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体内组装的真核核糖体复合物中5S、5.8S和28S rRNA与mRNA、tRNA、翻译因子及新生肽的可能相互作用位点。

Possible interaction sites of mRNA, tRNA, translation factors and the nascent peptide in 5S, 5.8S and 28S rRNA in in vivo assembled eukaryotic ribosomal complexes.

作者信息

Sloma M S, Nygård O

机构信息

Natural Science Section, Södertörns högskola, Huddinge, Sweden.

出版信息

Biochim Biophys Acta. 2001 Oct 31;1521(1-3):30-8. doi: 10.1016/s0167-4781(01)00286-x.

Abstract

We have investigated possible interaction sites for mRNA, tRNA, translation factors and the nascent peptide on 5S, 5.8S and 28S rRNA in in vivo assembled translational active mouse ribosomes by comparing the chemical footprinting patterns derived from native polysomes, salt-washed polysomes (mainly lacking translational factors) and salt-washed runoff ribosomes (lacking mRNA, tRNA and translational factors). Several ligand-induced footprints were observed in 28S rRNA while no reactivity changes were seen in 5S and 5.8S rRNA. Footprints derived from mRNA, tRNA and/or the nascent peptide chain were observed in domain I of 28S rRNA (hairpin 23), in domain II (helix 37/38 and helices 42 and 43 and in the eukaryotic expansion segment 15), in domain IV (helices 67 and 74) and in domain V (helices 94 and 96 and in the peptidyl transferase ring). Some of the protected sites were homologous to sites previously suggested to be involved in mRNA, tRNA and/or peptide binding in in vitro assembled prokaryotic complexes. Additional footprints were located in regions that have not previously been found involved in ligand binding. Part of these sites could derive from the nascent peptide in the exit channel of the ribosome.

摘要

我们通过比较天然多核糖体、盐洗多核糖体(主要缺乏翻译因子)和盐洗延伸核糖体(缺乏mRNA、tRNA和翻译因子)产生的化学足迹模式,研究了体内组装的具有翻译活性的小鼠核糖体中mRNA、tRNA、翻译因子和新生肽在5S、5.8S和28S rRNA上可能的相互作用位点。在28S rRNA中观察到几种配体诱导的足迹,而在5S和5.8S rRNA中未观察到反应性变化。在28S rRNA的结构域I(发夹23)、结构域II(螺旋37/38以及螺旋42和43和真核生物扩展片段15)、结构域IV(螺旋67和74)和结构域V(螺旋94和96以及肽基转移酶环)中观察到源自mRNA、tRNA和/或新生肽链的足迹。一些受保护的位点与先前认为参与体外组装的原核复合物中mRNA、tRNA和/或肽结合的位点同源。另外的足迹位于以前未发现参与配体结合的区域。这些位点的一部分可能源自核糖体出口通道中的新生肽。

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