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Identification of genomic features using microsyntenies of domains: Domain teams

机译:使用领域的微观同义来鉴定基因组特征:领域团队

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摘要

The detection, across several genomes, of local conservation of gene content and proximity considerably helps the prediction of features of interest, such as gene fusions or physical and functional interactions. Here, we want to process realistic models of chromosomes, in which genes (or genomic segments of several genes) can be duplicated within a chromosome, or be absent from some other chromosome(s). Our approach adopts the technique of temporarily forgetting genes and working directly with protein “domains” such as those found in Pfam. This allows the detection of strings of domains that are conserved in their content, but not necessarily in their order, which we refer to as domain teams. The prominent feature of the method is that it relaxes the rigidity of the orthology criterion and avoids many of the pitfalls of gene-families identification methods, often hampered by multidomain proteins or low levels of sequence similarity. This approach, that allows both inter- and intrachromosomal comparisons, proves to be more sensitive than the classical methods based on pairwise sequence comparisons, particularly in the simultaneous treatment of many species. The automated and fast detection of domain teams, together with its increased sensitivity at identifying segments of identical (protein-coding) gene contents as well as gene fusions, should prove a useful complement to other existing methods.
机译:跨多个基因组检测基因含量和邻近性的局部保守性,可以大大帮助预测目标特征,例如基因融合或物理和功能相互作用。在这里,我们要处理现实的染色体模型,其中的基因(或几个基因的基因组片段)可以在染色体内复制,也可以不在某些其他染色体上。我们的方法采用暂时忘记基因并直接与蛋白质“结构域”(例如Pfam中发现的结构域)一起工作的技术。这允许检测在内容中保留但不一定在其顺序中保守的域名字符串,我们将其称为域名团队。该方法的突出特点是,它放宽了矫正标准的刚性,避免了许多通常被多域蛋白或低水平序列相似性阻碍的基因家族鉴定方法的陷阱。这种方法允许进行染色体间和染色体内比较,事实证明它比基于成对序列比较的经典方法更为灵敏,尤其是在同时处理许多物种时。领域团队的自动化和快速检测,以及在识别相同(蛋白质编码)基因内容片段以及基因融合方面提高的敏感性,应证明是对其他现有方法的有益补充。

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