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The carcinogenicity of discontinuous inhaled benzene exposures in CD-1 and C57Bl/6 mice

✍ Scribed by Carroll A. Snyder; Arthur R. Sellakumar; D. J. James; Roy E. Albert


Publisher
Springer-Verlag
Year
1988
Tongue
English
Weight
505 KB
Volume
62
Category
Article
ISSN
0340-5761

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✦ Synopsis


Groups of male C57Bl and CD-1 mice were exposed to benzene via inhalation using two different exposure protocols. One protocol consisted of repetitive week-long exposures to 300 ppm benzene (6 h/d x 5 d/wk) interrupted by 2 weeks of non-exposure. The exposure pattern (1 week of exposure followed by 2 weeks of non-exposure) was continued until the death of the last exposed animal. The second protocol consisted of exposures to 1200 ppm benzene (6 h/d x 5 d/wk) for 10 weeks. Exposures were then terminated and the animals allowed to live out their lives. For each protocol, appropriate age-matched control mice received comparable exposures to filtered, conditioned air. The discontinuous exposure patterns mimic the patterns of exposure often encountered in the workplace and, in addition, prolong the survival of exposed animals so as to maximize potential tumorigenic responses. Both exposure protocols were markedly hematotoxic to both mouse strains as measured by peripheral blood counts. Both strains of mice responded to the intermittent 300 ppm benzene exposures with elevated incidences of malignant tumors. Particularly noteworthy was a 35% incidence of zymbal gland tumors in the C57Bl mice. In contrast, only the CD-1 mice responded to the 1200 ppm benzene exposures delivered over 10 weeks with elevated tumor incidences. A 46% incidence of lung adenoma was particularly striking in these mice. Neither of the benzene exposure protocols induced elevated incidences of leukemia/lymphoma in either strain.(ABSTRACT TRUNCATED AT 250 WORDS)


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Developmental toxicity of methanol: Path
✍ Sigmund J. Degitz; John M. Rogers; Robert M. Zucker; E. Sidney Hunter III πŸ“‚ Article πŸ“… 2004 πŸ› John Wiley and Sons 🌐 English βš– 247 KB πŸ‘ 2 views

## Abstract ## BACKGROUND Methanol causes axial skeleton and craniofacial defects in both CD‐1 and C57BL/6J mice during gastrulation, but C57BL/6J embryos are more severely affected. We evaluated methanol‐induced pathogenesis in CD‐1 and C57BL/6J embryos exposed during gastrulation in whole embryo