences
[3] Institut d’Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS),Magnetic Resonance Imaging Core Facility
[4] Jagiellonian University,Department of Medical Physics, Marian Smoluchowski Institute of Physics, Faculty of Physics, Astronomy and Applied Computer Science
[5] Department of Imaging and Pathology,Biomedical MRI/MoSAIC, Faculty of Medicine
[6] University Hospitals Leuven,Department of Obstetrics and Gynecology, Division Woman and Child
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摘要
Fetal growth restriction is one of the leading causes of perinatal mortality and morbidity and has consequences that extend well beyond the neonatal period. Current management relies on timely delivery rather than improving placental function. Several prenatal strategies have failed to show benefit in clinical trials after promising results in animal models. Most of these animal models have important developmental and structural differences compared to the human and/or are insufficiently characterized. We aimed to describe placental function and structure in an FGR rabbit model, and to characterize the early brain and lung developmental morbidity using a multimodal approach. FGR was induced in time-mated rabbits at gestational day 25 by partial uteroplacental vessel ligation in one horn. Umbilical artery Doppler was measured before caesarean delivery at gestational day 30, and placentas were harvested for computed microtomography and histology. Neonates underwent neurobehavioral or pulmonary functional assessment the day after delivery, followed by brain or lung harvesting, respectively. Neuropathological assessment included multiregional quantification of neuron density, apoptosis, astrogliosis, cellular proliferation, and oligodendrocyte progenitors. Brain region volumes and diffusion metrics were obtained from ex-vivo brain magnetic resonance imaging. Lung assessment included biomechanical tests and pulmonary histology. Fetal growth restriction was associated with labyrinth alterations in the placenta, driven by fetal capillary reduction, and overall reduced vessels volume. FGR caused altered neurobehavior paralleled by regional neuropathological deficits and reduced fractional anisotropy in the cortex, white matter, and hippocampus. In addition, FGR kittens presented functional alterations in the peripheral lung and structurally underdeveloped alveoli. In conclusion, in a uteroplacental insufficiency FGR rabbit model, placental vascular alterations coincide with neurodevelopmental and pulmonary disruption.
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