1992
DOI: 10.1002/em.2850200110
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Comparison of acyltransferase‐mediated mutagenicity and nucleic acid binding of n‐acetoxy‐4‐acetylaminobiphenyl by hepatic and bladder microsomes from rats and dogs

Abstract: Acyltransferase-mediated mutagenic and metabolic activation of N-acetoxy-4-acetylaminobiphenyl (N-OAc-AABP) by hepatic tissues of rats and dogs were compared. N-OAc-AABP was mutagenic in Salmonella typhimurium TA98 even in the absence of exogenous enzyme(s). However, supplementation with hepatic microsomes from dogs showed a dose-dependent increase in mutagenicity of N-OAc-AABP, whereas under the same conditions, rat microsomes were inactive. Incubation of liver microsomes with RNA showed that 46.4 and 11.2 nm… Show more

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Cited by 3 publications
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“…Hydrolysis of these N -glucuronides is rapid in acidic (pH 5-6) urine (Babu et al 1992;1996) as found in dogs and humans, as compared to the less acidic urine of rats (Kad-lubar et al 1981;Kadlubar 1986). In contrast, the major activation pathways in rodents appear to be N -and O-acetylation (Swaminathan and Hatcher 1992). Rodents also N -acetylate as a detoxi cation pathway.…”
Section: Metabolism As a Basis For Test Species Selectionmentioning
confidence: 96%
“…Hydrolysis of these N -glucuronides is rapid in acidic (pH 5-6) urine (Babu et al 1992;1996) as found in dogs and humans, as compared to the less acidic urine of rats (Kad-lubar et al 1981;Kadlubar 1986). In contrast, the major activation pathways in rodents appear to be N -and O-acetylation (Swaminathan and Hatcher 1992). Rodents also N -acetylate as a detoxi cation pathway.…”
Section: Metabolism As a Basis For Test Species Selectionmentioning
confidence: 96%