Bile Acids Affect Liver Mitochondrial Bioenergetics: Possible Relevance for Cholestasis Therapy

doi:10.1093/toxsci/57.1.177

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Toxicological Sciences 57, 177-185 (2000)
Copyright © 2000 by the Society of Toxicology

Systems Toxicology

Bile Acids Affect Liver Mitochondrial Bioenergetics: Possible Relevance for Cholestasis Therapy

Anabela P. Rolo¹, Paulo J. Oliveira, António J. M. Moreno and Carlos M. Palmeira²

Center for Neurosciences and Cell Biology of Coimbra, Department of Zoology, University of Coimbra, 3004–517 Coimbra, Portugal

It has been pointed out that intracellular accumulation of bileacids cause hepatocyte injury in cholestatic disease process.This study was aimed to test if cytotoxicity of these compoundsis mediated through mitochondria dysfunction. Bile acids effectson isolated rat liver mitochondrial were analyzed by monitoringchanges in membrane potential and mitochondrial respiration,as well as alterations in H⁺ membrane permeability and mitochondrialpermeability transition pore induction. Increasing concentrationsof the bile acids litocholic (LCA), deoxycholic (DCA), ursodeoxycholic(UDCA), chenodeoxycholic (CDCA), glycochenodeoxycholic (GCDC),or taurochenodeoxycholic (TCDC) decrease transmembrane potential( ${Delta}$ ${Psi}$ ) developed upon succinate energization. These compounds alsodecreased state 3 respiration and enhanced state 4. We havealso demonstrated that the observed concentration-dependentstimulation of state 4 by LCA, DCA, CDCA, TCDC, and GCDC, isassociated with an enhanced permeability of mitochondria toH⁺. Addition of LCA, DCA, CDCA, TCDC, GCDC, and UDCA to mitochondriaenergized with succinate resulted in a dose-dependent membranedepolarization and stimulation of mitochondrial permeabilitytransition. Tauroursodeoxycholate (TUDC) elicited no significanteffect on succinate-supported mitochondrial bioenergetics. Incontrast, in the presence of glycoursodeoxycholic (GUDC), ${Delta}$ ${Psi}$ increasesas a function of bile salt concentration. The results of thisinvestigation demonstrate that at toxicologically relevant concentrations,most but not all bile acids alter mitochondrial bioenergetics,so impairment of mitochondrial function can be clinically relevantfor patients with cholestasis.

Key Words: mitochondria; bile acids; permeability transition pore; membrane potential; respiration.

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