Abstract
The use of exhalation of ethane and n-pentane in experimental animals as parameters of lipid peroxidation led to an examination of pharmacokinetics of both compounds in rats. When rats were exposed, in a closed desiccator jar chamber, to a wide range of ethane concentrations, linear elimination pharmacokinetics were observed. n-Pentane, when concentrations higher than 100 ppm were applied, displayed saturation kinetics. These were formally explained by action of two competing metabolizing pathways or enzymes. Application of preexisting models could describe exhalation of both ethane and n-pentane by untreated control rats. Stimulation of lipid peroxidation by ferrous ions or by carbon tetrachloride resulted in dissimilar quantitative behaviours of ethane and n-pentane. Ethane production rates were enhanced after application of both compounds. Because of relatively slow metabolic eliminations this led to markedly elevated concentrations of ethane in the gas phase of the system. Pentane production rates were simultaneously enhanced. However, difficulties in interpretation arise because of rapid metabolic elimination of n-pentane. Compounds that diminish pentane metabolism are shown to evoke higher pentane concentrations in the system than compounds which only enhance the pentane production rate. Determinations of ethane exhalation should provide a more favourable parameter of lipid peroxidation than exhalation of pentane.
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References
Andersen ME (1981a) Saturable metabolism and its relationship to toxicity. CRC Crit Rev Toxicol 10: 105–150
Andersen ME (1981b) A physiologically based toxicokinetic description of the metabolism of inhaled gases and vapors: analysis at steady state. Toxicol Appl Pharmacol 60: 509–526
Bolt HM, Filser JG, Buchter A (1981) Inhalation pharmacokinetics based on gas uptake studies. III. A pharmacokinetic assessment in man of “peak concentrations” of vinyl chloride. Arch Toxicol 48: 213–228
Dillard CJ, Dumelin EE, Tappel AL (1977) Effect of dietary vitamin E on expiration of pentane and ethane by the rat. Lipids 12: 109–114
Filser JG, Bolt HM (1979) Pharmacokinetics of halogenated ethylenes in rats. Arch Toxicol 42: 123–136
Filser JG, Bolt HM (1981) Inhalation pharmacokinetics based on gas uptake studies. I. Improvement of kinetic models. Arch Toxicol 47: 279–292
Filser JG, Bolt HM (1983) Inhalation pharmacokinetics based on gas uptake studies. IV. The endogenous production of volatile hydrocarbons. Arch Toxicol 52: 123–133
Frank H, Hintze T, Bimboes D, Remmer H (1980) Monitoring lipid peroxidation by breath analysis: endogenous hydrocarbons and their metabolic elimination. Toxicol Appl Pharmacol 56: 337–344
Frommer U, Ullrich V, Staudinger HJ (1970) Hydroxylation of aliphatic compounds by liver microsomes. Hoppe-Seyler's Z Physiol Chem 351: 903–912
Gelmont D, Stein RA, Mead JF (1981) The bacterial origin of rat breath pentane. Biochem. Biophys Res Commun 102: 932–936
Hallier E, Filser JG, Bolt HM (1981) Inhalation pharmacokinetics based on gas uptake studies. II. Pharmacokinetics of acetone in rats. Arch Toxicol 47: 293–304
Hempel V, May R, Frank H, Remmer H, Köster U (1980) Isobutene formation during halothane anesthesia in man. Br J Anaesthesiol 52: 989–992
Kappus H, Kieczka H, Muliawan H, Schulze RM, Ottenwälder H (1982) Influence of ferrous ions on CCl4-induced lipid peroxidation. In: Snyder R, Parke DV, Kocsis JJ, Jollow DJ, Gibson CG, Witmer CM (eds) Biological Reactive Intermediates II, Part A. Plenum Press, New York pp 779–791
Kivits GAA, Ganguli-Swarttouw MACR, Christ EJ (1981) The composition of alkanes in exhaled air of rats as a result of lipid peroxidation in vivo. Biochim Biophys Acta 665: 559–570
Köster U, Albrecht D, Kappus H (1977) Evidence for carbon tetrachloride- and ethanol-induced lipid peroxidation in vivo demonstrated by ethane production in mice and rats. Toxicol Appl Pharmacol 41: 639–648
Litov RE, Irving DH, Downey JE, Tappel AL (1978) Lipid peroxidation: a mechanism involved in acute ethanol toxicity as demonstrated by in vivo pentane production in the rat. Lipids 13: 305–307
Riely CA, Cohen G, Lieberman M (1974) Ethane evolution: a new index of lipid peroxidation. Science 183: 208–210
Sagai M, Tappel AL (1979) Lipid peroxidation induced by some halomethanes as measured by in vivo pentane production in the rat. Toxicol Appl Pharmacol 49: 283–291
Tappel AL (1980) Measurement of and protection from in vivo lipid peroxidation. In: Pryor WA (ed) Free Radicals in Biology, vol IV. Academic Press, New York, pp 1–47
Wendel A, Dumelin EE (1981) Hydrocarbon exhalation. Meth Enzymol 77: 10–15
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Filser, J.G., Bolt, H.M., Muliawan, H. et al. Quantitative evaluation of ethane and n-pentane as indicators of lipid peroxidation in vivo. Arch Toxicol 52, 135–147 (1983). https://doi.org/10.1007/BF00354773
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DOI: https://doi.org/10.1007/BF00354773