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β-肌营养不良蛋白中一种 Importin alpha/beta 识别的核定位信号的特性。

Characterization of an Importin alpha/beta-recognized nuclear localization signal in beta-dystroglycan.

机构信息

Department of Genetics and Molecular Biology, Center for Research and Advanced Studies of the National Polytechnic Institute (CINVESTAV-IPN), Mexico City 07300, Mexico.

出版信息

J Cell Biochem. 2010 Jun 1;110(3):706-17. doi: 10.1002/jcb.22581.

DOI:10.1002/jcb.22581
PMID:20512930
Abstract

Beta-dystroglycan (beta-DG) is a widely expressed transmembrane protein that plays important roles in connecting the extracellular matrix to the cytoskeleton, and thereby contributing to plasma membrane integrity and signal transduction. We previously observed nuclear localization of beta-DG in cultured cell lines, implying the existence of a nuclear targeting mechanism that directs it to the nucleus instead of the plasma membrane. In this study, we delineate the nuclear import pathway of beta-DG, characterizing a functional nuclear localization signal (NLS) in the beta-DG cytoplasmic domain, within amino acids 776-782. The NLS either alone or in the context of the whole beta-DG protein was able to target the heterologous GFP protein to the nucleus, with site-directed mutagenesis indicating that amino acids R(779) and K(780) are critical for NLS functionality. The nuclear transport molecules Importin (Imp)alpha and Impbeta bound with high affinity to the NLS of beta-DG and were found to be essential for NLS-dependent nuclear import in an in vitro reconstituted nuclear transport assay; cotransfection experiments confirmed the dependence on Ran for nuclear accumulation. Intriguingly, experiments suggested that tyrosine phosphorylation of beta-DG may result in cytoplasmic retention, with Y(892) playing a key role. beta-DG thus follows a conventional Impalpha/beta-dependent nuclear import pathway, with important implications for its potential function in the nucleus.

摘要

β-肌营养不良聚糖(β-DG)是一种广泛表达的跨膜蛋白,在将细胞外基质与细胞骨架连接方面发挥重要作用,从而有助于保持质膜的完整性和信号转导。我们之前观察到培养细胞系中β-DG 的核定位,这意味着存在一种将其导向核而不是质膜的核靶向机制。在这项研究中,我们描绘了β-DG 的核输入途径,确定了β-DG 细胞质结构域内 776-782 个氨基酸的功能性核定位信号(NLS)。NLS 无论是单独存在还是在整个β-DG 蛋白的背景下,都能够将异源 GFP 蛋白靶向细胞核,定点突变表明氨基酸 R(779)和 K(780)对 NLS 功能至关重要。核转运分子 Importin(Imp)α和 Impβ与β-DG 的 NLS 具有高亲和力,并在体外重建的核转运测定中发现对于 NLS 依赖性核输入是必需的;共转染实验证实了对 Ran 的核积累依赖性。有趣的是,实验表明β-DG 的酪氨酸磷酸化可能导致细胞质滞留,其中 Y(892)起着关键作用。因此,β-DG 遵循传统的 Impα/β 依赖性核输入途径,这对其在核中的潜在功能具有重要意义。

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