Multiscale Modeling of Information Conveyed by Gene-Regulatory Signaling

Michael L. Mayo, K. Pilkiewicz
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引用次数: 2

Abstract

Cells leverage signaling molecules to carry information about the cellular state to receptors that regulate protein synthesis in order to suit the cell's dynamically evolving needs. This regulation remains efficient and robust, despite that substantial stochasticity pervades the sub-cellular environment. In electronic and wireless signaling systems, the mutual information quantifies the extent to which information in a signal can be received across a communications channel. Applying this same metric to gene-regulatory interactions can better clarify how these biological signaling systems mitigate environmental noise. In this paper we study the information-transmission characteristics of a single gene-regulatory interaction by employing an exactly solvable master equation model for the production and degradation of individual proteins. This molecular-scale description is then coupled to a mass-action kinetics model of dynamic protein concentrations in a macroscopic sample of cells, enabling parameter values to be obtained by experiments performed using cell-based assays. We find that the mutual information depends monotonically on two parameters: one which characterizes stochastic variations in the concentration of signaling molecules, and the other the ratio of kinetic production to degradation rates of the regulated protein.
基因调控信号传递信息的多尺度建模
细胞利用信号分子将有关细胞状态的信息传递给调节蛋白质合成的受体,以适应细胞动态进化的需要。尽管亚细胞环境中存在大量的随机性,但这种调控仍然有效而稳健。在电子和无线信号系统中,互信息量化了信号中的信息可以通过通信信道接收的程度。将相同的度量应用于基因调控相互作用可以更好地阐明这些生物信号系统如何减轻环境噪声。在本文中,我们研究了单基因调控相互作用的信息传递特征,采用了一个精确可解的主方程模型,用于单个蛋白质的产生和降解。然后,将这种分子尺度的描述与宏观细胞样本中动态蛋白质浓度的质量作用动力学模型相耦合,从而通过使用基于细胞的分析进行的实验获得参数值。我们发现互信息单调地依赖于两个参数:一个是表征信号分子浓度随机变化的参数,另一个是被调节蛋白质的动力学生产与降解率的比值。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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