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RanGTP介导的核输入复合物解离的结构基础

Structural basis for nuclear import complex dissociation by RanGTP.

作者信息

Lee Soo Jae, Matsuura Yoshiyuki, Liu Sai Man, Stewart Murray

机构信息

MRC Laboratory of Molecular Biology, Hills Rd, Cambridge CB2 2QH, UK.

出版信息

Nature. 2005 Jun 2;435(7042):693-6. doi: 10.1038/nature03578. Epub 2005 May 1.

Abstract

Nuclear protein import is mediated mainly by the transport factor importin-beta that binds cytoplasmic cargo, most often via the importin-alpha adaptor, and then transports it through nuclear pore complexes. This active transport is driven by disassembly of the import complex by nuclear RanGTP. The switch I and II loops of Ran change conformation with nucleotide state, and regulate its interactions with nuclear trafficking components. Importin-beta consists of 19 HEAT repeats that are based on a pair of antiparallel alpha-helices (referred to as the A- and B-helices). The HEAT repeats stack to yield two C-shaped arches, linked together to form a helicoidal molecule that has considerable conformational flexibility. Here we present the structure of full-length yeast importin-beta (Kap95p or karyopherin-beta) complexed with RanGTP, which provides a basis for understanding the crucial cargo-release step of nuclear import. We identify a key interaction site where the RanGTP switch I loop binds to the carboxy-terminal arch of Kap95p. This interaction produces a change in helicoidal pitch that locks Kap95p in a conformation that cannot bind importin-alpha or cargo. We suggest an allosteric mechanism for nuclear import complex disassembly by RanGTP.

摘要

核蛋白的输入主要由运输因子输入蛋白β介导,它通常通过输入蛋白α衔接子结合细胞质中的货物,然后通过核孔复合体进行运输。这种主动运输由核RanGTP驱动输入复合体的解体来实现。Ran的开关I和II环随核苷酸状态改变构象,并调节其与核运输组件的相互作用。输入蛋白β由19个HEAT重复序列组成,这些重复序列基于一对反平行的α螺旋(称为A螺旋和B螺旋)。HEAT重复序列堆叠形成两个C形拱,连接在一起形成一个具有相当大构象灵活性的螺旋状分子。在此,我们展示了与RanGTP复合的全长酵母输入蛋白β(Kap95p或核转运蛋白β)的结构,这为理解核输入关键的货物释放步骤提供了基础。我们确定了一个关键的相互作用位点,RanGTP开关I环在此处与Kap95p的羧基末端拱结合。这种相互作用导致螺旋螺距发生变化,从而将Kap95p锁定在一种无法结合输入蛋白α或货物的构象中。我们提出了一种由RanGTP介导核输入复合体解体的变构机制。

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