Influence of ozone on pentobarbital pharmacokinetics in mice
Previous studies have indicated that acute exposure to ambient concentrations of ozone (O 3) as low as 196 μg/m 3 (0.1 ppm) increases pentobarbital (PEN)-induced sleeping time in female mice. To elucidate potential mechanisms involved, additional studies were performed. A 3 h exposure to 9800 μg O 3...
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Veröffentlicht in: | Toxicology letters 1985-01, Vol.24 (2), p.163-170 |
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Format: | Artikel |
Sprache: | eng |
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Zusammenfassung: | Previous studies have indicated that acute exposure to ambient concentrations of ozone (O
3) as low as 196 μg/m
3 (0.1 ppm) increases pentobarbital (PEN)-induced sleeping time in female mice. To elucidate potential mechanisms involved, additional studies were performed. A 3 h exposure to 9800
μg O
3
m
3
(5 ppm) did not affect brain concentrations of PEN at time of awakening, even though sleeping time was increased. Exposure for 3 h to 9800 μg
O
3
m
3
(5 ppm) did not alter the pattern of brain or plasma metabolites of PEN. Pentobarbital clearance followed first-order kinetics with a one-compartment model. Mice exposed to 9800 μg
O
3
m
3
(5 ppm) for 3 h had a 106% increase in the plasma half-life of pentobarbital; at 1960μg
O
3
m
3
(1 ppm) for 3 h, a 71% increase was observed. It therefore appears possible that PEN-induced sleeping time might be increased due to an decrease in hepatic metabolism of PEN. |
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ISSN: | 0378-4274 1879-3169 |
DOI: | 10.1016/0378-4274(85)90053-0 |