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驱动蛋白KIF5B和KIF5C与Ran结合蛋白2(RanBP2)的对接是通过一个新的RanBP2结构域介导的。

The docking of kinesins, KIF5B and KIF5C, to Ran-binding protein 2 (RanBP2) is mediated via a novel RanBP2 domain.

作者信息

Cai Y, Singh B B, Aslanukov A, Zhao H, Ferreira P A

机构信息

Department of Pharmacology and Toxicology, Medical College of Wisconsin, Milwaukee, Wisconsin 53226, USA.

出版信息

J Biol Chem. 2001 Nov 9;276(45):41594-602. doi: 10.1074/jbc.M104514200. Epub 2001 Sep 11.

Abstract

The Ran-binding protein 2 (RanBP2) is a vertebrate mosaic protein composed of four interspersed RanGTPase binding domains (RBDs), a variable and species-specific zinc finger cluster domain, leucine-rich, cyclophilin, and cyclophilin-like (CLD) domains. Functional mapping of RanBP2 showed that the domains, zinc finger and CLD, between RBD1 and RBD2, and RBD3 and RBD4, respectively, associate specifically with the nuclear export receptor, CRM1/exportin-1, and components of the 19 S regulatory particle of the 26 S proteasome. Now, we report the mapping of a novel RanBP2 domain located between RBD2 and RBD3, which is also conserved in the partially duplicated isoform RanBP2L1. Yet, this domain leads to the neuronal association of only RanBP2 with two kinesin microtubule-based motor proteins, KIF5B and KIF5C. These kinesins associate directly in vitro and in vivo with RanBP2. Moreover, the kinesin light chain and RanGTPase are part of this RanBP2 macroassembly complex. These data provide evidence of a specific docking site in RanBP2 for KIF5B and KIF5C. A model emerges whereby RanBP2 acts as a selective signal integrator of nuclear and cytoplasmic trafficking pathways in neurons.

摘要

Ran结合蛋白2(RanBP2)是一种脊椎动物镶嵌蛋白,由四个散布的RanGTP酶结合结构域(RBD)、一个可变且物种特异性的锌指簇结构域、富含亮氨酸的结构域、亲环蛋白结构域和亲环蛋白样(CLD)结构域组成。RanBP2的功能图谱显示,分别位于RBD1与RBD2之间以及RBD3与RBD4之间的锌指结构域和CLD结构域,特异性地与核输出受体CRM1/输出蛋白1以及26S蛋白酶体的19S调节颗粒的组分相关联。现在,我们报告了一个位于RBD2和RBD3之间的新型RanBP2结构域的图谱,该结构域在部分重复的异构体RanBP2L1中也保守。然而,该结构域仅导致RanBP2与两种基于微管的驱动蛋白KIF5B和KIF5C发生神经元关联。这些驱动蛋白在体外和体内均直接与RanBP2相关联。此外,驱动蛋白轻链和RanGTP酶是这个RanBP2大分子组装复合体的一部分。这些数据为RanBP2中存在KIF5B和KIF5C的特异性对接位点提供了证据。由此出现了一个模型,即RanBP2作为神经元中核和细胞质运输途径的选择性信号整合器发挥作用。

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