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Two WXXF-based motifs in NECAPs define the specificity of accessory protein binding to AP-1 and AP-2

机译:NECAP中两个基于WXXF的基序定义了辅助蛋白与AP-1和AP-2结合的特异性

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摘要

The adaptor proteins AP-2 and AP-1/GGAs are essential components of clathrin coats at the plasma membrane and trans-Golgi network, respectively. The adaptors recruit accessory proteins to clathrin-coated pits, which is dependent on the adaptor ear domains engaging short peptide motifs in the accessory proteins. Here, we perform an extensive mutational analysis of a novel WXXF-based motif that functions to mediate the binding of an array of accessory proteins to the α-adaptin ear domain of AP-2. Using nuclear magnetic resonance and mutational studies, we identified WXXF-based motifs as major ligands for a site on the α-ear previously shown to bind the DPW-bearing proteins epsin 1/2. We also defined the determinants that allow for specific binding of the α-ear motif to AP-2 as compared to those that allow a highly related WXXF-based motif to bind to the ear domains of AP-1/GGAs. Intriguingly, placement of acidic residues around the WXXF cores is critical for binding specificity. These studies provide a structural basis for the specific recruitment of accessory proteins to appropriate sites of clathrin-coated vesicle formation.
机译:衔接蛋白AP-2和AP-1 / GGA分别是质膜和反式高尔基体网络上网格蛋白外壳的重要成分。衔接子将辅助蛋白募集到网格蛋白包被的凹坑中,这取决于衔接子耳域与辅助蛋白中的短肽基序结合。在这里,我们对基于WXXF的新型基序进行广泛的突变分析,该基序起介导一系列辅助蛋白与AP-2的α-adaptin耳结构域结合的作用。使用核磁共振和突变研究,我们确定了基于WXXF的基序是先前显示与结合DPW的蛋白epsin 1/2结合的α-ear上一个位点的主要配体。与那些允许高度相关的基于WXXF的基序与AP-1 / GGA的耳域结合的决定簇相比,我们还定义了允许α-ear基序与AP-2特异性结合的决定簇。有趣的是,在WXXF核心周围放置酸性残基对于结合特异性至关重要。这些研究为辅助蛋白特异性募集到网格蛋白包被的囊泡形成的适当位点提供了结构基础。

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