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A comprehensive comparison of multiple sequence alignment programs.

机译:多个序列比对程序的全面比较。

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In recent years improvements to existing programs and the introduction of new iterative algorithms have changed the state-of-the-art in protein sequence alignment. This paper presents the first systematic study of the most commonly used alignment programs using BAliBASE benchmark alignments as test cases. Even below the 'twilight zone' at 10-20% residue identity, the best programs were capable of correctly aligning on average 47% of the residues. We show that iterative algorithms often offer improved alignment accuracy though at the expense of computation time. A notable exception was the effect of introducing a single divergent sequence into a set of closely related sequences, causing the iteration to diverge away from the best alignment. Global alignment programs generally performed better than local methods, except in the presence of large N/C-terminal extensions and internal insertions. In these cases, a local algorithm was more successful in identifying the most conserved motifs. This study enables us to propose appropriate alignment strategies, depending on the nature of a particular set of sequences. The employment of more than one program based on different alignment techniques should significantly improve the quality of automatic protein sequence alignment methods. The results also indicate guidelines for improvement of alignment algorithms.
机译:近年来,对现有程序的改进和新迭代算法的引入改变了蛋白质序列比对的最新技术。本文介绍了使用BAliBASE基准比对作为测试用例的最常用比对程序的首次系统研究。即使在“暮光区”的残基同一性为10-20%之下,最好的程序也能够正确对齐平均47%的残基。我们表明,迭代算法通常会提供更高的对齐精度,尽管会浪费计算时间。一个显着的例外是将单个发散序列引入一组紧密相关的序列中的效果,从而导致迭代偏离最佳比对。全局比对程序通常比局部方法执行得更好,除了存在较大的N / C端扩展和内部插入之外。在这些情况下,局部算法在识别最保守的基序方面更为成功。这项研究使我们能够根据特定序列集的性质提出适当的比对策略。使用多个基于不同比对技术的程序可以显着提高自动蛋白质序列比对方法的质量。结果还为改进比对算法提供了指导。

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