Vascular Contributions to the Neurobiological Effects of Prenatal Alcohol Exposure.

Sarah Z Momin, Jacqueline T Le, Rajesh C Miranda
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Abstract

Background: Fetal alcohol spectrum disorders (FASD) are often characterized as a cluster of brain-based disabilities. Though cardiovascular effects of prenatal alcohol exposure (PAE) have been documented, the vascular deficits due to PAE are less understood, but may contribute substantially to the severity of neurobehavioral presentation and health outcomes in persons with FASD. Methods: We conducted a systematic review of research articles curated in PubMed to assess the strength of the research on vascular effects of PAE. 40 pertinent papers were selected, covering studies in both human populations and animal models. Results: Studies in human populations identified cardiac defects, and defects in vasculature, including increased tortuosity, defects in basement membranes, capillary basal hyperplasia, endarteritis, and disorganized and diminished cerebral vasculature due to PAE. Preclinical studies showed that PAE rapidly and persistently results in vasodilation of large afferent cerebral arteries, but to vasoconstriction of smaller cerebral arteries and microvasculature. Moreover, PAE continues to affect cerebral blood flow into middle-age. Human and animal studies also indicate that ocular vascular parameters may have diagnostic and predictive value. A number of intervening mechanisms were identified, including increased autophagy, inflammation and deficits in mitochondria. Studies in animals identified persistent changes in blood flow and vascular density associated with endocannabinoid, prostacyclin and nitric oxide signaling, as well as calcium mobilization. Conclusion: Although the brain has been a particular focus of studies on PAE, the cardiovascular system is equally affected. Studies in human populations, though constrained by small sample sizes, did link pathology in major blood vessels and tissue vasculature, including brain vasculature, to PAE. Animal studies highlighted molecular mechanisms that may be useful therapeutic targets. Collectively, these studies suggest that vascular pathology is a possible contributing factor to neurobehavioral and health problems across a lifespan in persons with a diagnosis of FASD. Furthermore, ocular vasculature may serve as a biomarker for neurovascular health in FASD.
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血管对产前酒精暴露的神经生物学效应的贡献。
胎儿酒精谱系障碍(FASD)通常被描述为一组基于大脑的残疾。虽然产前酒精暴露(PAE)对心血管的影响已有文献记载,但由于PAE导致的血管缺陷尚不清楚,但可能在很大程度上导致FASD患者神经行为表现的严重程度和健康结果。方法:我们对PubMed中收录的研究文章进行了系统回顾,以评估PAE血管效应研究的强度。选取了40篇相关论文,涵盖了人类和动物模型的研究。结果:对人群的研究发现了心脏缺陷和脉管系统缺陷,包括PAE引起的扭曲增加、基底膜缺陷、毛细血管基底增生、动脉内膜炎和脑组织紊乱和减少。临床前研究表明,PAE迅速而持续地导致大脑大传入动脉的血管扩张,但导致较小的大脑动脉和微血管的血管收缩。此外,PAE继续影响到中年的脑血流量。人类和动物研究也表明,眼部血管参数可能具有诊断和预测价值。许多干预机制被确定,包括增加自噬,炎症和线粒体缺陷。动物研究发现,血流和血管密度的持续变化与内源性大麻素、前列环素和一氧化氮信号以及钙动员有关。结论:尽管PAE研究的重点是大脑,但心血管系统也同样受到影响。在人群中进行的研究,虽然受到小样本量的限制,但确实将主要血管和组织血管系统(包括脑血管系统)的病理与PAE联系起来。动物研究强调了分子机制可能是有用的治疗靶点。总的来说,这些研究表明,血管病理学可能是FASD患者一生中神经行为和健康问题的一个促成因素。此外,眼血管系统可以作为FASD患者神经血管健康的生物标志物。
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