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Importin beta-depending nuclear import pathways: Role of the adapter proteins in the docking and releasing steps

机译:Importinβ依赖性核导入途径:衔接蛋白在对接和释放步骤中的作用

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摘要

Nuclear imports of uridine-rich small nuclear ribonucleoprotein (U1 snRNP) and proteins with classical nuclear localization signal (cNLS-protein) are mediated by importin beta. However, due to the presence of different import signals, the adapter protein of the imported molecules and importin beta is different for each pathway. Although the adapter for cNLS-protein is importin a, the adapter for U1 snRNP is snurportin1 (SPN1). Herein, we show that the use of distinct adapters by importin beta results in differences at the docking and releasing step for these two import pathways. Nuclear pore complex (NPC) docking of U1 snRNP but not of cNLS-protein was inhibited by an anti-CAN/Nup214 antibody. Thus, the initial NPC-binding site is different for each pathway. Pull-down assays between immobilized SPN1 and two truncated forms of importin P documented that SPN1 and importin alpha have different binding sites on importin beta. Importin beta fragment 1-618, which binds to SPN1 but not to importin alpha, was able to support the nuclear import of U1 snRNPs. After the translocation through the NPC, both import complexes associated with the nuclear side of the NPC. However, we found that the nature of the importin beta-binding domain of the adapters influences the release of the cargo into the nucleoplasm. [References: 39]
机译:富含尿苷的小核糖核蛋白(U1 snRNP)和具有经典核定位信号的蛋白(cNLS蛋白)的核输入由importin beta介导。但是,由于存在不同的导入信号,因此每种途径的导入分子的接头蛋白和importinβ均不同。尽管cNLS蛋白的衔接子是importin a,但U1 snRNP的衔接子是snurportin1(SPN1)。在本文中,我们显示importin beta使用不同的衔接子会导致这两种导入途径在对接和释放步骤产生差异。 U1 snRNP而不是cNLS蛋白的核孔复合物(NPC)对接被抗CAN / Nup214抗体抑制。因此,每种途径的初始NPC结合位点是不同的。固定化SPN1和两种截短形式的importin P之间的下拉测定法证明SPN1和importin alpha在importin beta上具有不同的结合位点。 Importin beta片段1-618与SPN1结合,但不与importin alpha结合,能够支持U1 snRNP的核导入。通过NPC易位后,两个进口复合物均与NPC的核侧有关。但是,我们发现衔接子的importinβ-结合结构域的性质影响货物释放到核质中。 [参考:39]

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