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首页> 外文OA文献 >Post-translational Maturation of Dystroglycan Is Necessary for Pikachurin Binding and Ribbon Synaptic Localization*
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Post-translational Maturation of Dystroglycan Is Necessary for Pikachurin Binding and Ribbon Synaptic Localization*

机译:皮卡丘林结合和功能区突触定位必需的dystroglycan的翻译后成熟。

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Pikachurin, the most recently identified ligand of dystroglycan, plays a crucial role in the formation of the photoreceptor ribbon synapse. It is known that glycosylation of dystroglycan is necessary for its ligand binding activity, and hypoglycosylation is associated with a group of muscular dystrophies that often involve eye abnormalities. Because little is known about the interaction between pikachurin and dystroglycan and its impact on molecular pathogenesis, here we characterize the interaction using deletion constructs and mouse models of muscular dystrophies with glycosylation defects (Largemyd and POMGnT1-deficient mice). Pikachurin-dystroglycan binding is calcium-dependent and relatively less sensitive to inhibition by heparin and high NaCl concentration, as compared with other dystroglycan ligand proteins. Using deletion constructs of the laminin globular domains in the pikachurin C terminus, we show that a certain steric structure formed by the second and the third laminin globular domains is necessary for the pikachurin-dystroglycan interaction. Binding assays using dystroglycan deletion constructs and tissue samples from Large-deficient (Largemyd) mice show that Large-dependent modification of dystroglycan is necessary for pikachurin binding. In addition, the ability of pikachurin to bind to dystroglycan prepared from POMGnT1-deficient mice is severely reduced, suggesting that modification of the GlcNAc-β1,2-branch on O-mannose is also necessary for the interaction. Immunofluorescence analysis reveals a disruption of pikachurin localization in the photoreceptor ribbon synapse of these model animals. Together, our data demonstrate that post-translational modification on O-mannose, which is mediated by Large and POMGnT1, is essential for pikachurin binding and proper localization, and suggest that their disruption underlies the molecular pathogenesis of eye abnormalities in a group of muscular dystrophies.
机译:皮卡丘林是dystroglycan的最新鉴定的配体,在感光带突触的形成中起关键作用。已知dystroglycan的糖基化对于其配体结合活性是必需的,并且低糖基化与一组肌肉营养不良有关,这些肌肉营养不良经常涉及眼睛异常。因为对皮卡丘林和dystroglycan之间的相互作用及其对分子发病机理的影响知之甚少,所以在这里我们使用缺失构建体和具有糖基化缺陷的肌营养不良症的小鼠模型(Largemyd和POMGnT1缺陷小鼠)来描述相互作用。与其他dystroglycan配体蛋白相比,皮卡丘林-dystroglycan结合是钙依赖性的,对肝素和高NaCl浓度的抑制作用相对较不敏感。使用在皮卡丘陵蛋白C末端层粘连蛋白球状结构域的删除构建体,我们表明由第二和第三个层粘连蛋白球状结构域形成的一定的空间结构是皮卡丘林蛋白-dystroglycan相互作用所必需的。使用dystroglycan删除构建体和大缺陷(Largemyd)小鼠组织样品的结合测定表明,dystroglycan的大依赖性修饰对于皮卡丘林蛋白的结合是必需的。此外,皮卡丘林与由POMGnT1缺陷型小鼠制备的dystroglycan结合的能力严重降低,这表明相互作用中还需要修饰Olc-甘露糖上GlcNAc-β1,2-分支。免疫荧光分析揭示了这些模型动物的感光带突触中皮卡丘林定位的破坏。总之,我们的数据表明,由大蛋白和POMGnT1介导的O-甘露糖的翻译后修饰对于皮卡丘林结合和正确定位必不可少,并表明它们的破坏是一组肌肉营养不良症眼异常的分子发病机理的基础。 。

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