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无参数方法区分Wnt信号通路模型并指导实验设计。

Parameter-free methods distinguish Wnt pathway models and guide design of experiments.

作者信息

MacLean Adam L, Rosen Zvi, Byrne Helen M, Harrington Heather A

机构信息

Mathematical Institute, University of Oxford, Oxford OX2 6GG, United Kingdom;

Department of Mathematics, University of California, Berkeley, CA 94720; and.

出版信息

Proc Natl Acad Sci U S A. 2015 Mar 3;112(9):2652-7. doi: 10.1073/pnas.1416655112. Epub 2015 Feb 17.

Abstract

The canonical Wnt signaling pathway, mediated by β-catenin, is crucially involved in development, adult stem cell tissue maintenance, and a host of diseases including cancer. We analyze existing mathematical models of Wnt and compare them to a new Wnt signaling model that targets spatial localization; our aim is to distinguish between the models and distill biological insight from them. Using Bayesian methods we infer parameters for each model from mammalian Wnt signaling data and find that all models can fit this time course. We appeal to algebraic methods (concepts from chemical reaction network theory and matroid theory) to analyze the models without recourse to specific parameter values. These approaches provide insight into aspects of Wnt regulation: the new model, via control of shuttling and degradation parameters, permits multiple stable steady states corresponding to stem-like vs. committed cell states in the differentiation hierarchy. Our analysis also identifies groups of variables that should be measured to fully characterize and discriminate between competing models, and thus serves as a guide for performing minimal experiments for model comparison.

摘要

由β-连环蛋白介导的经典Wnt信号通路在发育、成体干细胞组织维持以及包括癌症在内的许多疾病中都起着至关重要的作用。我们分析了现有的Wnt数学模型,并将它们与一个针对空间定位的新Wnt信号模型进行比较;我们的目的是区分这些模型并从中提炼出生物学见解。使用贝叶斯方法,我们从哺乳动物Wnt信号数据中推断出每个模型的参数,发现所有模型都能拟合这个时间进程。我们借助代数方法(化学反应网络理论和拟阵理论的概念)来分析这些模型,而无需依赖特定的参数值。这些方法为Wnt调节的各个方面提供了见解:新模型通过控制穿梭和降解参数,允许对应于分化层次中干细胞样与定向细胞状态的多个稳定稳态。我们的分析还确定了为全面表征和区分竞争模型而应测量的变量组,从而为进行模型比较的最小实验提供了指导。

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