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用于代谢控制的合成基因回路中的噪声传播。

Noise propagation in synthetic gene circuits for metabolic control.

作者信息

Oyarzún Diego A, Lugagne Jean-Baptiste, Stan Guy-Bart V

机构信息

Department of Mathematics, ‡Centre for Synthetic Biology and Innovation, Department of Bioengineering, Imperial College London , London SW7 2AZ, United Kingdom.

出版信息

ACS Synth Biol. 2015 Feb 20;4(2):116-25. doi: 10.1021/sb400126a. Epub 2014 May 1.

Abstract

Dynamic control of enzyme expression can be an effective strategy to engineer robust metabolic pathways. It allows a synthetic pathway to self-regulate in response to changes in bioreactor conditions or the metabolic state of the host. The implementation of this regulatory strategy requires gene circuits that couple metabolic signals with the genetic machinery, which is known to be noisy and one of the main sources of cell-to-cell variability. One of the unexplored design aspects of these circuits is the propagation of biochemical noise between enzyme expression and pathway activity. In this article, we quantify the impact of a synthetic feedback circuit on the noise in a metabolic product in order to propose design criteria to reduce cell-to-cell variability. We consider a stochastic model of a catalytic reaction under negative feedback from the product to enzyme expression. On the basis of stochastic simulations and analysis, we show that, depending on the repression strength and promoter strength, transcriptional repression of enzyme expression can amplify or attenuate the noise in the number of product molecules. We obtain analytic estimates for the metabolic noise as a function of the model parameters and show that noise amplification/attenuation is a structural property of the model. We derive an analytic condition on the parameters that lead to attenuation of metabolic noise, suggesting that a higher promoter sensitivity enlarges the parameter design space. In the theoretical case of a switch-like promoter, our analysis reveals that the ability of the circuit to attenuate noise is subject to a trade-off between the repression strength and promoter strength.

摘要

动态控制酶的表达可能是构建稳健代谢途径的有效策略。它能使合成途径根据生物反应器条件的变化或宿主的代谢状态进行自我调节。实施这种调控策略需要将代谢信号与遗传机制相耦合的基因回路,而遗传机制存在噪声,是细胞间变异性的主要来源之一。这些回路尚未探索的设计方面之一是酶表达与途径活性之间生化噪声的传播。在本文中,我们量化了合成反馈回路对代谢产物噪声的影响,以便提出降低细胞间变异性的设计标准。我们考虑了一个在产物对酶表达的负反馈下催化反应的随机模型。基于随机模拟和分析,我们表明,根据抑制强度和启动子强度,酶表达的转录抑制可以放大或减弱产物分子数量的噪声。我们获得了作为模型参数函数的代谢噪声的解析估计,并表明噪声放大/减弱是模型的一种结构特性。我们推导了导致代谢噪声减弱的参数的解析条件,表明较高的启动子敏感性会扩大参数设计空间。在类似开关的启动子的理论情况下,我们的分析表明,回路减弱噪声的能力在抑制强度和启动子强度之间存在权衡。

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