囊泡上单酶反应动力学:底物聚集的作用

V. Zhdanov, V. Zhdanov
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引用次数: 1

摘要

在体内脂质膜上发生的酶促反应可受到各种因素的影响,包括大分子拥挤,特别是底物聚集。在学术研究中,这些因素的作用可以通过跟踪单个脂质囊泡上发生的单酶动力学实验来澄清。为了扩展此类实验的概念基础,我们在此从数学上分析了相应的动力学,重点是底物聚集的作用。一般来说,聚合可能发生在不同的长度尺度上。例如,小聚集体可能包含一些蛋白质或肽,而大聚集体可能是介观的,如在脂质结构域的情况下,脂质结构域可以在由不同脂质组成的膜中形成。我们提出了一个动力学模型,全面描述了前一种类型的聚集对反应速率对底物膜浓度的依赖性的影响。在物理参数合理的情况下得到的结果表明,与传统的Michaelis-Menten动力学相比,聚集相关的偏差可能是明显的。特刊评论:这篇理论文章关注的是与底物聚集在单个囊泡上平行发生的单酶反应。这个主题与一些关于酶动力学和随机动力学的功能和数学方面的特刊文章有关。
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Kinetics of single-enzyme reactions on vesicles: Role of substrate aggregation
Enzymatic reactions occurring in vivo on lipid membranes can be influenced by various factors including macromolecular crowding in general and substrate aggregation in particular. In academic studies, the role of these factors can experimentally be clarified by tracking single-enzyme kinetics occurring on individual lipid vesicles. To extend the conceptual basis for such experiments, we analyze herein the corresponding kinetics mathematically with emphasis on the role of substrate aggregation. In general, the aggregation may occur on different length scales. Small aggregates may e.g. contain a few proteins or peptides while large aggregates may be mesoscopic as in the case of lipid domains which can be formed in the membranes composed of different lipids. We present a kinetic model describing comprehensively the effect of aggregation of the former type on the dependence of the reaction rate on substrate membrane concentration. The results obtained with physically reasonable parameters indicate that the aggregation-related deviations from the conventional Michaelis-Menten kinetics may be appreciable. Special Issue Comments: This theoretical article is focused on single-enzyme reactions occurring in parallel with substrate aggregation on individual vesicles. This subject is related to a few Special Issue articles concerning enzyme dynamics and function and mathematical aspects of stochastic kinetics.
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