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Galectin-1 is a novel structural component and a major regulator of H-Ras nanoclusters

机译:Galectin-1是H-Ras纳米簇的新型结构组分和主要调节剂

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The organization of Ras proteins into nanoclusters on the inner plasma membrane is essential for Ras signal transduction, but the mechanisms that drive nanoclustering are unknown. Here we show that epidermal growth factor receptor activation stimulates the formation of H-Ras. GTP-Galectin-1 (Gal-1) complexes on the plasma membrane that are then assembled into transient nanoclusters. Gal-1 is therefore an integral structural component of the H-Ras-signaling nanocluster. Increasing Gal-1 levels increases the stability of H-Ras nanoclusters, leading to enhanced effector recruitment and signal output. Elements in the H-Ras C-terminal hypervariable region and an activated G-domain are required for H-Ras-Gal-1 interaction. Palmitoylation is not required for H-Ras-Gal-1 complex formation, but is required to anchor H-Ras-Gal-1 complexes to the plasma membrane. Our data suggest a mechanism for H-Ras nanoclustering that involves a dual role for Gal-1 as a critical scaffolding protein and a molecular chaperone that contributes to H-Ras trafficking by returning depalmitoylated H-Ras to the Golgi complex for repalmitoylation.
机译:Ras蛋白在内质膜上形成纳米簇的组织对于Ras信号转导至关重要,但是驱动纳米簇的机制尚不清楚。在这里,我们表明表皮生长因子受体激活刺激H-Ras的形成。 GTP-Galectin-1(Gal-1)复合物在质膜上,然后组装成瞬态纳米簇。因此,Gal-1是H-Ras信号纳米簇的组成部分。 Gal-1水平的增加会增加H-Ras纳米簇的稳定性,从而导致效应子募集和信号输出增强。 H-Ras-Gal-1相互作用需要H-Ras C端高变区和激活的G结构域中的元​​素。棕榈酰化对于H-Ras-Gal-1复合物的形成不是必需的,但是对于将H-Ras-Gal-1复合物锚定到质膜是必需的。我们的数据表明,H-Ras纳米簇的机制涉及Gal-1作为关键支架蛋白和分子伴侣的双重作用,该分子伴侣通过使去棕榈酰化的H-Ras返回高尔基复合体进行再棕榈酸酯化,从而有助于H-Ras的运输。

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