首页> 外文会议>Research in Computational Molecular Biology; Lecture Notes in Bioinformatics; 4453 >Free Energy Estimates of All-Atom Protein Structures Using Generalized Belief Propagation
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Free Energy Estimates of All-Atom Protein Structures Using Generalized Belief Propagation

机译:使用广义信念传播的全原子蛋白质结构的自由能估计

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We present a technique for approximating the free energy of protein structures using Generalized Belief Propagation (GBP). The accuracy and utility of these estimates are then demonstrated in two different application domains. First, we show that the entropy component of our free energy estimates can be useful in distinguishing native protein structures from decoys — structures with similar internal energy to that of the native structure, but otherwise incorrect. Our method is able to correctly identify the native fold from among a set of decoys with 87.5% accuracy over a total of 48 different immunoglobin folds. The remaining 12.5% of native structures are ranked among the top 4 of all structures. Second, we show that our estimates of AAG upon mutation upon mutation for three different data sets have linear correlations between 0.63-0.70 with experimental values and statistically significant p-values. Together, these results suggests that GBP is an effective means for computing free energy in all-atom models of protein structures. GBP is also efficient, taking a few minutes to run on a typical sized protein, further suggesting that GBP may be an attractive alternative to more costly molecular dynamic simulations for some tasks.
机译:我们提出了一种使用广义信念传播(GBP)近似蛋白质结构自由能的技术。然后,在两个不同的应用领域中证明了这些估计的准确性和实用性。首先,我们表明,我们的自由能估计量的熵成分可用于区分天然蛋白质结构与诱饵-内部能量与天然结构相似但又不正确的结构。我们的方法能够从一组诱饵中正确识别天然折叠,准确度为87.5%,覆盖总共48种不同的免疫球蛋白折叠。其余的12.5%的本地结构位于所有结构的前4名中。第二,我们表明我们对三个不同数据集进行突变后的AAG估算值在0.63-0.70与实验值和统计学上显着的p值之间具有线性关系。总之,这些结果表明,GBP是一种在蛋白质结构的所有原子模型中计算自由能的有效手段。 GBP也是有效的,需要花费几分钟才能运行典型大小的蛋白质,这进一步表明,GBP对于某些任务而言可能是更昂贵的分子动力学模拟的诱人替代品。

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