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Neuronal and astrocytic interactions modulate brain endothelial properties during metabolic stresses of in vitro cerebral ischemia

机译:在体外脑缺血的代谢应激过程中神经元和星形细胞相互作用调节脑内皮功能。

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摘要

Neurovascular and gliovascular interactions significantly affect endothelial phenotype. Physiologically, brain endothelium attains several of its properties by its intimate association with neurons and astrocytes. However, during cerebrovascular pathologies such as cerebral ischemia, the uncoupling of neurovascular and gliovascular units can result in several phenotypical changes in brain endothelium. The role of neurovascular and gliovascular uncoupling in modulating brain endothelial properties during cerebral ischemia is not clear. Specifically, the roles of metabolic stresses involved in cerebral ischemia, including aglycemia, hypoxia and combined aglycemia and hypoxia (oxygen glucose deprivation and re-oxygenation, OGDR) in modulating neurovascular and gliovascular interactions are not known. The complex intimate interactions in neurovascular and gliovascular units are highly difficult to recapitulate in vitro. However, in the present study, we used a 3D co-culture model of brain endothelium with neurons and astrocytes in vitro reflecting an intimate neurovascular and gliovascular interactions in vivo. While the cellular signaling interactions in neurovascular and gliovascular units in vivo are much more complex than the 3D co-culture models in vitro, we were still able to observe several important phenotypical changes in brain endothelial properties by metabolically stressed neurons and astrocytes including changes in barrier, lymphocyte adhesive properties, endothelial cell adhesion molecule expression and in vitro angiogenic potential.
机译:神经血管和胶质血管的相互作用显着影响内皮表型。从生理学上讲,脑内皮细胞通过与神经元和星形胶质细胞紧密结合而获得其某些特性。然而,在诸如脑缺血之类的脑血管病理过程中,神经血管和胶质血管单位的解偶联会导致脑内皮细胞发生一些表型改变。神经血管和胶质细胞解偶联在调节脑缺血期间脑内皮特性中的作用尚不清楚。具体而言,尚不清楚与脑缺血有关的代谢应激在调节神经血管和神经胶质血管相互作用中的作用,包括血糖过低,缺氧以及合并的血糖过低和缺氧(氧葡萄糖剥夺和再充氧,OGDR)。神经血管和神经胶质血管单位中复杂的紧密相互作用在体外很难概括。但是,在本研究中,我们在体外使用了脑内皮细胞与神经元和星形胶质细胞的3D共培养模型,反映了体内亲密的神经血管和胶质血管相互作用。尽管体内神经血管和胶质血管单位中的细胞信号相互作用比体外3D共培养模型复杂得多,但我们仍然能够通过代谢应激神经元和星形胶质细胞观察到脑内皮特性的一些重要表型变化,包括屏障的变化,淋巴细胞粘附特性,内皮细胞粘附分子表达和体外血管生成潜力。

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