Kinetics and control of oxidative phosphorylation in rat liver mitochondria after dexamethasone treatment

The present investigation was undertaken in order to evaluate the contributions of ATP synthesis and proton leak reactions to the rate of active respiration of liver mitochondria, which is altered following dexamethasone treatment (1.5 mg/kg per day for 5 days). We applied top-down metabolic control analysis and its extension, elasticity analysis, to gain insight into the mechanisms of glucocorticoid regulation of mitochondrial bioenergetics. Liver mitochondria were isolated from dexamethasone-treated, pair-fed and control rats when in a fed or overnight fasted state. Injection of dexamethasone for 5 days resulted in an increase in the fraction of the proton cycle of phosphorylating liver mitochondria, which was associated with a decrease in the efficiency of the mitochondrial oxidative phosphorylation process in liver. This increase in proton leak activity occurred with little change in the mitochondrial membrane potential, despite a significant decrease in the rate of oxidative phosphorylation. Regulation analysis indicates that mitochondrial membrane potential homoeostasis is achieved by equal inhibition of the mitochondrial substrate oxidation and phosphorylation reactions in rats given dexamethasone. Our results also suggest that active liver mitochondria from dexamethasone-treated rats are capable of maintaining phosphorylation flux for cellular purposes, despite an increase in the energetic cost of mitochondrial ATP production due to increased basal proton permeability of the inner membrane. They also provide a complete description of the effects of dexamethasone treatment on liver mitochondrial bioenergetics.

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Field Value
Source ISSN: 0264-6021
Author Roussel, D., Dumas, J.F., Simard, G., Malthiery, Y., Ritz, P.
Maintainer CCSD
Last Updated May 19, 2026, 11:07 (UTC)
Created May 19, 2026, 11:07 (UTC)
Identifier hal-00069604
Language en
contributor Expression des gènes des phosphorylations oxydatives mitochondriales. Maintenance de l'ADN MT ; Institut National de la Santé et de la Recherche Médicale (INSERM)
creator Roussel, D.
date 2004-05-19T00:00:00
harvest_object_id aaa98fe1-c8a7-4aa9-965a-7e5281fa6df0
harvest_source_id 3374d638-d20b-4672-ba96-a23232d55657
harvest_source_title test moissonnage SELUNE
metadata_modified 2024-05-07T00:00:00
relation info:eu-repo/semantics/altIdentifier/doi/10.1042/BJ20040696
set_spec type:ART