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Spectrum Alignment: Efficient Resequencing by Hybridization

机译:光谱对齐:杂交高效重新排列

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Recent high-density microarray technologies allow, in principle, the determination of all k-mers that appear along a DNA sequence, for k = 8-10 in a single experiment on a standard chip. The k-mer contents, also called the spectrum of the sequence, is not sufficient to uniquely reconstruct a sequence longer than a few hundred bases. We have devised a polynomial algorithm that reconstructs the sequence, given the spectrum and a homologous sequence. This situation occurs, for example, in the identification of single nucleotide polymorphisms (SNPs, and whenever a homologue of the target sequence is known. The algorithm is robust, can handle errors in the spectrum and assumes no knowledge of the k-mer multiplicities. Our simulations show that with realistic levels of SNPs, the algorithm correctly reconstructs a target sequence of length up to 2000 nucleotides when a polymorphic sequence is known. The technique is generalized to handle profiles and HMMs as input instead of a single homologous sequence.
机译:最近的高密度微阵列技术原则上允许沿DNA序列出现的所有K-MERS,在标准芯片上的单一实验中k = 8-10。 K-MER内容,也称为序列的频谱,不足以唯一地重建长度超过几百个基础的序列。我们已经设计了一种多项式算法,其重建序列,给定光谱和同源序列。例如,在鉴定单一核苷酸多态性(SNP的情况下,这种情况发生这种情况,并且只要靶序列的同源物是已知的。该算法是稳健的,可以处理频谱中的错误,并假设不知道K-MER多倍。我们的模拟表明,当已知多态序列时,该算法正确地重建了高达2000个核苷酸的靶序列。该技术广泛地处理作为输入而不是单一同质序列的分布和HMM。

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