Immune cell trafficking across the blood-brain barrier in the absence and presence of neuroinflammation.

Vascular biology (Bristol, England) Pub Date : 2020-03-20 eCollection Date: 2020-01-01 DOI:10.1530/VB-19-0033
Luca Marchetti, Britta Engelhardt
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引用次数: 100

Abstract

To maintain the homeostatic environment required for proper function of CNS neurons the endothelial cells of CNS microvessels tightly regulate the movement of ions and molecules between the blood and the CNS. The unique properties of these blood vascular endothelial cells are termed blood-brain barrier (BBB) and extend to regulating immune cell trafficking into the immune privileged CNS during health and disease. In general, extravasation of circulating immune cells is a multi-step process regulated by the sequential interaction of adhesion and signalling molecules between the endothelial cells and the immune cells. Accounting for the unique barrier properties of CNS microvessels, immune cell migration across the BBB is distinct and characterized by several adaptations. Here we describe the mechanisms that regulate immune cell trafficking across the BBB during immune surveillance and neuroinflammation, with a focus on the current state-of-the-art in vitro and in vivo imaging observations.

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在没有或存在神经炎症的情况下,免疫细胞通过血脑屏障运输。
为了维持中枢神经系统神经元正常功能所需的稳态环境,中枢神经系统微血管内皮细胞严格调节血液和中枢神经系统之间离子和分子的运动。这些血管内皮细胞的独特特性被称为血脑屏障(BBB),并扩展到调节免疫细胞在健康和疾病期间进入免疫特权中枢神经系统的运输。一般来说,循环免疫细胞的外渗是一个多步骤的过程,由内皮细胞和免疫细胞之间的粘附和信号分子的连续相互作用调节。考虑到中枢神经系统微血管独特的屏障特性,免疫细胞跨血脑屏障的迁移是明显的,并以几种适应为特征。在这里,我们描述了在免疫监视和神经炎症期间调节免疫细胞在血脑屏障上运输的机制,重点是目前最先进的体外和体内成像观察。
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