Ethanol Gestational Exposure Impairs Vascular Development and Endothelial Potential to Control BBB-Associated Astrocyte Function in the Developing Cerebral Cortex

Ethanol consumption during pregnancy or lactation period can induce permanent damage to the development of the central nervous system (CNS), resulting in fetal alcohol spectrum disorders (FASD). CNS development depends on proper neural cells and blood vessel (BV) development and blood-brain barrier...

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Veröffentlicht in:	Molecular neurobiology 2021-04, Vol.58 (4), p.1755-1768
Hauptverfasser:	Siqueira, Michele, Araujo, Ana Paula Bérgamo, Gomes, Flávia Carvalho Alcantara, Stipursky, Joice
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Schlagworte:	Angiogenesis Animals Animals, Newborn Astrocytes Astrocytes - pathology Biomedical and Life Sciences Biomedicine Blood Vessels - embryology Blood-brain barrier Blood-Brain Barrier - pathology Cell Biology Central nervous system Cerebral cortex Cerebral Cortex - embryology Connexin 43 Endothelial cells Endothelial Cells - metabolism Endothelial Cells - pathology Ethanol Ethanol - adverse effects Female Fetal Alcohol Spectrum Disorders - pathology Fetal alcohol syndrome Gene Expression Profiling Gene Expression Regulation Glial fibrillary acidic protein Humans IL-1β Inflammation Interleukin 1 Interleukin 6 Lactation Lipocalin Mice Neovascularization, Physiologic Neurobiology Neurology Neurosciences NF-κB protein Nitric oxide Phenotype Phenotypes Pregnancy Prenatal Exposure Delayed Effects - pathology Tumor necrosis factor Zonula occludens-1 protein
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creator	Siqueira, Michele Araujo, Ana Paula Bérgamo Gomes, Flávia Carvalho Alcantara Stipursky, Joice
description	Ethanol consumption during pregnancy or lactation period can induce permanent damage to the development of the central nervous system (CNS), resulting in fetal alcohol spectrum disorders (FASD). CNS development depends on proper neural cells and blood vessel (BV) development and blood-brain barrier (BBB) establishment; however, little is known about how ethanol affects these events. Here, we investigated the impact of ethanol exposure to endothelial cells (ECs) function and to ECs interaction with astrocytes in the context of BBB establishment. Cerebral cortex of newborn mice exposed in utero to ethanol (FASD model) presented a hypervascularized phenotype, revealed by augmented vessel density, length, and branch points. Further, aberrant distribution of the tight junction ZO-1 protein along BVs and increased rates of perivascular astrocytic endfeet around BVs were observed. In vitro exposure of human brain microcapillary ECs (HBMEC) to ethanol significantly disrupted ZO-1 distribution, decreased Claudin-5 and GLUT-1 expression and impaired glucose uptake, and increased nitric oxide secretion. These events were accompanied by upregulation of angiogenesis-related secreted proteins by ECs in response to ethanol exposure. Treatment of cortical astrocytes with conditioned medium (CM) from ethanol exposed ECs, upregulated astrocyte’s expression of GFAP, Cx43, and Lipocalin-2 genes, as well as the pro-inflammatory genes, IL-1beta, IL-6, and TNF-alpha, which was accompanied by NF-kappa B protein nuclear accumulation. Our findings suggest that ethanol triggers a dysfunctional phenotype in brain ECs, leading to impairment of cortical vascular network formation, and promotes ECs-induced astrocyte dysfunction, which could dramatically affect BBB establishment in the developing brain.
