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Altered expression of claudin family proteins in Alzheimer’s disease and vascular dementia brains

机译:克劳丁家族蛋白在阿尔茨海默氏病和血管性痴呆脑中的表达改变

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摘要

Claudins (Cls) are a multigene family of transmembrane proteins with different tissue distribution, which have an essential role in the formation and sealing capacity of tight junctions (TJs). At the level of the blood–brain barrier (BBB), TJs are the main molecular structures which separate the neuronal milieu from the circulatory space, by a restriction of the paracellular flow of water, ions and larger molecules into the brain. Different studies suggested recently significant BBB alterations in both vascular and degenerative dementia types. In a previous study we found in Alzheimer’s disease (AD) and vascular dementia (VaD) brains an altered expression of occludin, a molecular partner of Cls in the TJs structure. Therefore in this study, using an immunohistochemical approach, we investigated the expression of Cl family proteins (Cl-2, Cl-5 and Cl-11) in frontal cortex of aged control, AD and VaD brains. To estimate the number of Cl-expressing cells, we applied a random systematic sampling and the unbiased optical fractionator method. We found selected neurons, astrocytes, oligodendrocytes and endothelial cells expressing Cl-2, Cl-5 and Cl-11 at detectable levels in all cases studied. We report a significant increase in ratio of neurons expressing Cl-2, Cl-5 and Cl-11 in both AD and VaD as compared to aged controls. The ratio of astrocytes expressing Cl-2 and Cl-11 was significantly higher in AD and VaD as compared to aged controls. The ratio of oligodendrocytes expressing Cl-11 was significantly higher in AD and the ratio of oligodendrocytes expressing Cl-2 was significantly higher in VaD as compared to aged controls. Within the cerebral cortex, Cls were selectively expressed by pyramidal neurons, which are the ones responsible for cognitive processes and affected by AD pathology. Our findings suggest a new function of Cl family proteins which might be linked to response to cellular stress.
机译:Claudins(Cls)是跨膜蛋白的多基因家族,具有不同的组织分布,在紧密连接(TJs)的形成和密封能力中起着至关重要的作用。在血脑屏障(BBB)水平上,TJ是通过限制水,离子和较大分子进入细胞的旁细胞流动而将神经元环境与循环空间分开的主要分子结构。不同的研究表明,最近血管性和变性性痴呆类型的血脑屏障明显改变。在先前的研究中,我们发现阿尔茨海默氏病(AD)和血管性痴呆(VaD)脑中的occludin(TJs结构中Cls的分子伴侣)的表达发生了改变。因此,在这项研究中,我们使用免疫组织化学方法,研究了老年控制,AD和VaD脑额叶皮层中Cl家族蛋白(Cl-2,Cl-5和Cl-11)的表达。为了估计表达Cl的细胞的数量,我们应用了随机系统采样和无偏光学分馏器方法。我们发现在所有研究的案例中,选定的神经元,星形胶质细胞,少突胶质细胞和内皮细胞均以可检测的水平表达Cl-2,Cl-5和Cl-11。我们报道与老年对照组相比,AD和VaD中表达Cl-2,Cl-5和Cl-11的神经元比率显着增加。与老年对照组相比,AD和VaD中表达Cl-2和Cl-11的星形胶质细胞比例明显更高。与老年对照组相比,在AD中,表达Cl-11的少突胶质细胞的比例显着较高,而在VaD中表达Cl-2的少突胶质细胞的比例显着较高。在大脑皮层中,Cls由锥体神经元选择性表达,锥体神经元是负责认知过程并受AD病理影响的神经元。我们的发现表明,C1家族蛋白的新功能可能与细胞应激反应有关。

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