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Molecular basis for Nup37 and ELY5/ELYS recruitment to the nuclear pore complex

机译:Nup37和ELY5 / ELYS募集到核孔复合物中的分子基础

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摘要

Nucleocytoplasmic transport is mediated by nuclear pore complexes (NPCs), enormous assemblies composed of multiple copies of ∼30 different proteins called nucleoporins. To unravel the basic scaffold underlying the NPC, we have characterized the species-specific scaffold nucleoporin Nup37 and ELY5/ELYS. Both proteins integrate directly via Nup120/160 into the universally conserved heptameric Y-complex, the critical unit for the assembly and functionality of the NPC. We present the crystal structure of Schizosaccharomyces pombe Nup37 in complex with Nup120, a 174-kDa subassembly that forms one of the two short arms of the Y-complex. Nup37 binds near the bend of the L-shaped Nup120 protein, potentially stabilizing the relative orientation of its two domains. By means of reconstitution assays, we pinpoint residues crucial for this interaction. In vivo and in vitro results show that ELY5 binds near an interface of the Nup120–Nup37 complex. Complementary biochemical and cell biological data refine and consolidate the interactions of Nup120 within the current Y-model. Finally, we propose an orientation of the Y-complex relative to the pore membrane, consistent with the lattice model.
机译:核细胞质运输是由核孔复合体(NPC)介导的,核复合体是由30多种不同蛋白(称为核孔蛋白)的多个副本组成的巨大装配体。为了弄清NPC的基本支架,我们已经对物种特异性支架核孔蛋白Nup37和ELY5 / ELYS进行了表征。两种蛋白都通过Nup120 / 160直接整合到普遍保守的七聚体Y复合物中,这是NPC组装和功能的关键单元。我们目前与Nup120,一个174 kDa的子集,形成Y复合物的两个短臂之一的复合物中,裂殖酵母Nup37的晶体结构。 Nup37在L形Nup120蛋白的弯曲附近结合,可能稳定其两个结构域的相对方向。通过重构分析,我们可以确定对于这种相互作用至关重要的残基。体内和体外结果表明,ELY5在Nup120–Nup37复合体的界面附近结合。互补的生化和细胞生物学数据完善并巩固了Nup120在当前Y模型中的相互作用。最后,我们提出Y络合物相对于孔膜的取向,与晶格模型一致。

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