๐”– Bobbio Scriptorium
โœฆ   LIBER   โœฆ

Toxicological evaluation of 1-chloroacetophenone and dibenz[b,f]-1,4-oxazepine after repeated inhalation exposure in mice

โœ Scribed by Pravin Kumar; S. J. S. Flora; S. C. Pant; A. S. Sachan; S. P. Saxena; S. Das Gupta

Publisher
John Wiley and Sons
Year
1994
Tongue
English
Weight
641 KB
Volume
14
Category
Article
ISSN
0260-437X

No coin nor oath required. For personal study only.

โœฆ Synopsis

Toxicological evaluation was made on the effects of two peripheral sensory irritants (tear gases): 1chloroacetophenone (CN) and dibenz[ b,&1,4-oxazepine (CR). Animals had a 15-min daily inhalation exposure to average vapour concentrations of 87.6 mg CN m-' or 1008 mg CR m-3 (both equal to 0.05 ws0) for 5 or 10 days and were sacrificed 24 h after the last exposure, when biochemical and histopathological observations were made. Both chemicals caused a significant decrease in body weight gain. Histological changes in lung, liver and kidneys were more severe after 10 than after 5 days of exposure and were more severe in CNexposed than in CR-exposed mice. Organ weight to body weight ratios remained normal except for the spleen to body weight ratio, which decreased in CN-exposed mice afler both 5 and 10 days of exposure. Biochemical indicators showed a toxic response only in CN-exposed mice, but the only consistent change was an increase in blood glucose. Hepatic alkaline phosphatase was not influenced, malondialdehyde concentration and acid phosphatase activity were increased only after 5 days of exposure and liver GSH concentration decreased after 10 days of exposure. Results indicate that CN is not only more toxic than CR in absolute terms but is also more toxic at the 5% level of their L C , . .


## Animals


Randomly bred male Swiss albino mice (25 ? 2 g) obtained from the animal facilities of our establishment CCC O260-437W94/06O411-O6

๐Ÿ“œ SIMILAR VOLUMES

Analysis of the 1H and 13C{1H} NMR Spect
Analysis of the 1H and 13C{1H} NMR Spectral Parameters of the Tear Gases ฮฑ-Chloroacetophenone, Dibenz[b,f][1,4]oxazepine, and 2-Chlorobenzylidene Malononitrile
โœ Markku Mesilaakso ๐Ÿ“‚ Article ๐Ÿ“… 1996 ๐Ÿ› John Wiley and Sons ๐ŸŒ English โš– 475 KB ๐Ÿ‘ 1 views

The 'H and '3C{'H) NMR spectra of the tear gases a-chloroacetophenone, dibenz[b,f] [ 1,4)oxazepine and 2chlorobenzylidene malononitrile were recorded in CDCl, , CD,CI, and (CD,),CO and analysed. Assignments of the resonances were confirmed by homonuclear and heteronuclear correlation spectroscopy. D

Blood pharmacokinetics of tertiary amyl
Blood pharmacokinetics of tertiary amyl methyl ether in male and female F344 rats and CD-1 mice after nose-only inhalation exposure
โœ Susan C. J. Sumner; Derek B. Janszen; Bahman Asgharian; Timothy A. Moore; Carol ๐Ÿ“‚ Article ๐Ÿ“… 2003 ๐Ÿ› John Wiley and Sons ๐ŸŒ English โš– 144 KB

Interest in understanding the biological behavior of aliphatic ethers has increased owing to their use as gasoline additives. The purpose of this study was to investigate the blood pharmacokinetics of the oxygenate tertiary amyl methyl ether (TAME), its major metabolite tertiary amyl alcohol (TAA) a

Mutational specificity: Assessment of 1,
Mutational specificity: Assessment of 1,3-butadiene mutagenicity in the bone marrow of B6C3F1 lacl transgenic mice (Big Blueยฎ): A review of mutational spectrum and LACL mutant frequency after a 5-day 625 PPM 1,3-butadiene exposure
โœ Leslie Recio; Kathy G. Meyer; Linda J. Pluta; Owen R. Moss; Christopher J. Saran ๐Ÿ“‚ Article ๐Ÿ“… 1996 ๐Ÿ› John Wiley and Sons ๐ŸŒ English โš– 547 KB

Carolina 1,3-Butadiene (BD) is a carcinogen that is bioactivated to at least two genotoxic metabolites. In the present article, we review briefly our previous studies on the in vivo mutagenicity and mutational spectra of BD in bone marrow and extend these studies to examine the effect of exposure ti