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Residues crucial for maintaining short paths in network communication mediate signaling in proteins

机译:对维持网络通信中的短路径至关重要的残基介导蛋白质中的信号传导

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摘要

Here, we represent protein structures as residue interacting networks, which are assumed to involve a permanent flow of information between amino acids. By removal of nodes from the protein network, we identify fold centrally conserved residues, which are crucial for sustaining the shortest pathways and thus play key roles in long-range interactions. Analysis of seven protein families (myoglobins, G-protein-coupled receptors, the trypsin class of serine proteases, hemoglobins, oligosaccharide phosphorylases, nuclear receptor ligand-binding domains and retroviral proteases) confirms that experimentally many of these residues are important for allosteric communication. The agreement between the centrally conserved residues, which are key in preserving short path lengths, and residues experimentally suggested to mediate signaling further illustrates that topology plays an important role in network communication. Protein folds have evolved under constraints imposed by function. To maintain function, protein structures need to be robust to mutational events. On the other hand, robustness is accompanied by an extreme sensitivity at some crucial sites. Thus, here we propose that centrally conserved residues, whose removal increases the characteristic path length in protein networks, may relate to the system fragility.
机译:在这里,我们将蛋白质结构表示为残基相互作用网络,假定它们涉及氨基酸之间的永久信息流。通过从蛋白质网络中删除节点,我们识别出折叠的中央保守残基,这对于维持最短途径至关重要,因此在远距离相互作用中起关键作用。对七个蛋白质家族(肌球蛋白,G蛋白偶联受体,丝氨酸蛋白酶的胰蛋白酶类,血红蛋白,寡糖磷酸化酶,核受体配体结合域和逆转录病毒蛋白酶)的分析证实,从实验上讲,这些残基中的许多对变构通讯很重要。中央保守残基之间的一致性是保持短路径长度的关键,而实验上建议的残基可以介导信号传导,这进一步说明拓扑在网络通信中起着重要作用。蛋白质折叠是在功能限制下进化的。为了维持功能,蛋白质结构必须对突变事件具有鲁棒性。另一方面,在某些关键位置,鲁棒性伴随着极大的敏感性。因此,在此我们提出集中保留的残基(其去除会增加蛋白质网络中特征路径的长度)可能与系统的脆弱性有关。

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