Mechanisms and mathematical modeling of ROS production by the mitochondrial electron transport chain
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Publication year
2022Source
American Journal of Physiology : Cell Physiology, 323, 1, (2022), pp. C69-c83ISSN
Publication type
Article / Letter to editor
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Organization
Biochemistry (UMC)
Paediatrics
Journal title
American Journal of Physiology : Cell Physiology
Volume
vol. 323
Issue
iss. 1
Page start
p. C69
Page end
p. c83
Subject
Radboudumc 6: Metabolic Disorders RIMLS: Radboud Institute for Molecular Life Sciences; Paediatrics - Radboud University Medical CenterAbstract
Reactive oxygen species (ROS) are recognized both as damaging molecules and intracellular signaling entities. In addition to its role in ATP generation, the mitochondrial electron transport chain (ETC) constitutes a relevant source of mitochondrial ROS, in particular during pathological conditions. Mitochondrial ROS homeostasis depends on species- and site-dependent ROS production, their bioreactivity, diffusion, and scavenging. However, our quantitative understanding of mitochondrial ROS homeostasis has thus far been hampered by technical limitations, including a lack of truly site- and/or ROS-specific reporter molecules. In this context, the use of computational models is of great value to complement and interpret empirical data, as well as to predict variables that are difficult to assess experimentally. During the past decades, various mechanistic models of ETC-mediated ROS production have been developed. Although these often-complex models have generated novel insights, their parameterization, analysis, and integration with other computational models are not straightforward. In contrast, phenomenological (sometimes termed "minimal") models use a relatively small set of equations to describe empirical relationship(s) between ROS-related and other parameters and generally aim to explore system behavior and generate hypotheses for experimental validation. In this review, we first discuss ETC-linked ROS homeostasis and introduce various detailed mechanistic models. Next, we present how bioenergetic parameters (e.g., NADH/NAD(+) ratio and mitochondrial membrane potential) relate to site-specific ROS production within the ETC and how these relationships can be used to design minimal models of ROS homeostasis. Finally, we illustrate how minimal models have been applied to explore pathophysiological aspects of ROS.
This item appears in the following Collection(s)
- Academic publications [243859]
- Electronic publications [130605]
- Faculty of Medical Sciences [92795]
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