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首页> 外文期刊>Mathematical Biosciences: An International Journal >The quasi-steady-state approximations revisited: Timescales, small parameters, singularities, and normal forms in enzyme kinetics
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The quasi-steady-state approximations revisited: Timescales, small parameters, singularities, and normal forms in enzyme kinetics

机译:重新审议的准稳态近似值:酶动力学中的时间尺度,小参数,奇点和正常形式

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摘要

In this work, we revisit the scaling analysis and commonly accepted conditions for the validity of the standard, reverse and total quasi-steady-state approximations through the lens of dimensional Tikhonov-Fenichel parameters and their respective critical manifolds. By combining Tikhonov-Fenichel parameters with scaling analysis and energy methods, we derive improved upper bounds on the approximation error for the standard, reverse and total quasi-steady-state approximations. Furthermore, previous analyses suggest that the reverse quasi-steady-state approximation is only valid when initial enzyme concentrations greatly exceed initial substrate concentrations. However, our results indicate that this approximation can be valid when initial enzyme and substrate concentrations are of equal magnitude. Using energy methods, we find that the condition for the validity of the reverse quasi-steady-state approximation is far less restrictive than was previously assumed, and we derive a new "small" parameter that determines the validity of this approximation. In doing so, we extend the established domain of validity for the reverse quasi-steady-state approximation. Consequently, this opens up the possibility of utilizing the reverse quasi-steady-state approximation to model enzyme catalyzed reactions and estimate kinetic parameters in enzymatic assays at much lower enzyme to substrate ratios than was previously thought. Moreover, we show for the first time that the critical manifold of the reverse quasi-steady-state approximation contains a singular point where normal hyperbolicity is lost. Associated with this singularity is a transcritical bifurcation, and the corresponding normal form of this bifurcation is recovered through scaling analysis.
机译:在这项工作中,我们通过尺寸Tikhonov-Fenichel参数及其各自的关键歧管来重新求解标准,反向和总准稳态近似的有效性的缩放分析和常识条件。通过将Tikhonov-Fenichel参数与缩放分析和能量方法组合,我们在标准,反向和总准稳态近似的近似误差上获得了改进的上限。此外,先前的分析表明,当初始酶浓度大大超过初始衬底浓度时,反向准稳态近似仅有效。然而,我们的结果表明,当初始酶和衬底浓度相等时,该近似可能是有效的。使用能量方法,我们发现反向准稳态近似的有效性的条件远远不如先前假设的限制,我们得出了一种确定该近似的有效性的新的“小”参数。在这样做时,我们将建立的有效领域扩展到反向准稳态近似。因此,这开辟了利用反向准稳态近似的可能性与模型酶催化反应,并在酶法中估计动力学参数,比以前认为碱基比的酶比碱基比较。此外,我们首次展示了反向准稳态近似的关键歧管包含常规双曲性丢失的奇点。与这种奇点相关的是跨临界分叉,通过缩放分析回收该分叉的相应正常形式。

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