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Selective regulation of YB-1 mRNA translation by the mTOR signaling pathway is not mediated by 4E-binding protein

机译:通过4TOR结合蛋白不介导mTOR信号通路对YB-1 mRNA翻译的选择性调节

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摘要

The Y-box binding protein 1 (YB-1) is a key regulator of gene expression at the level of both translation and transcription. The mode of its action on cellular events depends on its subcellular distribution and the amount in the cell. So far, the regulatory mechanisms of YB-1 synthesis have not been adequately studied. Our previous finding was that selective inhibition of YB-1 mRNA translation was caused by suppression of activity of the mTOR signaling pathway. It was suggested that this event may be mediated by phosphorylation of the 4E-binding protein (4E-BP). Here, we report that 4E-BP alone can only slightly inhibit YB-1 synthesis both in the cell and in vitro, although it essentially decreases binding of the 4F-group translation initiation factors to mRNA. With inhibited mTOR kinase, the level of mRNA binding to the eIF4F-group factors was decreased, while that to 4E-BP1 was increased, as was observed for both mTOR kinase-sensitive mRNAs and those showing low sensitivity. This suggests that selective inhibition of translation of YB-1 mRNA, and probably some other mRNAs as well, by mTOR kinase inhibitors is not mediated by the action of the 4E-binding protein upon functions of the 4F-group translation initiation factors.
机译:Y盒结合蛋白1(YB-1)是在翻译和转录水平上基因表达的关键调节因子。其对细胞事件的作用方式取决于其亚细胞分布和细胞中的数量。迄今为止,尚未充分研究YB-1合成的调控机制。我们以前的发现是YB-1 mRNA翻译的选择性抑制是由mTOR信号通路活性的抑制引起的。提示此事件可能是由4E结合蛋白(4E-BP)的磷酸化介导的。在这里,我们报道单独的4E-BP只能在细胞和体外略微抑制YB-1的合成,尽管它实质上降低了4F-组翻译起始因子与mRNA的结合。使用受抑制的mTOR激酶,与eIF4F-group因子结合的mRNA水平降低,而与4E-BP1结合的mRNA水平则升高,这对于mTOR激酶敏感的mRNA和低敏感性的mRNA均可见。这表明mTOR激酶抑制剂选择性抑制YB-1 mRNA以及可能的其他一些mRNA的翻译不受4E结合蛋白对4F-组翻译起始因子功能的影响介导。

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