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Dynamic Allostery of the Catabolite Activator Protein Revealed by Interatomic Forces

机译:原子间力揭示的分解代谢活化蛋白的动态变构。

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摘要

The Catabolite Activator Protein (CAP) is a showcase example for entropic allostery. For full activation and DNA binding, the homodimeric protein requires the binding of two cyclic AMP (cAMP) molecules in an anti-cooperative manner, the source of which appears to be largely of entropic nature according to previous experimental studies. We here study at atomic detail the allosteric regulation of CAP with Molecular dynamics (MD) simulations. We recover the experimentally observed entropic penalty for the second cAMP binding event with our recently developed force covariance entropy estimator and reveal allosteric communication pathways with Force Distribution Analyses (FDA). Our observations show that CAP binding results in characteristic changes in the interaction pathways connecting the two cAMP allosteric binding sites with each other, as well as with the DNA binding domains. We identified crucial relays in the mostly symmetric allosteric activation network, and suggest point mutants to test this mechanism. Our study suggests inter-residue forces, as opposed to coordinates, as a highly sensitive measure for structural adaptations that, even though minute, can very effectively propagate allosteric signals.
机译:分解代谢活化蛋白(CAP)是熵变构的一个展示实例。对于完全激活和DNA结合,同二聚体蛋白需要以反合作方式结合两个环状AMP(cAMP)分子,根据先前的实验研究,其来源似乎主要是熵性质的。我们在这里详细地研究了分子动力学(MD)模拟的CAP的变构调节。我们用我们最近开发的力协方差熵估计器恢复了第二个cAMP结合事件的实验观察到的熵罚,并用力分布分析(FDA)揭示了变构通讯途径。我们的观察结果表明,CAP结合会导致连接两个cAMP变构结合位点以及DNA结合域的相互作用途径发生特征性变化。我们在大多数对称的变构激活网络中确定了关键的继电器,并建议使用点突变体来测试这种机制。我们的研究表明,与坐标相反,残基间力是对结构适应性的高度敏感的度量,即使很小,也可以非常有效地传播变构信号。

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