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Maternal Pravastatin Prevents Altered Fetal Brain Development in a Preeclamptic CD-1 Mouse Model

OBJECTIVE: Using an animal model, we have previously shown that preeclampsia results in long-term adverse neuromotor outcomes in the offspring, and this phenotype was prevented by antenatal treatment with pravastatin. This study aims to localize the altered neuromotor programming in this animal mode...

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Autores principales: Carver, Alissa R., Andrikopoulou, Maria, Lei, Jun, Tamayo, Esther, Gamble, Phyllis, Hou, Zhipeng, Zhang, Jiangyang, Mori, Susumu, Saade, George R., Costantine, Maged M., Burd, Irina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4071009/
https://www.ncbi.nlm.nih.gov/pubmed/24963809
http://dx.doi.org/10.1371/journal.pone.0100873
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author Carver, Alissa R.
Andrikopoulou, Maria
Lei, Jun
Tamayo, Esther
Gamble, Phyllis
Hou, Zhipeng
Zhang, Jiangyang
Mori, Susumu
Saade, George R.
Costantine, Maged M.
Burd, Irina
author_facet Carver, Alissa R.
Andrikopoulou, Maria
Lei, Jun
Tamayo, Esther
Gamble, Phyllis
Hou, Zhipeng
Zhang, Jiangyang
Mori, Susumu
Saade, George R.
Costantine, Maged M.
Burd, Irina
author_sort Carver, Alissa R.
collection PubMed
description OBJECTIVE: Using an animal model, we have previously shown that preeclampsia results in long-term adverse neuromotor outcomes in the offspring, and this phenotype was prevented by antenatal treatment with pravastatin. This study aims to localize the altered neuromotor programming in this animal model and to evaluate the role of pravastatin in its prevention. MATERIALS AND METHODS: For the preeclampsia model, pregnant CD-1 mice were randomly allocated to injection of adenovirus carrying sFlt-1 or its control virus carrying mFc into the tail vein. Thereafter they received pravastatin (sFlt-1-pra “experimental group”) or water (sFlt-1 “positive control”) until weaning. The mFc group (“negative control”) received water. Offspring at 6 months of age were sacrificed, and whole brains underwent magnetic resonance imaging (MRI). MRIs were performed using an 11.7 Tesla vertical bore MRI scanner. T2 weighted images were acquired to evaluate the volumes of 28 regions of interest, including areas involved in adaptation and motor, spatial and sensory function. Cytochemistry and cell quantification was performed using neuron-specific Nissl stain. One-way ANOVA with multiple comparison testing was used for statistical analysis. RESULTS: Compared with control offspring, male sFlt-1 offspring have decreased volumes in the fimbria, periaquaductal gray, stria medullaris, and ventricles and increased volumes in the lateral globus pallidus and neocortex; however, female sFlt-1 offspring showed increased volumes in the ventricles, stria medullaris, and fasciculus retroflexus and decreased volumes in the inferior colliculus, thalamus, and lateral globus pallidus. Neuronal quantification via Nissl staining exhibited decreased cell counts in sFlt-1 offspring neocortex, more pronounced in males. Prenatal pravastatin treatment prevented these changes. CONCLUSION: Preeclampsia alters brain development in sex-specific patterns, and prenatal pravastatin therapy prevents altered neuroanatomic programming in this animal model.
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spelling pubmed-40710092014-06-27 Maternal Pravastatin Prevents Altered Fetal Brain Development in a Preeclamptic CD-1 Mouse Model Carver, Alissa R. Andrikopoulou, Maria Lei, Jun Tamayo, Esther Gamble, Phyllis Hou, Zhipeng Zhang, Jiangyang Mori, Susumu Saade, George R. Costantine, Maged M. Burd, Irina PLoS One Research Article OBJECTIVE: Using an animal model, we have previously shown that preeclampsia results in long-term adverse neuromotor outcomes in the offspring, and this phenotype was prevented by antenatal treatment with pravastatin. This study aims to localize the altered neuromotor programming in this animal model and to evaluate the role of pravastatin in its prevention. MATERIALS AND METHODS: For the preeclampsia model, pregnant CD-1 mice were randomly allocated to injection of adenovirus carrying sFlt-1 or its control virus carrying mFc into the tail vein. Thereafter they received pravastatin (sFlt-1-pra “experimental group”) or water (sFlt-1 “positive control”) until weaning. The mFc group (“negative control”) received water. Offspring at 6 months of age were sacrificed, and whole brains underwent magnetic resonance imaging (MRI). MRIs were performed using an 11.7 Tesla vertical bore MRI scanner. T2 weighted images were acquired to evaluate the volumes of 28 regions of interest, including areas involved in adaptation and motor, spatial and sensory function. Cytochemistry and cell quantification was performed using neuron-specific Nissl stain. One-way ANOVA with multiple comparison testing was used for statistical analysis. RESULTS: Compared with control offspring, male sFlt-1 offspring have decreased volumes in the fimbria, periaquaductal gray, stria medullaris, and ventricles and increased volumes in the lateral globus pallidus and neocortex; however, female sFlt-1 offspring showed increased volumes in the ventricles, stria medullaris, and fasciculus retroflexus and decreased volumes in the inferior colliculus, thalamus, and lateral globus pallidus. Neuronal quantification via Nissl staining exhibited decreased cell counts in sFlt-1 offspring neocortex, more pronounced in males. Prenatal pravastatin treatment prevented these changes. CONCLUSION: Preeclampsia alters brain development in sex-specific patterns, and prenatal pravastatin therapy prevents altered neuroanatomic programming in this animal model. Public Library of Science 2014-06-25 /pmc/articles/PMC4071009/ /pubmed/24963809 http://dx.doi.org/10.1371/journal.pone.0100873 Text en © 2014 Carver et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Carver, Alissa R.
Andrikopoulou, Maria
Lei, Jun
Tamayo, Esther
Gamble, Phyllis
Hou, Zhipeng
Zhang, Jiangyang
Mori, Susumu
Saade, George R.
Costantine, Maged M.
Burd, Irina
Maternal Pravastatin Prevents Altered Fetal Brain Development in a Preeclamptic CD-1 Mouse Model
title Maternal Pravastatin Prevents Altered Fetal Brain Development in a Preeclamptic CD-1 Mouse Model
title_full Maternal Pravastatin Prevents Altered Fetal Brain Development in a Preeclamptic CD-1 Mouse Model
title_fullStr Maternal Pravastatin Prevents Altered Fetal Brain Development in a Preeclamptic CD-1 Mouse Model
title_full_unstemmed Maternal Pravastatin Prevents Altered Fetal Brain Development in a Preeclamptic CD-1 Mouse Model
title_short Maternal Pravastatin Prevents Altered Fetal Brain Development in a Preeclamptic CD-1 Mouse Model
title_sort maternal pravastatin prevents altered fetal brain development in a preeclamptic cd-1 mouse model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4071009/
https://www.ncbi.nlm.nih.gov/pubmed/24963809
http://dx.doi.org/10.1371/journal.pone.0100873
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