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Escherichia coli ribosomal protein L20 binds as a single monomer to its own mRNA bearing two potential binding sites

机译:大肠杆菌核糖体蛋白L20作为单个单体与自身带有两个潜在结合位点的mRNA结合

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摘要

Ribosomal protein L20 is crucial for the assembly of the large ribosomal subunit and represses the translation of its own mRNA. L20 mRNA carries two L20-binding sites, the first folding into a pseudoknot and the second into an imperfect stem and loop. These two sites and the L20-binding site on 23S ribosomal RNA are recognized similarly using a single RNA-binding site located on one face of L20. In this work, using gel filtration and fluorescence cross-correlation spectroscopy (FCCS) experiments, we first exclude the possibility that L20 forms a dimer, which would allow each monomer to bind one site of the mRNA. Secondly we show, using affinity purification and FCCS experiments, that only one molecule of L20 binds to the L20 mRNA despite the presence of two potential binding sites. Thirdly, using RNA chemical probing, we show that the two L20-binding sites are in interaction. This interaction provides an explanation for the single occupancy of the mRNA. The two interacting sites could form a single hybrid site or the binding of L20 to a first site may inhibit binding to the second. Models of regulation compatible with our data are discussed.
机译:核糖体蛋白L20对于组装大型核糖体亚基至关重要,并抑制其自身mRNA的翻译。 L20 mRNA带有两个L20结合位点,第一个折叠成假结,第二个折叠成不完善的茎和环。这两个位点和23S核糖体RNA上的L20结合位点可以使用位于L20的一个面上的单个RNA结合位点类似地识别。在这项工作中,使用凝胶过滤和荧光互相关光谱(FCCS)实验,我们首先排除了L20形成二聚体的可能性,该二聚体将允许每个单体结合mRNA的一个位点。其次,我们使用亲和纯化和FCCS实验表明,尽管存在两个潜在的结合位点,但只有一个L20分子与L20 mRNA结合。第三,使用RNA化学探测,我们表明两个L20结合位点相互作用。这种相互作用为mRNA的单次占据提供了解释。两个相互作用位点可以形成单个杂合位点,或者L20与第一个位点的结合可以抑制与第二个位点的结合。讨论了与我们的数据兼容的监管模型。

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