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Proteome-Wide Discovery of Evolutionary Conserved Sequences in Disordered Regions

机译:进化保守序列的全蛋白质组的发现在无序区

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摘要

At least 30% of human proteins are thought to contain intrinsically disordered regions, which lack stable structural conformation. Despite lacking enzymatic functions and having few protein domains, disordered regions are functionally important for protein regulation and contain short linear motifs (short peptide sequences involved in protein-protein interactions), but in most disordered regions, the functional amino acid residues remain unknown. We searched for evolutionarily conserved sequences within disordered regions according to the hypothesis that conservation would indicate functional residues. Using a phylogenetic hidden Markov model (phylo-HMM), we made accurate, specific predictions of functional elements in disordered regions even when these elements are only two or three amino acids long. Among the conserved sequences that we identified were previously known and newly identified short linear motifs, and we experimentally verified key examples, including a motif that may mediate interaction between protein kinase Cbk1 and its substrates. We also observed that hub proteins, which interact with many partners in a protein interaction network, are highly enriched in these conserved sequences. Our analysis enabled the systematic identification of the functional residues in disordered regions and suggested that at least 5% of amino acids in disordered regions are important for function.
机译:至少有30%的人类蛋白质被认为含有内在无序的区域,这些区域缺乏稳定的结构构象。尽管缺乏酶促功能并具有少量蛋白质结构域,无序区域对于蛋白质调节具有功能性重要,并且含有短的线性基序(蛋白质 - 蛋白质相互作用的短肽序列),但在大多数无序区域中,官能氨基酸残基仍然未知。根据保守表明功能残留的假设,我们搜索了在无序区域内的进化状态序列。使用系统发育隐患Markov模型(Phylo-HMM),即使当这些元素只有两个或三个氨基酸,我们也是准确的,特异性地预测失调区域中的功能元素。在我们鉴定的保守序列中,先前已知和新鉴定的短线性基序,以及我们通过实验验证的关键实例,包括可以介导蛋白激酶CBK1及其基材之间的相互作用的基序。我们还观察到,与许多蛋白质相互作用网络中的许多合作伙伴相互作用的轮毂蛋白在这些保守序列中高度富集。我们的分析使无序区域中功能残留物的系统鉴定,并提出了至少5%的无序区域中的氨基酸对于功能很重要。

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