doi_str_mv	10.1007/s12035-020-02214-8
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These events were accompanied by upregulation of angiogenesis-related secreted proteins by ECs in response to ethanol exposure. Treatment of cortical astrocytes with conditioned medium (CM) from ethanol exposed ECs, upregulated astrocyte’s expression of GFAP, Cx43, and Lipocalin-2 genes, as well as the pro-inflammatory genes, IL-1beta, IL-6, and TNF-alpha, which was accompanied by NF-kappa B protein nuclear accumulation. 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CNS development depends on proper neural cells and blood vessel (BV) development and blood-brain barrier (BBB) establishment; however, little is known about how ethanol affects these events. Here, we investigated the impact of ethanol exposure to endothelial cells (ECs) function and to ECs interaction with astrocytes in the context of BBB establishment. Cerebral cortex of newborn mice exposed in utero to ethanol (FASD model) presented a hypervascularized phenotype, revealed by augmented vessel density, length, and branch points. Further, aberrant distribution of the tight junction ZO-1 protein along BVs and increased rates of perivascular astrocytic endfeet around BVs were observed. In vitro exposure of human brain microcapillary ECs (HBMEC) to ethanol significantly disrupted ZO-1 distribution, decreased Claudin-5 and GLUT-1 expression and impaired glucose uptake, and increased nitric oxide secretion. These events were accompanied by upregulation of angiogenesis-related secreted proteins by ECs in response to ethanol exposure. Treatment of cortical astrocytes with conditioned medium (CM) from ethanol exposed ECs, upregulated astrocyte’s expression of GFAP, Cx43, and Lipocalin-2 genes, as well as the pro-inflammatory genes, IL-1beta, IL-6, and TNF-alpha, which was accompanied by NF-kappa B protein nuclear accumulation. Our findings suggest that ethanol triggers a dysfunctional phenotype in brain ECs, leading to impairment of cortical vascular network formation, and promotes ECs-induced astrocyte dysfunction, which could dramatically affect BBB establishment in the developing brain.</description><subject>Angiogenesis</subject><subject>Animals</subject><subject>Animals, Newborn</subject><subject>Astrocytes</subject><subject>Astrocytes - pathology</subject><subject>Biomedical and Life Sciences</subject><subject>Biomedicine</subject><subject>Blood Vessels - embryology</subject><subject>Blood-brain barrier</subject><subject>Blood-Brain Barrier - pathology</subject><subject>Cell Biology</subject><subject>Central nervous system</subject><subject>Cerebral cortex</subject><subject>Cerebral Cortex - embryology</subject><subject>Connexin 43</subject><subject>Endothelial cells</subject><subject>Endothelial Cells - metabolism</subject><subject>Endothelial Cells - pathology</subject><subject>Ethanol</subject><subject>Ethanol - 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CNS development depends on proper neural cells and blood vessel (BV) development and blood-brain barrier (BBB) establishment; however, little is known about how ethanol affects these events. Here, we investigated the impact of ethanol exposure to endothelial cells (ECs) function and to ECs interaction with astrocytes in the context of BBB establishment. Cerebral cortex of newborn mice exposed in utero to ethanol (FASD model) presented a hypervascularized phenotype, revealed by augmented vessel density, length, and branch points. Further, aberrant distribution of the tight junction ZO-1 protein along BVs and increased rates of perivascular astrocytic endfeet around BVs were observed. In vitro exposure of human brain microcapillary ECs (HBMEC) to ethanol significantly disrupted ZO-1 distribution, decreased Claudin-5 and GLUT-1 expression and impaired glucose uptake, and increased nitric oxide secretion. 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subjects	Angiogenesis Animals Animals, Newborn Astrocytes Astrocytes - pathology Biomedical and Life Sciences Biomedicine Blood Vessels - embryology Blood-brain barrier Blood-Brain Barrier - pathology Cell Biology Central nervous system Cerebral cortex Cerebral Cortex - embryology Connexin 43 Endothelial cells Endothelial Cells - metabolism Endothelial Cells - pathology Ethanol Ethanol - adverse effects Female Fetal Alcohol Spectrum Disorders - pathology Fetal alcohol syndrome Gene Expression Profiling Gene Expression Regulation Glial fibrillary acidic protein Humans IL-1β Inflammation Interleukin 1 Interleukin 6 Lactation Lipocalin Mice Neovascularization, Physiologic Neurobiology Neurology Neurosciences NF-κB protein Nitric oxide Phenotype Phenotypes Pregnancy Prenatal Exposure Delayed Effects - pathology Tumor necrosis factor Zonula occludens-1 protein
title	Ethanol Gestational Exposure Impairs Vascular Development and Endothelial Potential to Control BBB-Associated Astrocyte Function in the Developing Cerebral Cortex
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