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首页> 外文期刊>Journal of cell biology >Posttranslational marks control architectural and functional plasticity of the nuclear pore complex basket
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Posttranslational marks control architectural and functional plasticity of the nuclear pore complex basket

机译:翻译后标记控制核孔复合体篮的结构和功能可塑性

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摘要

The nuclear pore complex (NPC) serves as both the unique gate between the nucleus and the cytoplasm and a major platform that coordinates nucleocytoplasmic exchanges, gene expression, and genome integrity. To understand how the NPC integrates these functional constraints, we dissected here the posttranslational modifications of the nuclear basket protein Nup60 and analyzed how they intervene to control the plasticity of the NPC. Combined approaches highlight the role of monoubiquitylation in regulating the association dynamics of Nup60 and its partner, Nup2, with the NPC through an interaction with Nup84, a component of the Y complex. Although major nuclear transport routes are not regulated by Nup60 modifications, monoubiquitylation of Nup60 is stimulated upon genotoxic stress and regulates the DNA-damage response and telomere repair. Together, these data reveal an original mechanism contributing to the plasticity of the NPC at a molecular-organization and functional level.
机译:核孔复合物(NPC)既是细胞核与细胞质之间的唯一通道,又是协调核细胞质交换,基因表达和基因组完整性的主要平台。为了了解NPC如何整合这些功能限制,我们在此剖析了核篮蛋白Nup60的翻译后修饰,并分析了它们如何干预以控制NPC的可塑性。结合的方法强调了单泛素化在通过与N复合物Nup84的相互作用来调节Nup60及其伙伴Nup2与NPC缔合动力学中的作用。尽管主要的核转运途径不受Nup60修饰的调节,但是Nup60的单泛素化会在遗传毒性胁迫下被刺激并调节DNA损伤反应和端粒修复。总之,这些数据揭示了在分子组织和功能水平上有助于NPC可塑性的原始机制。

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