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多功能蛋白YB-1与IRP2相互作用通过铁反应元件实现新型翻译调控。

Novel translational control through an iron-responsive element by interaction of multifunctional protein YB-1 and IRP2.

作者信息

Ashizuka Megumi, Fukuda Takao, Nakamura Takanori, Shirasuna Kanemitsu, Iwai Kazuhiro, Izumi Hiroto, Kohno Kimitoshi, Kuwano Michihiko, Uchiumi Takeshi

机构信息

Department of Medical Biochemistry, Graduate School of Medical Sciences, Kyushu University, Higashi-ku, Fukuoka 812-8582, Japan.

出版信息

Mol Cell Biol. 2002 Sep;22(18):6375-83. doi: 10.1128/MCB.22.18.6375-6383.2002.

Abstract

The eukaryotic Y-box-binding protein YB-1 functions in various biological processes, including DNA repair, cell proliferation, and transcriptional and translational controls. To gain further insight into how human YB-1 plays its role in pleiotropic functions, we here used two-hybrid screenings to identify partners of this protein; the results showed that YB-1 itself, iron-regulatory protein 2 (IRP2), and five ribosomal proteins each served as partners to YB-1. We then examined the biological effect of the interaction of YB-1 and IRP2 on translational regulation. Both in vitro binding and coimmunoprecipitation assays showed the direct interaction of YB-1 and IRP2 in the presence of a high concentration of iron. RNA gel shift assays showed that YB-1 reduced the formation of the IRP2-mRNA complex when the iron-responsive element of the ferritin mRNA 5' untranslated region (UTR) was used as a probe. By using an in vitro translation assay using luciferase mRNA ligated to the ferritin mRNA 5'UTR as a reporter construct, we showed that both YB-1 and IRP2 inhibited the translation of the mRNA. However, coadministration of YB-1 and IRP2 proteins abrogated the inhibition of protein synthesis by each protein. An In vivo coimmunoprecipitation assay showed that IRP2 bound to YB-1 in the presence of iron and a proteasome inhibitor. The direct interaction of YB-1 and IRP2 provides the first evidence of the involvement of YB-1 in the translational regulation of an iron-related protein.

摘要

真核生物Y盒结合蛋白YB-1在多种生物学过程中发挥作用,包括DNA修复、细胞增殖以及转录和翻译控制。为了更深入了解人类YB-1如何在多效性功能中发挥作用,我们在此使用双杂交筛选来鉴定该蛋白的相互作用伙伴;结果表明,YB-1自身、铁调节蛋白2(IRP2)以及五种核糖体蛋白各自作为YB-1的相互作用伙伴。然后,我们研究了YB-1与IRP2相互作用对翻译调控的生物学效应。体外结合和免疫共沉淀分析均表明,在高浓度铁存在的情况下,YB-1与IRP2直接相互作用。RNA凝胶迁移分析表明,当使用铁蛋白mRNA 5'非翻译区(UTR)的铁反应元件作为探针时,YB-1减少了IRP2-mRNA复合物的形成。通过使用以连接到铁蛋白mRNA 5'UTR的荧光素酶mRNA作为报告构建体的体外翻译分析,我们表明YB-1和IRP2均抑制该mRNA的翻译。然而,同时给予YB-1和IRP2蛋白可消除每种蛋白对蛋白质合成的抑制作用。体内免疫共沉淀分析表明,在铁和蛋白酶体抑制剂存在的情况下,IRP2与YB-1结合。YB-1与IRP2的直接相互作用首次证明了YB-1参与铁相关蛋白的翻译调控。

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本文引用的文献

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