Isopropanol 13-Week Vapor Inhalation Study in Rats and Mice with Neurotoxicity Evaluation in Rats

Isopropanol 13-Week Vapor Inhalation Study in Rats and Mice with Neurotoxicity Evaluation in Rats

Isopropanol 13-Week Vapor Inhalation Study in Rats and Mice with Neurotoxicity Evaluation in Rats. Burleighflayer, H. D., Gill, M. W., Strother, D. E., Masten, L. W., McKee, R. H., Tyler, T. R., and Gardiner, T. (1994). Fundam. Appl. Toxicol. 23, 421-428. This study was conducted to evaluate the pos...

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Veröffentlicht in:Fundamental and applied toxicology 1994-10, Vol.23 (3), p.421-428
Hauptverfasser: Burleigh-Flayer, Heather D., Gill, Michael W., Strother, Dale E., Masten, Lawrence W., McKee, Richard H., Tyler, Tipton R., Gardiner, Thomas
Format: Artikel
Sprache:eng
Schlagworte:
1-Propanol - administration & dosage
1-Propanol - toxicity
Administration, Inhalation
Animals
Biological and medical sciences
Blood - drug effects
Body Weight - drug effects
Brain - drug effects
Chemical and industrial products toxicology. Toxic occupational diseases
Eating - drug effects
Female
Kidney - drug effects
Kidney - pathology
Male
Medical sciences
Mice
Motor Activity - drug effects
Rats
Rats, Inbred F344
Solvents
Toxicology
Volatilization
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Zusammenfassung:Isopropanol 13-Week Vapor Inhalation Study in Rats and Mice with Neurotoxicity Evaluation in Rats. Burleighflayer, H. D., Gill, M. W., Strother, D. E., Masten, L. W., McKee, R. H., Tyler, T. R., and Gardiner, T. (1994). Fundam. Appl. Toxicol. 23, 421-428. This study was conducted to evaluate the possible subchronic toxicity as well as neurobehavioral effects of isopropanol, a widely used industrial and commercial solvent. Five groups, each containing 10 Fischer 344 rats/sex and 10 CD-1 mice/sex, were exposed for 6 hr/day, 5 days/week, for 13 weeks to isopropanol vapor at concentrations of 0 (control), 100, 500, 1500, or 5000 ppm. An additional 15 rats/sex were assigned to the 0, 500, 1500, and 5000 ppm groups for assessment of neurobehavioral function. No exposure-related mortalities occurred during the study. The narcotic effects of isopropanol were noted only during exposures at 1500 and 5000 ppm. These signs, noted during exposures, were typically absent following exposures. The only clinical signs observed following exposures included swollen periocular tissue, perinasal encrustation, and ataxia for rats of the 5000 ppm group. Neurobehavioral evaluations indicated no changes in any of the parameters of the functional observational battery; however, increased motor activity for female rats in the 5000 ppm group was noted at Weeks 9 and 13. Decreases in body weight and body weight gain were observed for rats of the 5000 ppm group at the end of the first week of exposure. During the remaining weeks, increases in body weight and/or body weight gain were observed for rats of the 1500 and 5000 ppm groups. No exposure-related effects on body weight were noted for male mice; however, increased body weight and body weight gain were observed for female mice of the 5000 ppm group. Increases or decreases in food and water consumption generally corresponded to changes in body weight and body weight gain. Various changes in clinical pathology parameters were observed for rats and female mice of the 5000 ppm group. The only organ weight effect noted was an increased relative liver weight in both sexes of rats and female mice of the 5000 ppm group. At necropsy, there were no gross lesions determined to be exposure related. Furthermore, the only micro, scopic change observed was hyaline droplets within the kidneys of all male rats (including controls). The size and frequency of the hyaline droplets were increased for the isopropanol exposure groups compared to the cont
ISSN:0272-0590
1095-6832
DOI:10.1006/faat.1994.1123