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生物开关参数空间的映射。

Mapping parameter spaces of biological switches.

机构信息

Department of Chemical and Biological Engineering, Princeton University, Princeton, New Jersey, United States of America.

Lewis-Sigler Institute for Integrative Genomics, Princeton University, Princeton, New Jersey, United States of America.

出版信息

PLoS Comput Biol. 2021 Feb 8;17(2):e1008711. doi: 10.1371/journal.pcbi.1008711. eCollection 2021 Feb.

Abstract

Since the seminal 1961 paper of Monod and Jacob, mathematical models of biomolecular circuits have guided our understanding of cell regulation. Model-based exploration of the functional capabilities of any given circuit requires systematic mapping of multidimensional spaces of model parameters. Despite significant advances in computational dynamical systems approaches, this analysis remains a nontrivial task. Here, we use a nonlinear system of ordinary differential equations to model oocyte selection in Drosophila, a robust symmetry-breaking event that relies on autoregulatory localization of oocyte-specification factors. By applying an algorithmic approach that implements symbolic computation and topological methods, we enumerate all phase portraits of stable steady states in the limit when nonlinear regulatory interactions become discrete switches. Leveraging this initial exact partitioning and further using numerical exploration, we locate parameter regions that are dense in purely asymmetric steady states when the nonlinearities are not infinitely sharp, enabling systematic identification of parameter regions that correspond to robust oocyte selection. This framework can be generalized to map the full parameter spaces in a broad class of models involving biological switches.

摘要

自 1961 年 Monod 和 Jacob 的开创性论文以来,生物分子电路的数学模型一直指导着我们对细胞调控的理解。基于模型的对任何给定电路的功能能力的探索都需要对模型参数的多维空间进行系统的映射。尽管在计算动力系统方法方面取得了重大进展,但这种分析仍然是一项非平凡的任务。在这里,我们使用一个非线性常微分方程组来模拟果蝇卵母细胞的选择,这是一个稳健的对称性破缺事件,依赖于卵母细胞特征因子的自调节定位。通过应用一种实现符号计算和拓扑方法的算法方法,我们在非线性调节相互作用变为离散开关时,枚举稳定稳定状态的所有相图。利用这个初始的精确分区,并进一步使用数值探索,我们找到了参数区域,当非线性不是无限尖锐时,在纯不对称稳定状态中是密集的,从而能够系统地识别与稳健卵母细胞选择相对应的参数区域。该框架可以推广到映射涉及生物开关的广泛模型类的完整参数空间。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d3db/7895388/6505f14e79a4/pcbi.1008711.g001.jpg

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