Mitochondrial respiration and membrane potential are regulated by the allosteric ATP-inhibition of cytochrome c oxidase |
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Authors: | Rabia Ramzan Katrin Staniek Bernhard Kadenbach Sebastian Vogt |
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Affiliation: | a Biomedical Research Center, Cardiovascular Laboratory, Philipps-University, D-35032 Marburg, Germany b Fachbereich Chemie, Philipps-University, D-35032 Marburg, Germany c Molecular Pharmacology and Toxicology Unit, Department of Biomedical Sciences, University of Veterinary Medicine Vienna, Veterinärplatz 1, A-1210 Vienna, Austria |
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Abstract: | ![]() This paper describes the problems of measuring the allosteric ATP-inhibition of cytochrome c oxidase (CcO) in isolated mitochondria. Only by using the ATP-regenerating system phosphoenolpyruvate and pyruvate kinase full ATP-inhibition of CcO could be demonstrated by kinetic measurements. The mechanism was proposed to keep the mitochondrial membrane potential (?Ψm) in living cells and tissues at low values (100-140 mV), when the matrix ATP/ADP ratios are high. In contrast, high ?Ψm values (180-220 mV) are generally measured in isolated mitochondria. By using a tetraphenyl phosphonium electrode we observed in isolated rat liver mitochondria with glutamate plus malate as substrates a reversible decrease of ?Ψm from 233 to 123 mV after addition of phosphoenolpyruvate and pyruvate kinase. The decrease of ?Ψm is explained by reversal of the gluconeogenetic enzymes pyruvate carboxylase and phosphoenolpyruvate carboxykinase yielding ATP and GTP, thus increasing the matrix ATP/ADP ratio. With rat heart mitochondria, which lack these enzymes, no decrease of ?Ψm was found. From the data we conclude that high matrix ATP/ADP ratios keep ?Ψm at low values by the allosteric ATP-inhibition of CcO, thus preventing the generation of reactive oxygen species which could generate degenerative diseases. It is proposed that respiration in living eukaryotic organisms is normally controlled by the ?Ψm-independent “allosteric ATP-inhibition of CcO.” Only when the allosteric ATP-inhibition is switched off under stress, respiration is regulated by “respiratory control,” based on ?Ψm according to the Mitchell Theory. |
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Keywords: | BSA, bovine serum albumin CCCP, carbonyl cyanide m-chlorophenylhydrazone CcO, cytochrome c oxidase ?Ψm, mitochondrial membrane potential PEP, phosphorenolpyruvate PK, pyruvate kinase ROS, reactive oxygen species TPP+, tetraphenyl phosphonium ion |
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