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神经胶质细胞对人类血脑屏障的影响。

Glial cell influence on the human blood-brain barrier.

作者信息

Prat A, Biernacki K, Wosik K, Antel J P

机构信息

Neuroimmunology unit, Montréal Neurological Institute, McGill University, Montréal, Québec, Canada.

出版信息

Glia. 2001 Nov;36(2):145-55. doi: 10.1002/glia.1104.

DOI:10.1002/glia.1104
PMID:11596123
Abstract

The blood-brain barrier (BBB) is a specialized structure of the central nervous system (CNS) that restricts immune cell migration and soluble molecule diffusion from the systemic compartment into the CNS. Astrocytes and microglia are resident cells of the CNS that contribute to the formation of the BBB. In this article, we consider the influence of these glial cells on the immune regulatory functions of the microvascular endothelium, with special emphasis on the human BBB. A series of in vitro studies demonstrate that soluble factors produced by glial cells, under basal culture conditions, help restrict development of inflammation within the CNS. These soluble factor effects include upregulating expression of molecules including HT7, UEA-1 lectin-binding sites, and angiotensin receptors that help define the phenotype of endothelial cells. These factors also induce tight junction formation between brain endothelial cells, contributing to the restricted permeability of the BBB. In contrast, these factors have little effect on expression of molecules by ECs that either promote lymphocyte migration, such as chemokines and adhesion molecules or molecules that are required for competent antigen presentation, such as MHC and co-stimulatory molecules. Glial cells that become activated in response to signals derived from the immune system or generated within the CNS, produce an array of inflammatory molecules that increase permeability and promote lymphocyte trafficking and persistence. These observations emphasize the bidirectional nature of neural-immune interactions; this dynamic system should be amenable to therapeutic interventions.

摘要

血脑屏障(BBB)是中枢神经系统(CNS)的一种特殊结构,它限制免疫细胞迁移以及可溶性分子从全身循环进入中枢神经系统。星形胶质细胞和小胶质细胞是中枢神经系统的驻留细胞,它们对血脑屏障的形成有作用。在本文中,我们探讨这些胶质细胞对微血管内皮细胞免疫调节功能的影响,特别关注人类血脑屏障。一系列体外研究表明,在基础培养条件下,胶质细胞产生的可溶性因子有助于限制中枢神经系统内炎症的发展。这些可溶性因子的作用包括上调包括HT7、UEA - 1凝集素结合位点和血管紧张素受体等分子的表达(这些分子有助于确定内皮细胞的表型)。这些因子还诱导脑内皮细胞之间紧密连接的形成,从而导致血脑屏障的通透性受限。相比之下,这些因子对内皮细胞表达那些促进淋巴细胞迁移的分子(如趋化因子和黏附分子)或对抗抗原呈递所必需的分子(如MHC和共刺激分子)影响很小。响应来自免疫系统或中枢神经系统内产生的信号而被激活的胶质细胞会产生一系列炎症分子,这些分子会增加通透性并促进淋巴细胞运输和滞留。这些观察结果强调了神经免疫相互作用的双向性;这个动态系统应该适合进行治疗干预。

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