首页> 外文期刊>Biological & pharmaceutical bulletin >Selective Protein Expression Changes of Leukocyte-Migration-Associated Cluster of Differentiation Antigens at the Blood-Brain Barrier in a Lipopolysaccharide-Induced Systemic Inflammation Mouse Model without Alteration of Transporters, Receptors or Tight Junction-Related Protein
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Selective Protein Expression Changes of Leukocyte-Migration-Associated Cluster of Differentiation Antigens at the Blood-Brain Barrier in a Lipopolysaccharide-Induced Systemic Inflammation Mouse Model without Alteration of Transporters, Receptors or Tight Junction-Related Protein

机译:在脂多糖诱导的全身炎症小鼠模型中血脑屏障在血脑屏障中的白细胞迁移相关抗原簇的选择性蛋白表达变化,无需转运蛋白,受体或紧密结合相关蛋白质

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Leukocyte migration across the blood brain barrier (BBB) is an important step in the progression of brain dysfunction in systemic inflammation. The purpose of this study was to identify the key regulatory molecule(s) at the BBB among the cluster of differentiation (CD) antigens involved in leucocyte migration in lipopolysaccharide (LPS)-induced systemic inflammation based on their absolute protein expressions. Here, we identified the absolute expression levels of 17 CD antigens in isolated brain capillaries (Bcap) of LPS-administered mice. Among them, the expression levels of CD54 and CD106 were dramatically increased in LPS-administered mice compared to the control by 6.21- and 3.67-fold, respectively. In peripheral blood mononuclear cells, the expression levels of CD11a/CD18, the counter-receptor for CD54, were similar to those of CD54 in Bcap of LPS-administered mice. On the other hand, the expression level of CD49d, part of CD29/CD49d complex, which is the counter-receptor for CD106, was under the limit of quantification. It is thus likely that CD54 at the BBB is predominantly involved in promoting leukocyte migration across the BBB in systemic inflammation. The expression levels of CD9, CD49c and CD97, which are thought to be involved in cell-to-cell interaction, were decreased by 40-60% in Bcap of LPS-administered mice. In contrast, the expression levels of 9 transporters, 2 receptors, and 1 tight junction-related protein in Bcap of LPS-administered mice were essentially unchanged compared to the control. These results suggest that enhancement of leucocyte migration in systemic inflammation involves dynamic changes of CD antigens without alterations of other major functional molecules.
机译:白细胞迁移穿过血脑屏障(BBB)是全身炎症脑功能障碍进展的重要一步。本研究的目的是鉴定基于其绝对蛋白表达的脂多糖(LPS)诱导的全身炎症的白细胞迁移的分化(CD)抗原簇中BBB的关键调节分子。在这里,我们鉴定了LPS施用小鼠的分离脑毛细血管(BCAP)中的17个CD抗原的绝对表达水平。其中,与对照分别在6.21-和3.67倍的对照相比,在LPS施用的小鼠中,CD54和CD106的表达水平显着增加。在外周血单核细胞中,CD11A / CD18,CD54的反应受体的表达水平与LPS给药小鼠的BCAP中的CD54的表达水平类似。另一方面,CD49D的表达水平,CD29 / CD49D复合物的一部分是CD106的反受体,在定量的限度下。因此,BBB的CD54可能主要涉及在全身炎症中促进穿过BBB的白细胞迁移。被认为参与细胞对细胞相互作用的CD9,CD49C和CD97的表达水平在LPS施用小鼠的BCAP中降低了40-60%。相反,与对照相比,LPS施用的小鼠的BCAP中,9转运物,2个受体和1个紧密结合相关蛋白的表达水平基本不变。这些结果表明,增强全身炎症中的白细胞迁移涉及CD抗原的动态变化,而不改变其他主要功能分子。

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