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首页> 外文期刊>Molecular cell >IRP-1 binding to ferritin mRNA prevents the recruitment of the small ribosomal subunit by the cap-binding complex eIF4F.
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IRP-1 binding to ferritin mRNA prevents the recruitment of the small ribosomal subunit by the cap-binding complex eIF4F.

机译:IRP-1与铁蛋白mRNA的结合可防止通过帽结合复合物eIF4F募集小核糖体亚基。

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摘要

Binding of iron regulatory proteins (IRPs) to IREs located in proximity to the cap structure of ferritin H- and L-chain mRNAs blocks ferritin synthesis by preventing the recruitment of the small ribosomal subunit to the mRNA. We have devised a novel procedure to examine the assembly of translation initiation factors (eIFs) on regulated mRNAs. Unexpectedly, we find that the cap binding complex eIF4F (comprising eIF4E, eIF4G, and eIF4A) assembles even when IRP-1 is bound to the cap-proximal IRE. This assembly is futile, because bridging interactions between eIF4F and the small ribosomal subunit cannot be established in the presence of IRP-1. Our findings provide insight into translational control by an mRNA binding protein at the level of translation initiation factors and uncover a key regulatory step in iron homeostasis.
机译:铁调节蛋白(IRP)与位于铁蛋白H和L链mRNA帽结构附近的IRE的结合通过阻止小核糖体亚基募集到mRNA来阻止铁蛋白合成。我们设计了一种新颖的程序来检查受调控的mRNA的翻译起始因子(eIF)的装配。出乎意料的是,我们发现即使将IRP-1结合到靠近帽的IRE上,帽结合复合物eIF4F(包含eIF4E,eIF4G和eIF4A)也会组装。这种组装是徒劳的,因为在存在IRP-1的情况下,无法建立eIF4F与核糖体小亚基之间的架桥作用。我们的发现提供了在翻译起始因子水平上通过mRNA结合蛋白进行翻译控制的见解,并揭示了铁稳态中的关键调控步骤。

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