首页> 美国卫生研究院文献>Molecular and Cellular Biology >Interaction of Eukaryotic Translation Initiation Factor 4G with the Nuclear Cap-Binding Complex Provides a Link between Nuclear and Cytoplasmic Functions of the m7 Guanosine Cap
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Interaction of Eukaryotic Translation Initiation Factor 4G with the Nuclear Cap-Binding Complex Provides a Link between Nuclear and Cytoplasmic Functions of the m7 Guanosine Cap

机译:真核翻译起始因子4G与核帽结合复合物的相互作用提供了m7鸟苷帽的核和细胞质功能之间的联系。

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摘要

In eukaryotes the majority of mRNAs have an m7G cap that is added cotranscriptionally and that plays an important role in many aspects of mRNA metabolism. The nuclear cap-binding complex (CBC; consisting of CBP20 and CBP80) mediates the stimulatory functions of the cap in pre-mRNA splicing, 3′ end formation, and U snRNA export. As little is known about how nuclear CBC mediates the effects of the cap in higher eukaryotes, we have characterized proteins that interact with CBC in HeLa cell nuclear extracts as potential mediators of its function. Using cross-linking and coimmunoprecipitation, we show that eukaryotic translation initiation factor 4G (eIF4G), in addition to its function in the cytoplasm, is a nuclear CBC-interacting protein. We demonstrate that eIF4G interacts with CBC in vitro and that, in addition to its cytoplasmic localization, there is a significant nuclear pool of eIF4G in mammalian cells in vivo. Immunoprecipitation experiments suggest that, in contrast to the cytoplasmic pool, much of the nuclear eIF4G is not associated with eIF4E (translation cap binding protein of eIF4F) but is associated with CBC. While eIF4G stably associates with spliceosomes in vitro and shows close association with spliceosomal snRNPs and splicing factors in vivo, depletion studies show that it does not participate directly in the splicing reaction. Taken together the data indicate that nuclear eIF4G may be recruited to pre-mRNAs via its interaction with CBC and accompanies the mRNA to the cytoplasm, facilitating the switching of CBC for eIF4F. This may provide a mechanism to couple nuclear and cytoplasmic functions of the mRNA cap structure.
机译:在真核生物中,大多数mRNA具有m 7 G帽,该帽通过转录共添加,并且在mRNA代谢的许多方面起着重要作用。核帽结合复合物(CBC;由CBP20和CBP80组成)在pre-mRNA剪接,3'末端形成和U snRNA输出中介导了帽的刺激功能。关于核CBC如何介导高级真核生物中帽的作用所知甚少,我们已经表征了与HeLa细胞核提取物中CBC相互作用的蛋白质是其功能的潜在介体。使用交联和coimmunoprecipitation,我们显示,真核翻译起始因子4G(eIF4G),除了其在细胞质中的功能,是一种核CBC相互作用蛋白。我们证明,eIF4G在体外与CBC相互作用,除其胞质定位外,在体内哺乳动物细胞中还有重要的eIF4G核库。免疫沉淀实验表明,与细胞质库相反,大部分核eIF4G与eIF4E(eIF4F的翻译帽结合蛋白)不相关,但与CBC相关。尽管eIF4G在体外与剪接体稳定缔合,并在体内与剪接体snRNPs和剪接因子密切相关,但耗竭研究表明eIF4G不直接参与剪接反应。数据合计表明,核eIF4G可能通过其与CBC的相互作用而被募集到pre-mRNA中,并将mRNA伴随到细胞质中,从而促进CBC转换为eIF4F。这可以提供偶联mRNA帽结构的核和细胞质功能的机制。

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