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Foxc1突变体中的脑血管缺陷与来自脑膜的视黄酸下游异常的WNT和VEGF-A信号通路相关。

Cerebrovascular defects in Foxc1 mutants correlate with aberrant WNT and VEGF-A pathways downstream of retinoic acid from the meninges.

作者信息

Mishra Swati, Choe Youngshik, Pleasure Samuel J, Siegenthaler Julie A

机构信息

Department of Pediatrics, Section of Developmental Biology, University of Colorado, School of Medicine Aurora, CO 80045, USA.

Department of Neurology, Programs in Neuroscience and Developmental Biology, Institute for Regenerative Medicine, UC San Francisco, San Francisco, CA 94158, USA.

出版信息

Dev Biol. 2016 Dec 1;420(1):148-165. doi: 10.1016/j.ydbio.2016.09.019. Epub 2016 Sep 23.

Abstract

Growth and maturation of the cerebrovasculature is a vital event in neocortical development however mechanisms that control cerebrovascular development remain poorly understood. Mutations in or deletions that include the FOXC1 gene are associated with congenital cerebrovascular anomalies and increased stroke risk in patients. Foxc1 mutant mice display severe cerebrovascular hemorrhage at late gestational ages. While these data demonstrate Foxc1 is required for cerebrovascular development, its broad expression in the brain vasculature combined with Foxc1 mutant's complex developmental defects have made it difficult to pinpoint its function(s). Using global and conditional Foxc1 mutants, we find 1) significant cerebrovascular growth defects precede cerebral hemorrhage and 2) expression of Foxc1 in neural crest-derived meninges and brain pericytes, though not endothelial cells, is required for normal cerebrovascular development. We provide evidence that reduced levels of meninges-derived retinoic acid (RA), caused by defects in meninges formation in Foxc1 mutants, is a major contributing factor to the cerebrovascular growth defects in Foxc1 mutants. We provide data that suggests that meninges-derived RA ensures adequate growth of the neocortical vasculature via regulating expression of WNT pathway proteins and neural progenitor derived-VEGF-A. Our findings offer the first evidence for a role of the meninges in brain vascular development and provide new insight into potential causes of cerebrovascular defects in patients with FOXC1 mutations.

摘要

脑血管系统的生长和成熟是新皮质发育中的一个重要事件,然而,控制脑血管发育的机制仍知之甚少。包括FOXC1基因在内的突变或缺失与先天性脑血管异常以及患者中风风险增加有关。Foxc1突变小鼠在妊娠晚期表现出严重的脑血管出血。虽然这些数据表明Foxc1是脑血管发育所必需的,但其在脑血管系统中的广泛表达以及Foxc1突变体复杂的发育缺陷使得难以确定其功能。利用全身性和条件性Foxc1突变体,我们发现:1)在脑出血之前存在明显的脑血管生长缺陷;2)正常脑血管发育需要Foxc1在神经嵴来源的脑膜和脑周细胞中表达,而在内皮细胞中则不需要。我们提供的证据表明,Foxc1突变体中脑膜形成缺陷导致的脑膜来源视黄酸(RA)水平降低是Foxc1突变体脑血管生长缺陷的主要促成因素。我们提供的数据表明,脑膜来源的RA通过调节WNT信号通路蛋白和神经祖细胞来源的VEGF-A的表达来确保新皮质血管系统的充分生长。我们的研究结果首次证明了脑膜在脑血管发育中的作用,并为FOXC1突变患者脑血管缺陷的潜在原因提供了新的见解。

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本文引用的文献

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Diverse Functions of Retinoic Acid in Brain Vascular Development.视黄酸在脑血管发育中的多种功能
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3
Foxc1 is required for early stage telencephalic vascular development.早期端脑血管发育需要Foxc1。
Dev Dyn. 2015 May;244(5):703-11. doi: 10.1002/dvdy.24269. Epub 2015 Apr 8.
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