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Ensemble-Based Analysis of the Dynamic Allostery in the PSD-95 PDZ3 Domain in Relation to the General Variability of PDZ Structures

机译:基于合奏的PSD-95 PDZ3域的动态仿生分析与PDZ结构一般可变性的关系

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PDZ domains are abundant interaction hubs found in a number of different proteins and they exhibit characteristic differences in their structure and ligand specificity. Their internal dynamics have been proposed to contribute to their biological activity via changes in conformational entropy upon ligand binding and allosteric modulation. Here we investigate dynamic structural ensembles of PDZ3 of the postsynaptic protein PSD-95, calculated based on previously published backbone and side-chain S 2 order parameters. We show that there are distinct but interdependent structural rearrangements in PDZ3 upon ligand binding and the presence of the intramolecular allosteric modulator helix α 3. We have also compared these rearrangements in PDZ1-2 of PSD-95 and the conformational diversity of an extended set of PDZ domains available in the PDB database. We conclude that although the opening-closing rearrangement, occurring upon ligand binding, is likely a general feature for all PDZ domains, the conformer redistribution upon ligand binding along this mode is domain-dependent. Our findings suggest that the structural and functional diversity of PDZ domains is accompanied by a diversity of internal motional modes and their interdependence.
机译:PDZ结构域是在许多不同蛋白质中发现的丰富相互作用的集线器,并且它们具有其结构和配体特异性的特征差异。已经提出了它们的内部动力学通过组合熵对配体结合和变构调制的变化有助于它们的生物活性。在这里,我们研究了基于先前公布的骨干和侧链S 2阶参数计算的突触蛋白PSD-95的动态结构集合。我们表明,在配体结合时,PDZ3中存在明显但相互依存的结构重排,并且分子内变形调节剂螺旋α3的存在。我们还在PSD-95的PDZ1-2中与这些重排和延伸组的构象多样性进行了比较了这些重排。 PDB数据库中可用的PDZ域。我们得出结论,尽管在配体结合时发生的开口重排部可能是所有PDZ结构域的一般特征,但是沿着该模式的配体结合时的符合子再分配是畴依赖性的。我们的研究结果表明,PDZ域的结构和功能多样性伴随着内部运动模式的多样性及其相互依赖性。

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