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Dynamic Changes in Endothelial Cell Adhesion Molecule Nepmucin/CD300LG Expression under Physiological and Pathological Conditions

机译:生理和病理条件下内皮细胞粘附分子Nepmucin / CD300LG表达的动态变化

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摘要

Vascular endothelial cells often change their phenotype to adapt to their local microenvironment. Here we report that the vascular endothelial adhesion molecule nepmucin/CD300LG, which is implicated in lymphocyte binding and transmigration, shows unique expression patterns in the microvascular endothelial cells of different tissues. Under physiological conditions, nepmucin/CD300LG was constitutively and selectively expressed at the luminal surface of the small arterioles, venules, and capillaries of most tissues, but it was only weakly expressed in the microvessels of the splenic red pulp and thymic medulla. Furthermore, it was barely detectable in immunologically privileged sites such as the brain, testis, and uterus. The nepmucin/CD300LG expression rapidly decreased in lymph nodes receiving acute inflammatory signals, and this loss was mediated at least in part by TNF-α. It was also down-regulated in tumors and tumor-draining lymph nodes, indicating that nepmucin/CD300LG expression is negatively regulated by locally produced signals under these circumstances. In contrast, nepmucin/CD300LG was induced in the high endothelial venule-like blood vessels of chronically inflamed pancreatic islets in an animal model of non-obese diabetes. Interestingly, the activated CD4+ T cells infiltrating the inflamed pancreas expressed high levels of the nepmucin/CD300LG ligand(s), supporting the idea that nepmucin/CD300LG and its ligand interactions are locally involved in pathological T cell trafficking. Taken together, these observations indicate that the nepmucin/CD300LG expression in microvascular endothelial cells is influenced by factor(s) that are locally produced in tissues, and that its expression is closely correlated with the level of leukocyte infiltration in certain tissues.
机译:血管内皮细胞经常改变其表型以适应其局部微环境。在这里我们报道血管内皮粘附分子nepmucin / CD300LG,与淋巴细胞的结合和迁移有关,在不同组织的微血管内皮细胞中表现出独特的表达方式。在生理条件下,nepmucin / CD300LG在大多数组织的小小动脉,小静脉和毛细血管的腔表面组成性和选择性表达,但在脾脏红髓和胸腺髓质的微血管中表达较弱。此外,它在大脑,睾丸和子宫等具有免疫功能的部位几乎无法检测到。在接受急性炎症信号的淋巴结中,nepmucin / CD300LG表达迅速降低,并且这种损失至少部分由TNF-α介导。在肿瘤和引流淋巴结的淋巴结中它也被下调,表明在这些情况下,nepmucin / CD300LG表达被局部产生的信号负调节。相反,在非肥胖型糖尿病动物模型中,nepmucin / CD300LG在慢性发炎的胰岛的高内皮小静脉样血管中被诱导。有趣的是,渗透到发炎胰腺的活化的CD4 + T细胞表达了高水平的nepmucin / CD300LG配体,支持了nepmucin / CD300LG及其配体相互作用局部参与病理性T细胞的想法贩运综上所述,这些观察结果表明,微血管内皮细胞中的nepmucin / CD300LG表达受组织中局部产生的因子的影响,并且其表达与某些组织中白细胞浸润的水平密切相关。

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