超生理核输出信号独立于RanGTP结合CRM1并在Nup358处阻滞。

Supraphysiological nuclear export signals bind CRM1 independently of RanGTP and arrest at Nup358.

作者信息

Engelsma Dieuwke, Bernad Rafael, Calafat Jero, Fornerod Maarten

机构信息

Department of Tumor Biology, The Netherlands Cancer Institute, Amsterdam, The Netherlands.

出版信息

EMBO J. 2004 Sep 15;23(18):3643-52. doi: 10.1038/sj.emboj.7600370. Epub 2004 Aug 26.

DOI:10.1038/sj.emboj.7600370

PMID:15329671

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC517610/

Abstract

Leucine-rich nuclear export signals (NESs) mediate rapid nuclear export of proteins via interaction with CRM1. This interaction is stimulated by RanGTP but remains of a relatively low affinity. In order to identify strong signals, we screened a 15-mer random peptide library for CRM1 binding, both in the presence and absence of RanGTP. Under each condition, strikingly similar signals were enriched, conforming to the NES consensus sequence. A derivative of an NES selected in the absence of RanGTP exhibits very high affinity for CRM1 in vitro and stably binds without the requirement of RanGTP. Localisation studies and RNA interference demonstrate inefficient CRM1-mediated export and accumulation of CRM1 complexed with the high-affinity NES at nucleoporin Nup358. These results provide in vivo evidence for a nuclear export reaction intermediate. They suggest that NESs have evolved to maintain low affinity for CRM1 to allow efficient export complex disassembly and release from Nup358.

摘要

富含亮氨酸的核输出信号（NESs）通过与CRM1相互作用介导蛋白质的快速核输出。这种相互作用受RanGTP刺激，但亲和力相对较低。为了鉴定强信号，我们在有和没有RanGTP的情况下，针对CRM1结合筛选了一个15聚体随机肽库。在每种条件下，显著相似的信号都得到了富集，符合NES共有序列。在没有RanGTP的情况下选择的NES衍生物在体外对CRM1表现出非常高的亲和力，并且无需RanGTP即可稳定结合。定位研究和RNA干扰表明，CRM1介导的输出效率低下，且与高亲和力NES复合的CRM1在核孔蛋白Nup358处积累。这些结果为核输出反应中间体提供了体内证据。它们表明，NESs已经进化到对CRM1保持低亲和力，以允许有效的输出复合物解体并从Nup358释放。

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