R Suter-Eichenberger scite author profile

Developmental and adult toxicity of musk xylene was studied in Long Evans (LE) rats fed with chow containing musk xylene (MX) in food pellets in concentrations of 1 mg, 10 mg, 33 mg, 100 mg and 1000 mg MX per 1 kg chow corresponding to a daily intake of 0.07-0.08 mg MX/kg up to 70-80 mg MX/kg body weight. Adult male and female rats were MX exposed for a minimum of 10 weeks before mating. Exposure continued throughout pregnancy, birth and lactation. The effects of MX on CYP1A1/1A2 were studied in liver microsomes by EROD (7-ethoxyresorufin-o-deethylase) for CYP1A1 and by MROD (methoxyresorufin-o-demethylase) for CYP1A2 activity and by Western blotting. MX induced these enzymes dose dependently in adult and developing rats at PN (postnatal day) 1 and 14. The lowest effective maternal dose was 2-3 mg MX/kg/day. Western blot data of CYP2B and CYP3A indicated the induction of both P450 enzyme proteins in developing rats at PN 14 at the higher dose of 70-80 mg MX/kg/day. In contrast, upon high MX exposure CYP2B but not CYP3A was found to be induced in adult first generation male and female rats, indicating differential sensitivity to MX in development.

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CYP 450 enzyme induction by chronic oral musk xylene in adult and developing rats

Suter-Eichenberger

Boelsterli

Conscience-Egli

et al. 2000

Toxicology Letters

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Bioaccumulation and induction of CYP450 liver enzymes by synthetic musk fragrances in developing and adult rats

Schlumpf¹,

Suter-Eichenberger²,

Conscience-Egli³

et al. 1998

Toxicology Letters

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Musk xylene (MX): Bioaccumulation, enzyme induction and developmental toxicity

Suter-Eichenberger¹

1999

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