Markov state models (MSMs) have been successful in computing metastable states, slow relaxation timescales and associated structural changes, and stationary or kinetic experimental observables of complex molecules from large amounts of molecular dynamics simulation data. However, MSMs approximate the true dynamics by assuming a Markov chain on a clusters discretization of the state space. This approximation is difficult to make for high-dimensional biomolecular systems, and the quality and reproducibility of MSMs has, therefore, been limited. Here, we discard the assumption that dynamics are Markovian on the discrete clusters. Instead, we only assume that the full phase-space molecular dynamics is Markovian, and a projection of this full dynamics is observed on the discrete states, leading to the concept of Projected Markov Models (PMMs). Robust estimation methods for PMMs are not yet available, but we derive a practically feasible approximation via Hidden Markov Models (HMMs). It is shown how various molecular observables of interest that are often computed from MSMs can be computed from HMMs/PMMs. The new framework is applicable to both, simulation and single-molecule experimental data. We demonstrate its versatility by applications to educative model systems, a 1 ms Anton MD simulation of the bovine pancreatic trypsin inhibitor protein, and an optical tweezer force probe trajectory of an RNA hairpin.
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机译:马尔可夫状态模型(MSM)已成功地从大量的分子动力学模拟数据计算出亚稳态,缓慢的弛豫时间尺度和相关的结构变化以及复杂分子的稳态或动力学实验观测值。但是,MSM通过假设状态空间的群集离散化上的马尔可夫链来近似真实的动力学。对于高维生物分子系统而言,这种近似很难实现,因此,MSM的质量和可重复性受到限制。在这里,我们放弃了在离散簇上动力学是马尔可夫的假设。取而代之的是,我们仅假设完整的相空间分子动力学是马尔可夫模型,并且在离散状态下观察到了完整的动力学模型,从而提出了投影马尔可夫模型(PMM)的概念。 PMM的稳健估计方法尚不可用,但是我们通过隐马尔可夫模型(HMM)得出了一种切实可行的近似值。显示了如何从HMM / PMM中计算出经常从MSM中计算出的各种感兴趣的分子可观察物。新框架适用于模拟和单分子实验数据。我们通过将其应用到教育模型系统,牛胰胰蛋白酶抑制剂蛋白的1 ms Anton MD模拟以及RNA发夹的光学镊子力探针轨迹来证明其多功能性。
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