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Analysis of genomic tRNA sets from Bacteria, Archaea, and Eukarya points to anticodon–codon hydrogen bonds as a major determinant of tRNA compositional variations

机译:来自细菌,古细菌和真核生物的基因组tRNA集的分析指出,反密码子-密码子氢键是tRNA组成变异的主要决定因素

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摘要

Analysis of 100 complete sets of the cytoplasmic elongator tRNA genes from Bacteria, Archaea, and Eukarya pointed to correspondences between types of anticodon and composition of the rest of the tRNA body. The number of the hydrogen bonds formed between the complementary nucleotides in the anticodon–codon duplex appeared as a major quantitative parameter determining covariations in all three domains of life. Our analysis has supported and advanced the “extended anticodon” concept that is based on the argument that the decoding performance of the anticodon is enhanced by selection of a matching anticodon stem–loop sequence, as reported by Yarus in 1982. In addition to the anticodon stem–loop, we have found covariations between the anticodon nucleotides and the composition of the distant regions of their respective tRNAs that include dihydrouridine (D) and thymidyl (T) stem–loops. The majority of the covariable tRNA positions were found at the regions with the increased dynamic potential—such as stem–loop and stem–stem junctions. The consistent occurrences of the covariations on the multigenomic level suggest that the number and pattern of the hydrogen bonds in the anticodon–codon duplex constitute a major factor in the course of translation that is reflected in the fine-tuning of the tRNA composition and structure.
机译:对来自细菌,古细菌和真核生物的100套完整的胞质延伸子tRNA基因的分析指出了反密码子类型与其余tRNA体组成之间的对应关系。反密码子-密码子双链体中互补核苷酸之间形成的氢键数目似乎是决定生命中所有三个域中协变的主要定量参数。我们的分析支持并提出了“扩展反密码子”概念,该概念基于这样的论点,即通过选择匹配的反密码子茎-环序列来增强反密码子的解码性能,正如Yarus在1982年所报道的那样。茎环,我们发现了反密码子核苷酸与它们各自的tRNA远端区域组成之间的协变,包括二氢尿苷(D)和胸苷(T)茎环。大多数协变量tRNA位置位于动态潜力增加的区域,例如茎环和茎干连接处。在多基因组水平上协变的一致出现表明,反密码子-密码子双链体中氢键的数量和样式是翻译过程中的主要因素,这反映在tRNA组成和结构的微调中。

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