首页> 外文期刊>Journal of Molecular Biology >Structural lability in stem-loop 1 drives a 5' UTR-3' UTR interaction in coronavirus replication.
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Structural lability in stem-loop 1 drives a 5' UTR-3' UTR interaction in coronavirus replication.

机译:茎环1中的结构不稳定性驱动冠状病毒复制中的5'UTR-3'UTR相互作用。

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The leader RNA of the 5' untranslated region (UTR) of coronaviral genomes contains two stem-loop structures denoted SL1 and SL2. Herein, we show that SL1 is functionally and structurally bipartite. While the upper region of SL1 is required to be paired, we observe strong genetic selection against viruses that contain a deletion of A35, an extrahelical nucleotide that destabilizes SL1, in favor of genomes that contain a diverse panel of destabilizing second-site mutations, due to introduction of a noncanonical base pair near A35. Viruses containing destabilizing SL1-DeltaA35 mutations also contain one of two specific mutations in the 3' UTR. Thermal denaturation and imino proton solvent exchange experiments reveal that the lower half of SL1 is unstable and that second-site SL1-DeltaA35 substitutions are characterized by one or more features of the wild-type SL1. We propose a "dynamic SL1" model, in which the base of SL1 has an optimized lability required to mediate a physical interaction between the 5' UTR and the 3' UTR that stimulates subgenomic RNA synthesis. Although not conserved at the nucleotide sequence level, these general structural characteristics of SL1 appear to be conserved in other coronaviral genomes.
机译:冠状病毒基因组5'非翻译区(UTR)的前导RNA包含两个茎环结构,分别表示为SL1和SL2。在此,我们表明SL1在功能和结构上都是二分的。虽然需要将SL1的上部区域配对,但我们观察到针对包含A35缺失的病毒的强大遗传选择,A35是使SL1不稳定的螺旋外核苷酸,有利于基因组包含各种不稳定的第二位点突变,这是由于在A35附近引入一个非经典碱基对。含有不稳定的SL1-DeltaA35突变的病毒在3'UTR中也含有两个特定突变之一。热变性和亚氨基质子溶剂交换实验表明,SL1的下半部分不稳定,第二位SL1-DeltaA35取代的特征是野生型SL1的一个或多个特征。我们提出了一种“动态SL1”模型,其中SL1的碱基具有优化的不稳定性,可调节介导5'UTR和3'UTR之间刺激亚基因组RNA合成的物理相互作用。尽管在核苷酸序列水平上不是保守的,但SL1的这些一般结构特征似乎在其他冠状病毒基因组中是保守的。

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