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Multiscale complex network of protein conformational fluctuations in single-molecule time series

机译:单分子时间序列中蛋白质构象波动的多尺度复杂网络

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摘要

Conformational dynamics of proteins can be interpreted as itinerant motions as the protein traverses from one state to another on a complex network in conformational space or, more generally, in state space. Here we present a scheme to extract a multiscale state space network (SSN) from a single-molecule time series. Analysis by this method enables us to lift degeneracy—different physical states having the same value for a measured observable—as much as possible. A state or node in the network is defined not by the value of the observable at each time but by a set of subsequences of the observable over time. The length of the subsequence can tell us the extent to which the memory of the system is able to predict the next state. As an illustration, we investigate the conformational fluctutation dynamics probed by single-molecule electron transfer (ET), detected on a photon-by-photon basis. We show that the topographical features of the SSNs depend on the time scale of observation; the longer the time scale, the simpler the underlying SSN becomes, leading to a transition of the dynamics from anomalous diffusion to normal Brownian diffusion.
机译:蛋白质的构象动力学可以解释为迭代运动,因为蛋白质在构象空间中或更普遍地在状态空间中在复杂网络上从一种状态穿越到另一种状态。在这里,我们提出了一种从单分子时间序列中提取多尺度状态空间网络(SSN)的方案。通过这种方法进行的分析使我们能够尽可能地消除简并性-不同的物理状态具有相同的可测量观测值。网络中的状态或节点不是由每次的可观察值决定,而是由随时间变化的可观察子集组成。子序列的长度可以告诉我们系统内存能够预测下一个状态的程度。作为说明,我们研究了在单光子的基础上检测到的单分子电子转移(ET)探测的构象变化动力学。我们表明,SSNs的地形特征取决于观测的时间尺度。时间尺度越长,底层的SSN越简单,从而导致动力学从异常扩散过渡到正常布朗扩散。

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