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星形胶质细胞和周细胞在发育和缺氧损伤过程中对血脑屏障特性的调节存在差异。

Astrocytes and pericytes differentially modulate blood-brain barrier characteristics during development and hypoxic insult.

作者信息

Al Ahmad Abraham, Taboada Carole Bürgi, Gassmann Max, Ogunshola Omolara O

机构信息

Institute of Veterinary Physiology, Vetsuisse Faculty, University of Zürich, Zürich, Switzerland.

出版信息

J Cereb Blood Flow Metab. 2011 Feb;31(2):693-705. doi: 10.1038/jcbfm.2010.148. Epub 2010 Sep 8.

Abstract

Understanding regulation of blood-brain barrier (BBB) is crucial to reduce/prevent its disruption during injury. As high brain complexity makes interpretation of in vivo data challenging, BBB studies are frequently performed using simplified in vitro models. However, many models fail to address the three-dimensional (3D) cellular interactions that occur in vivo, an important feature that may explain discrepancies in translation of in vitro data to the in vivo situation. We have designed and characterized an innovative 3D model that reproduces morphological and functional characteristics of the BBB in vivo and used it to investigate cellular interactions and contribution of astrocytes and pericytes to BBB development. Our model shows that both astrocytes and pericytes significantly suppress endothelial proliferation. In contrast, differential effects on tubulogenesis were observed with astrocytes reducing the number of tubes formed but increasing diameters and length, whereas pericytes had the opposite effect. Pericytes also induce proper localization of barrier proteins, lumen polarization, and functional activity of ATP-binding cassette (ABC) transporters similar to astrocytes, but the presence of both cells is required to maintain optimal barrier characteristics during hypoxic exposure. This model is simple, dynamic, and convenient to study many aspects of BBB function and represents an exciting new tool to address open questions of BBB regulation.

摘要

了解血脑屏障(BBB)的调控对于减少/预防损伤期间其破坏至关重要。由于大脑高度复杂,使得体内数据的解读具有挑战性,因此血脑屏障研究经常使用简化的体外模型进行。然而,许多模型未能解决体内发生的三维(3D)细胞相互作用,这一重要特征可能解释了体外数据转化为体内情况时出现差异的原因。我们设计并表征了一种创新的3D模型,该模型再现了体内血脑屏障的形态和功能特征,并用于研究星形胶质细胞和周细胞对血脑屏障发育的细胞相互作用及贡献。我们的模型表明,星形胶质细胞和周细胞均能显著抑制内皮细胞增殖。相比之下,观察到对血管生成有不同影响,星形胶质细胞减少形成的血管数量,但增加血管直径和长度,而周细胞则有相反的作用。周细胞还能诱导屏障蛋白的正确定位、管腔极化以及ATP结合盒(ABC)转运蛋白的功能活性,类似于星形胶质细胞,但在缺氧暴露期间需要两种细胞同时存在才能维持最佳的屏障特征。该模型简单、动态且便于研究血脑屏障功能的许多方面,是解决血脑屏障调控未解决问题的一种令人兴奋的新工具。

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