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The use of sequence comparison to detect 'identities' in tRNA genes.

机译:使用序列比较来检测tRNA基因中的“身份”。

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We have developed a computational method that detects 'identities' in tRNA genes by using principal component analysis to classify the sequences of bases in tRNA genes into groups of similar sequences and then comparing the distribution of sequences of bases, in order to extract characteristic bases that are conserved within a group but differ between groups. These classification and comparison procedures are applied recursively to classify the sequences into hierarchical groups, so that multiple levels of characteristic sites can be detected. By using this computational method, we were able to detect many characteristic sites in the T and D domains of tRNAs, as well as the characteristic sites that had already been detected experimentally. This suggests that bases not only in the contact regions but also in the elbow regions, which determine the structure and dynamics of the whole tRNA molecule, are important to the tRNA-aminoacyl tRNA synthetase recognition.
机译:我们已经开发出一种计算方法,该方法通过使用主成分分析将tRNA基因中的碱基序列分为相似序列组,然后比较碱基序列的分布,从而提取出特征性碱基来检测tRNA基因中的“身份”。在组内是保守的,但组之间是不同的。这些分类和比较过程将递归应用,以将序列分类为分层组,以便可以检测到多个级别的特征位点。通过使用这种计算方法,我们能够检测tRNA的T和D结构域中的许多特征位点,以及已经通过实验检测到的特征位点。这表明,不仅确定接触区域而且确定肘区域的碱基,对于整个tRNA分子的结构和动力学也很重要,这对于tRNA-氨酰基tRNA合成酶的识别至关重要。

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