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首页> 外文期刊>Journal of Molecular Biology >Conformation effects of base modification on the anticodon stem-loop of Bacillus subtilis tRNA(Tyr).
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Conformation effects of base modification on the anticodon stem-loop of Bacillus subtilis tRNA(Tyr).

机译:碱基修饰对枯草芽孢杆菌tRNA(Tyr)反密码子茎环的构象影响。

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tRNA molecules contain 93 chemically unique nucleotide base modifications that expand the chemical and biophysical diversity of RNA and contribute to the overall fitness of the cell. Nucleotide modifications of tRNA confer fidelity and efficiency to translation and are important in tRNA-dependent RNA-mediated regulatory processes. The three-dimensional structure of the anticodon is crucial to tRNA-mRNA specificity, and the diverse modifications of nucleotide bases in the anticodon region modulate this specificity. We have determined the solution structures and thermodynamic properties of Bacillus subtilis tRNA(Tyr) anticodon arms containing the natural base modifications N(6)-dimethylallyl adenine (i(6)A(37)) and pseudouridine (psi(39)). UV melting and differential scanning calorimetry indicate that the modifications stabilize the stem and may enhance base stacking in the loop. The i(6)A(37) modification disrupts the hydrogen bond network of the unmodified anticodon loop including a C(32)-A(38)(+) base pair and an A(37)-U(33) base-base interaction. Although the i(6)A(37) modification increases the dynamic nature of the loop nucleotides, metal ion coordination reestablishes conformational homogeneity. Interestingly, the i(6)A(37) modification and Mg(2+) are sufficient to promote the U-turn fold of the anticodon loop of Escherichia coli tRNA(Phe), but these elements do not result in this signature feature of the anticodon loop in tRNA(Tyr).
机译:tRNA分子包含93种化学上独特的核苷酸碱基修饰,可扩展RNA的化学和生物物理多样性并有助于细胞的整体适应性。 tRNA的核苷酸修饰赋予保真度和翻译效率,并且在依赖tRNA的RNA介导的调节过程中很重要。反密码子的三维结构对于tRNA-mRNA的特异性至关重要,而反密码子区域核苷酸碱基的多种修饰调节了这种特异性。我们已经确定了包含天然碱基修饰N(6)-二甲基烯丙基腺嘌呤(i(6)A(37))和拟尿苷(psi(39))的枯草芽孢杆菌tRNA(Tyr)反密码子臂的溶液结构和热力学性质。 UV熔融和差示扫描量热法表明,修饰稳定了茎,并可能增强了环中碱基的堆积。 i(6)A(37)修饰破坏未修饰反密码子环的氢键网络,该反密码子环包括C(32)-A(38)(+)碱基对和A(37)-U(33)碱基对相互作用。尽管i(6)A(37)修饰增加了环核苷酸的动态性质,但金属离子配位重建了构象均一性。有趣的是,i(6)A(37)修饰和Mg(2+)足以促进大肠杆菌tRNA(Phe)反密码子环的掉头折叠,但这些元素并未导致这种特征tRNA(Tyr)中的反密码子环。

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