Enhanced interaction between focal adhesion and adherens junction proteins: involvement in sphingosine 1-phosphate-induced endothelial barrier enhancement.

Sun X; Shikata Y; Wang L; Ohmori K; Watanabe N; Wada J; Shikata K; Birukov KG; Makino H; Jacobson JR; Dudek SM; Garcia JG

首页> 外文期刊>Microvascular Research: An International Journal >Enhanced interaction between focal adhesion and adherens junction proteins: involvement in sphingosine 1-phosphate-induced endothelial barrier enhancement.

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Enhanced interaction between focal adhesion and adherens junction proteins: involvement in sphingosine 1-phosphate-induced endothelial barrier enhancement.

机译：粘着斑粘附和粘附连接蛋白之间增强的相互作用：参与鞘氨醇1-磷酸诱导的内皮屏障增强。

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Sphingosine 1-phosphate (S1P) is an important vascular barrier regulatory agonist which enhances the junctional integrity of human lung endothelial cell monolayers. We have now demonstrated that S1P induced cortical actin ring formation and redistribution of focal adhesion kinase (FAK) and paxillin to the cell periphery suggesting the critical role of cell-cell adhesion in endothelial barrier enhancement. Co-immunoprecipitation studies revealed increased association of VE-cadherin with FAK and paxillin in S1P-challenged human pulmonary artery endothelial cell (HPAEC) monolayers. Furthermore, S1P-induced enhancement of VE-cadherin interaction with alpha-catenin and beta-catenin was associated with the increased formation of FAK-beta-catenin protein complexes. Depletion of beta-catenin (siRNA) resulted in loss of S1P-mediated VE-cadherin association with FAK and paxillin rearrangement. Furthermore, transendothelial electrical resistance (an index of barrier function) demonstrated that beta-catenin siRNA significantly attenuated S1P-induced barrier enhancement. These results demonstrate a mechanism of S1P-induced endothelial barrier enhancement via beta-catenin-linked adherens junction and focal adhesion interaction.

机译：1-磷酸鞘氨醇（S1P）是一种重要的血管屏障调节激动剂，可增强人肺内皮细胞单层的连接完整性。现在我们已经证明S1P诱导皮质肌动蛋白环的形成以及粘着斑激酶（FAK）和paxillin在细胞周围的重新分布，提示细胞粘附在内皮屏障增强中的关键作用。免疫共沉淀研究表明，在S1P攻击的人肺动脉内皮细胞（HPAEC）单层中，VE-钙黏着蛋白与FAK和Paxillin的关联增加。此外，S1P诱导的VE-钙粘蛋白与α-catenin和β-catenin相互作用的增强与FAK-β-catenin蛋白复合物形成的增加有关。 β-catenin（siRNA）的耗尽导致S1P介导的VE-钙粘着蛋白与FAK和paxillin重排的关联丧失。此外，跨内皮电阻（屏障功能指数）证明β-cateninsiRNA显着减弱了S1P诱导的屏障增强。这些结果证明了通过β-连环蛋白连接的粘附连接和局灶性粘附相互作用的S1P诱导内皮屏障增强的机制。

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《Microvascular Research: An International Journal》 |2009年第3期|共10页
作者
Sun X; Shikata Y; Wang L; Ohmori K; Watanabe N; Wada J; Shikata K; Birukov KG; Makino H; Jacobson JR; Dudek SM; Garcia JG;
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正文语种 eng
中图分类心脏、血管（循环系）疾病;
关键词
Adherens Junctions; Cadherins; Cell Adhesion; Cell Membrane Permeability; Cells; Cultured; Electric Impedance; Endothelium; Vascular; Focal Adhesion Protein-Tyrosine Kinases; Gene Silencing; Humans; Lysophospholipids; Paxillin; Pulmonary Artery; RNA; Small Interfering; Sphingosine; alpha Catenin; beta Catenin; *钙粘着糖蛋白类; 细胞粘附; 细胞膜渗透性; 细胞; 培养的; 电阻抗; 内皮; 血管; 溶磷脂素类; 肺动脉; 鞘氨醇;

机译：Adherens Junctions;Cadherins;Cell Adhesion;Cell Membrane Permeability;Cells;Cultured;Electric Impedance;Endothelium;Vascular;Focal Adhesion Protein-Tyrosine Kinases;Gene Silencing;Humans;Lysophospholipids;Paxillin;Pulmonary Artery;RNA;Small Interfering;Sphingosine;alpha Catenin;beta Catenin;*钙粘着糖蛋白类;细胞粘附;细胞膜渗透性;细胞;培养的;电阻抗;内皮;血管;溶磷脂素类;肺动脉;鞘氨醇;

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专利

1. Enhanced interaction between focal adhesion and adherens junction proteins: involvement in sphingosine 1-phosphate-induced endothelial barrier enhancement. [J] . Sun X, Shikata Y, Wang L, Microvascular Research: An International Journal . 2009,第3期

机译：粘着斑粘附和粘附连接蛋白之间增强的相互作用：参与鞘氨醇1-磷酸诱导的内皮屏障增强。
2. Endothelial barrier protection by FTY720 under hyperglycemic condition: involvement of focal adhesion kinase, small GTPases, and adherens junction proteins. [J] . Sarai K, Shikata K, Shikata Y American Journal of Physiology . 2009,第4aPta1期

机译：在高血糖情况下，FTY720对内皮屏障的保护：涉及粘着斑激酶，小GTP酶和粘附连接蛋白。
3. Hydroxyalkenals and oxidized phospholipids modulation of endothelial cytoskeleton, focal adhesion and adherens junction proteins in regulating endothelial barrier function [J] . UsatyukP.V., NatarajanV. Microvascular Research: An International Journal . 2012,第1期

机译：羟基烯醛和氧化磷脂调节内皮细胞骨架，粘着斑和粘附连接蛋白在调节内皮屏障功能中的作用
4. Paxillin is Required for Cyclic Stretch-Induced Orientation of Endothelial Cells by Scaffolding for Accumulation of Focal Adhesion Proteins [C] . Wenjing HUANG, Naoya SAKAMOTO, Ryotaro MIYAZAWA, Mechanical Engineering Congress . 2012

机译：通过支撑局灶性粘附蛋白的积累，患有循环拉伸诱导的内皮细胞诱导取向所必需的paxillin
5. Functional Implications of the Interaction Between the Tetraspanin CD82/KAI1 and Adherens Junction Proteins. [D] . Smith, Danielle Leigh. 2010

机译：四跨膜蛋白CD82 / KAI1和粘附连接蛋白之间相互作用的功能含义。
6. Enhanced interaction between focal adhesion and adherens junction proteins: Involvement in sphingosine 1-phosphate-induced endothelial barrier enhancement [O] . Xiaoguang Sun, Yasushi Shikata, Lichun Wang, -1

机译：增强粘着斑和粘附连接蛋白之间的相互作用：参与鞘氨醇1-磷酸酯诱导的内皮屏障增强
7. Enhanced interaction between focal adhesion and adherens junction proteins: Involvement in sphingosine 1-phosphate-induced endothelial barrier enhancement [O] . Xiaoguang Sun, Yasushi Shikata, Lichun Wang, 2009

机译：增强局灶性粘附和粘附结蛋白之间的相互作用：参与鞘氨醇1-磷酸盐诱导的内皮屏障增强

Enhanced interaction between focal adhesion and adherens junction proteins: involvement in sphingosine 1-phosphate-induced endothelial barrier enhancement.

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