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Discs large 1 (Dlg1) 支架蛋白与网格蛋白和衔接蛋白复合物 1 (AP-1) 一起参与形成内皮细胞的 Weibel-Palade 体。

Discs large 1 (Dlg1) scaffolding protein participates with clathrin and adaptator protein complex 1 (AP-1) in forming Weibel-Palade bodies of endothelial cells.

机构信息

INSERM U698, Université Paris 7, Hemostasis, Bio-Engineering and Cardiovascular Remodeling, CHU X. Bichat, 75018 Paris, France.

出版信息

J Biol Chem. 2013 May 3;288(18):13046-56. doi: 10.1074/jbc.M112.441261. Epub 2013 Mar 26.

DOI:10.1074/jbc.M112.441261
PMID:23532850
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3642347/
Abstract

Weibel-Palade bodies (WPBs) are specific cigar-shaped granules that store von Willebrand factor (VWF) for its regulated secretion by endothelial cells. The first steps of the formation of these granules at the trans-Golgi network specifically require VWF aggregation and an external scaffolding complex that contains the adaptator protein complex 1 (AP-1) and clathrin. Discs large 1 (Dlg1) is generally considered to be a modular scaffolding protein implicated in the control of cell polarity in a large variety of cells by specific recruiting of receptors, channels, or signaling proteins to specialized zones of the plasma membrane. We propose here that in endothelial cells, Dlg1, in a complex with AP-1 and clathrin, participates in the biogenesis of WPBs. Supporting data show that Dlg1 colocalizes with microtubules, intermediate filaments, and Golgi markers. Tandem mass spectrometry experiments led to the identification of clathrin as an Dlg1-interacting partner. Interaction was confirmed by in situ proximity ligation assays. Furthermore, AP-1 and VWF immunoprecipitate and colocalize with Dlg1 in the juxtanuclear zone. Finally, Dlg1 depletion by siRNA duplexes disrupts trans-Golgi network morphology and WPB formation. Our results provide the first evidence for an unexpected role of Dlg1 in controlling the formation of specific secretory granules involved in VWF exocytosis in endothelial cells.

摘要

Weibel-Palade 小体(WPBs)是一种特殊的雪茄形颗粒,可储存血管性血友病因子(VWF),以供内皮细胞对其进行调节性分泌。这些颗粒在高尔基体内网络中的形成的第一步,特别需要 VWF 聚集和一个外部支架复合物,该复合物包含衔接蛋白复合物 1(AP-1)和网格蛋白。Discs large 1(Dlg1)通常被认为是一种模块化支架蛋白,通过将受体、通道或信号蛋白特异性募集到质膜的特定区域,参与多种细胞的细胞极性的控制。在这里,我们提出 Dlg1 与 AP-1 和网格蛋白形成复合物,参与 WPB 的生物发生。支持数据表明 Dlg1 与微管、中间丝和高尔基体标记物共定位。串联质谱实验鉴定到网格蛋白是 Dlg1 的相互作用伙伴。通过原位邻近连接测定实验证实了相互作用。此外,AP-1 和 VWF 免疫沉淀与 Dlg1 在核周区共定位。最后,通过 siRNA 双链体耗尽 Dlg1 会破坏高尔基体内网络形态和 WPB 的形成。我们的研究结果为 Dlg1 在控制内皮细胞中 VWF 胞吐作用所涉及的特定分泌颗粒形成中的意外作用提供了第一个证据。

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本文引用的文献

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von Willebrand disease biology.血管性血友病生物学
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2
von Willebrand factor: an emerging target in stroke therapy.血管性血友病因子:脑卒中治疗的新兴靶点。
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Myosin 1b promotes the formation of post-Golgi carriers by regulating actin assembly and membrane remodelling at the trans-Golgi network.肌球蛋白 1b 通过调节高尔基网络中转部位的肌动蛋白组装和膜重塑促进了高尔基体后载体的形成。
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Identification of mitogen-activated protein/extracellular signal-responsive kinase kinase 2 as a novel partner of the scaffolding protein human homolog of disc-large.鉴定丝裂原活化蛋白/细胞外信号调节激酶激酶 2 为支架蛋白人同源物 disc-large 的新伴侣。
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A role for Rab10 in von Willebrand factor release discovered by an AP-1 interactor screen in C. elegans.通过在秀丽隐杆线虫中进行 AP-1 相互作用筛选发现 Rab10 在血管性血友病因子释放中的作用。
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