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翻译增强剂可提高核糖体从翻译起始处的释放。

Translation enhancer improves the ribosome liberation from translation initiation.

机构信息

Department of Biomolecular Engineering, Tokyo Institute of Technology, B-53, 4259 Nagatsuda, Midori-ku, Yokohama 226-8501, Japan.

出版信息

J Am Chem Soc. 2013 Sep 4;135(35):13096-106. doi: 10.1021/ja405967h. Epub 2013 Aug 22.

Abstract

For translation initiation in bacteria, the Shine-Dalgarno (SD) and anti-SD sequence of the 30S subunit play key roles for specific interactions between ribosomes and mRNAs to determine the exact position of the translation initiation region. However, ribosomes also must dissociate from the translation initiation region to slide toward the downstream sequence during mRNA translation. Translation enhancers upstream of the SD sequences of mRNAs, which likely contribute to a direct interaction with ribosome protein S1, enhance the yields of protein biosynthesis. Nevertheless, the mechanism of the effect of translation enhancers to initiate the translation is still unknown. In this paper, we investigated the effects of the SD and enhancer sequences on the binding kinetics of the 30S ribosomal subunits to mRNAs and their translation efficiencies. mRNAs with both the SD and translation enhancers promoted the amount of protein synthesis but destabilized the interaction between the 30S subunit and mRNA by increasing the dissociation rate constant (koff) of the 30S subunit. Based on a model for kinetic parameters, a 16-fold translation efficiency could be achieved by introducing a tandem repeat of adenine sequences (A20) between the SD and translation enhancer sequences. Considering the results of this study, translation enhancers with an SD sequence regulate ribosomal liberation from translation initiation to determine the translation efficiency of the downstream coding region.

摘要

对于细菌中的翻译起始,30S 亚基的 Shine-Dalgarno (SD) 和反 SD 序列在核糖体和 mRNA 之间的特异性相互作用中起关键作用,以确定翻译起始区的准确位置。然而,核糖体在 mRNA 翻译过程中也必须从翻译起始区解离,以向下游序列滑动。SD 序列上游的翻译增强子可能与核糖体蛋白 S1 直接相互作用,从而增强蛋白质生物合成的产量。然而,翻译增强子启动翻译的机制仍然未知。在本文中,我们研究了 SD 和增强子序列对 30S 核糖体亚基与 mRNA 结合动力学及其翻译效率的影响。具有 SD 和翻译增强子的 mRNA 促进了蛋白质合成的量,但通过增加 30S 亚基的解离速率常数 (koff) 来破坏 30S 亚基和 mRNA 之间的相互作用。基于动力学参数模型,通过在 SD 和翻译增强子序列之间引入串联重复的腺嘌呤序列 (A20),可以实现 16 倍的翻译效率。考虑到这项研究的结果,具有 SD 序列的翻译增强子调节核糖体从翻译起始的释放,以确定下游编码区的翻译效率。

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