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Long-range translational coupling in single-stranded RNA bacteriophages: an evolutionary analysis.

机译:单链RNA噬菌体中的远程翻译偶联:进化分析。

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In coliphage MS2 RNA a long-distance interaction (LDI) between an internal segment of the upstream coat gene and the start region of the replicase gene prevents initiation of replicase synthesis in the absence of coat gene translation. Elongating ribosomes break up the repressor LDI and thus activate the hidden initiation site. Expression studies on partial MS2 cDNA clones identified base pairing between 1427-1433 and 1738-1744, the so-called Min Jou (MJ) interaction, as the molecular basis for the long-range coupling mechanism. Here, we examine the biological significance of this interaction for the control of replicase gene translation. The LDI was disrupted by mutations in the 3'-side and the evolutionary adaptation was monitored upon phage passaging. Two categories of pseudorevertants emerged. The first type had restored the MJ interaction but not necessarily the native sequence. The pseudorevertants of the second type acquired a compensatory substitution some 80 nt downstream of the MJ interaction that stabilizes an adjacent LDI. In one examined case we confirmed that the second site mutations had restored coat-replicase translational coupling. Our results show the importance of translational control for fitness of the phage. They also reveal that the structure that buries the replicase start extends to structure elements bordering the MJ interaction.
机译:在大肠杆菌噬菌体MS2 RNA中,上游外壳基因的内部区段与复制酶基因的起始区域之间的长距离相互作用(LDI)可在没有外壳基因翻译的情况下阻止复制酶合成的启动。伸长的核糖体破坏了阻遏物LDI,从而激活了隐藏的起始位点。对部分MS2 cDNA克隆的表达研究确定了1427-1433和1738-1744之间的碱基配对,即所谓的Min Jou(MJ)相互作用,作为长程偶联机制的分子基础。在这里,我们检查这种相互作用的生物学意义,以控制复制酶基因翻译。 LDI被3'侧的突变所破坏,并且在噬菌体传代过程中监测了进化适应性。出现了两类伪还原剂。第一种已经恢复了MJ相互作用,但不一定恢复了天然序列。第二类型的伪回复剂在MJ相互作用的下游约80 nt处获得了补偿性取代,从而稳定了相邻的LDI。在一个检查的案例中,我们证实了第二个位点突变已恢复了外套复制子的翻译偶联。我们的结果表明翻译控制对噬菌体适应性的重要性。他们还揭示了掩盖复制酶起始的结构扩展到与MJ相互作用接壤的结构元素。

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