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Systematic parameter estimation in data-rich environments for cell signalling dynamics

机译:用于细胞信号动态的数据丰富环境中的系统参数估计

摘要

Motivation: Computational models of biological signalling networks, based on ordinary differential equations (ODEs), have generated many insights into cellular dynamics, but the model-building process typically requires estimating rate parameters based on experimentally observed concentrations. New proteomic methods can measure concentrations for all molecular species in a pathway; this creates a new opportunity to decompose the optimization of rate parameters.Results: In contrast with conventional parameter estimation methods that minimize the disagreement between simulated and observed concentrations, the SPEDRE method fits spline curves through observed concentration points, estimates derivatives and then matches the derivatives to the production and consumption of each species. This reformulation of the problem permits an extreme decomposition of the high-dimensional optimization into a product of low-dimensional factors, each factor enforcing the equality of one ODE at one time slice. Coarsely discretized solutions to the factors can be computed systematically. Then the discrete solutions are combined using loopy belief propagation, and refined using local optimization. SPEDRE has unique asymptotic behaviour with runtime polynomial in the number of molecules and timepoints, but exponential in the degree of the biochemical network. SPEDRE performance is comparatively evaluated on a novel model of Akt activation dynamics including redox-mediated inactivation of PTEN (phosphatase and tensin homologue).
机译:动机:基于普通微分方程(ODE)的生物信号网络计算模型已对细胞动力学产生了许多见解,但模型构建过程通常需要根据实验观察到的浓度估算速率参数。新的蛋白质组学方法可以测量途径中所有分子种类的浓度。结果:与传统的参数估计方法相比,SPEDRE方法通过观察的浓度点拟合样条曲线,估计导数,然后匹配导数,这与分解速率参数的优化方法相反。每种物种的生产和消费。对问题的这种重新表述允许将高维优化极端分解为低维因子的乘积,每个因子在一个时间片上强制一个ODE相等。可以对这些因素的粗离散解进行系统地计算。然后,使用循环置信度传播组合离散解决方案,并使用局部优化进行完善。 SPEDRE具有独特的渐近行为,在分子数量和时间点上具有运行时多项式,但在生化网络的程度上呈指数级。 SPEDRE性能在Akt激活动力学的新型模型(包括氧化还原介导的PTEN失活(磷酸酶和张力蛋白同源物))上进行了比较评估。

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