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首页> 外文期刊>The journal of physical chemistry, B. Condensed matter, materials, surfaces, interfaces & biophysical >Maximum Caliber Can Build and Infer Models of Oscillation in a Three-Gene Feedback Network
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Maximum Caliber Can Build and Infer Models of Oscillation in a Three-Gene Feedback Network

机译:最大水平可以在三基因反馈网络中构建和推断振荡模型

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Single-cell protein expression time trajectories provide rich temporal data quantifying cellular variability and its role in dictating fitness. However, theoretical models to analyze and fully extract information from these measurements remain limited for three reasons: (i) gene expression profiles are noisy, rendering models of averages inapplicable, (ii) experiments typically measure only a few protein species while leaving other molecular actors-necessary to build traditional bottom-up models-unnoticed, and (iii) measured data are in fluorescence, not particle number. We recently addressed these challenges in an alternate top-down approach using the principle of Maximum Caliber (MaxCal) to model genetic switches with one and two protein species. In the present work we address scalability and broader applicability of MaxCal by extending to a three-gene (A, B, C) feedback network that exhibits oscillation, commonly known as the repressilator. We test MaxCal's inferential power by using synthetic data of noisy protein number time traces-serving as a proxy for experimental data-generated from a known underlying model. We notice that the minimal MaxCal model-accounting for production, degradation, and only one type of symmetric coupling between all three species-reasonably infers several underlying features of the circuit such as the effective production rate, degradation rate, frequency of oscillation, and protein number distribution. Next, we build models of higher complexity including different levels of coupling between A, B, and C and rigorously assess their relative performance. While the minimal model (with four parameters) performs remarkably well, we note that the most complex model (with six parameters) allowing all possible forms of crosstalk between A, B, and C slightly improves prediction of rates, but avoids ad hoc assumption of all the other models. It is also the model of choice based on Bayesian information criteria. We further analyzed time trajectories in arbitrary fluorescence (using synthetic trajectories) to mimic realistic data. We conclude that even with a three-protein system including both fluorescence noise and intrinsic gene expression fluctuations, MaxCal can faithfully infer underlying details of the network, opening future directions to model other network motifs with many species.
机译:单细胞蛋白表达时间轨迹提供丰富的时间数据量量化蜂窝变异性及其在规定的健身中的作用。然而,从这些测量的分析和完全提取信息的理论模型仍然有限限制:(i)基因表达谱是嘈杂的,渲染平均值不适用的模型,(ii)实验通常只测量少量蛋白质物种,同时留下其他分子作用 - 必须建立传统的自下而上模型 - 未被注意(III)测量数据在荧光,而不是粒子数。我们最近使用最大口径(MAXCAL)的原理来解决这些挑战,使用最大口径(MAXCAL)来模拟遗传开关与一种和两种蛋白质。在本工作中,我们通过延伸到展示振荡的三种基因(A,B,C)反馈网络来解决MaxCal的可扩展性和更广泛的适用性,该网络通常称为抑郁符。通过使用嘈杂的蛋白质数时间迹线的合成数据来测试MaxCal的推理能力 - 用作从已知的底层模型产生的实验数据的代理。我们注意到最小的MAXCAL模型 - 占生产,降级和所有三种物种之间的一个对称耦合 - 合理的电路的几个底层特征,例如有效的生产率,降解率,振荡频率和蛋白质号码分布。接下来,我们构建具有较高复杂性的模型,包括A,B和C之间的不同耦合水平,并严格评估它们的相对性能。虽然最小模型(具有四个参数)表现出显着良好,但我们注意到最复杂的模型(具有六个参数),允许在A,B和C之间的所有可能形式的串扰略微提高速率预测,但避免了临时假设所有其他型号。它也是基于贝叶斯信息标准的选择模式。我们进一步分析了任意荧光(使用合成轨迹)的时间轨迹来模仿现实数据。我们得出结论,即使具有三种蛋白质系统,包括荧光噪声和内在基因表达波动,Maxcal也可以忠实地推断网络的底层细节,开放未来的方向,以利用许多物种建模其他网络图案。

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