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Landscape of nuclear transport receptor cargo specificity

机译:核运输受体货物特异性的概况

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Abstract Nuclear transport receptors (NTRs) recognize localization signals of cargos to facilitate their passage across the central channel of nuclear pore complexes (NPCs). About 30 different NTRs constitute different transport pathways in humans and bind to a multitude of different cargos. The exact cargo spectrum of the majority of NTRs, their specificity and even the extent to which active nucleocytoplasmic transport contributes to protein localization remains understudied because of the transient nature of these interactions and the wide dynamic range of cargo concentrations. To systematically map cargo?¢????NTR relationships in situ , we used proximity ligation coupled to mass spectrometry (BioID). We systematically fused the engineered biotin ligase BirA* to 16 NTRs. We estimate that a considerable fraction of the human proteome is subject to active nuclear transport. We quantified the specificity and redundancy in NTR interactions and identified transport pathways for cargos. We extended the BioID method by the direct identification of biotinylation sites. This approach enabled us to identify interaction interfaces and to discriminate direct versus piggyback transport mechanisms. Data are available via ProteomeXchange with identifier PXD007976.
机译:摘要核转运受体(NTR)识别货物的定位信号,以促进其通过核孔复合体(NPC)的中央通道。大约30种不同的NTR在人类中构成不同的运输途径,并与多种不同的货物结合。由于这些相互作用的瞬时性质和货物浓度的宽动态范围,大多数NTR的确切货物谱,它们的特异性,甚至活性核质运输对蛋白质定位的贡献程度仍未得到研究。为了系统地映射货物的原位NTR关系,我们使用了邻近结扎质谱联用技术(BioID)。我们系统地将工程化的生物素连接酶BirA *与16个NTR融合。我们估计人类蛋白质组中相当一部分受到主动核运输。我们量化了NTR相互作用的特异性和冗余性,并确定了货物的运输途径。我们通过直接识别生物素化位点扩展了BioID方法。这种方法使我们能够识别交互界面,并区分直接运输方式和搭载运输方式。数据可通过ProteomeXchange获得,其标识符为PXD007976。

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