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Nup53 与 Ndc1 和 Nup155 的相互作用对于核孔复合体的组装是必需的。

Interaction of Nup53 with Ndc1 and Nup155 is required for nuclear pore complex assembly.

机构信息

Friedrich Miescher Laboratory of the Max Planck Society, Spemannstr. 39, 72076 Tübingen, Germany.

出版信息

J Cell Sci. 2014 Feb 15;127(Pt 4):908-21. doi: 10.1242/jcs.141739. Epub 2013 Dec 20.

Abstract

Nuclear pore complexes (NPCs) are the gateways for nucleocytoplasmic exchange. The ordered assembly of these huge complexes from several hundred individual components into an intricate protein interaction network which deforms the two membranes of the nuclear envelope into a pore is only rudimentarily understood. Here, we show that the interaction between Nup53 and the integral pore membrane protein Ndc1 is essential for vertebrate NPC assembly. The Ndc1 binding site on Nup53 overlaps with a region that induces membrane bending and is specifically required to modulate this activity, suggesting that the membrane-deforming capability of Nup53 is adjusted during the NPC assembly process. We further demonstrate that the interaction of Nup53 and Nup155 has a crucial role in NPC formation as the main determinant of recruitment of Nup155 to the assembling pore. Overall, our results pinpoint the diversity of interaction modes accomplished by Nup53, highlighting this protein as an essential link between the pore membrane and the NPC, and as a crucial factor in the formation of the pore membrane.

摘要

核孔复合体(NPC)是核质交换的门户。这些巨大的复合物由数百个单独的组件有序组装成一个错综复杂的蛋白质相互作用网络,将核膜的两层变形为一个孔,目前对此只有初步的了解。在这里,我们表明,核孔蛋白 Ndc1 与整孔膜蛋白 Nup53 之间的相互作用对于脊椎动物 NPC 的组装是必不可少的。Nup53 上与 Ndc1 结合的区域与一个诱导膜弯曲的区域重叠,并且该区域对于调节该活性是特异性必需的,这表明 Nup53 的膜变形能力在 NPC 组装过程中被调节。我们进一步证明,Nup53 和 Nup155 之间的相互作用在 NPC 形成中起着至关重要的作用,因为它是将 Nup155 招募到组装孔的主要决定因素。总的来说,我们的结果指出了 Nup53 完成的多种相互作用模式,突出了该蛋白作为核孔膜与 NPC 之间的重要连接,以及作为核孔膜形成的关键因素。

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