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A computational strategy for the prediction of functional linear peptide motifs in proteins

机译:预测蛋白质中功能性线性肽基序的计算策略

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Motivation: Short linear peptide motifs mediate protein-protein interaction, cell compartment targeting and represent the sites of post-translational modification. The identification of functional motifs by conventional sequence searches, however, is hampered by the short length of the motifs resulting in a large number of hits of which only a small portion is functional. Results: We have developed a procedure for the identification of functional motifs, which scores pattern conservation in homologous sequences by taking explicitly into account the sequence similarity to the query sequence. For a further improvement of this method, sequence filters have been optimized to mask those sequence regions containing little or no linear motifs. The performance of this approach was verified by measuring its ability to identify 576 experimentally validated motifs among a total of 15 563 instances in a set of 415 protein sequences. Compared to a random selection procedure, the joint application of sequence filters and the novel scoring scheme resulted in a 9-fold enrichment of validated functional motifs on the first rank. In addition, only half as many hits need to be investigated to recover 75 of the functional instances in our dataset. Therefore, this motif-scoring approach should be helpful to guide experiments because it allows focusing on those short linear peptide motifs that have a high probability to be functional.
机译:动机:短的线性肽基序介导蛋白质-蛋白质相互作用,靶向细胞区室并代表翻译后修饰的位点。然而,通过常规序列搜索对功能性基元的识别受制于基元的短长度,从而导致大量的命中,其中只有一小部分起作用。结果:我们开发了一种识别功能性基序的程序,该程序通过明确考虑与查询序列的序列相似性来对同源序列中的模式保守性进行评分。为了对该方法的进一步改进,已对序列过滤器进行了优化,以掩盖那些包含很少或没有线性基序的序列区域。通过测量其在415个蛋白序列中的总共15563个实例中鉴定576个经过实验验证的基序的能力,验证了该方法的性能。与随机选择程序相比,序列过滤器和新颖的计分方案的联合应用使经过验证的功能基序富集了9倍。此外,只需调查一半的点击量即可恢复我们数据集中的75个功能实例。因此,这种基序评分方法应有助于指导实验,因为它可以集中于那些很有可能起作用的短线性肽基序。

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