Aflatoxin B1-2,3-oxide: evidence for its formation in rat liver in vivo and by human liver microsomes in vitro |
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Authors: | D H Swenson E C Miller J A Miller |
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Affiliation: | McArdle Laboratory for Cancer Research, University of Wisconsin Medical Center, Madison, Wisconsin 53706 USA |
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Abstract: | Injection of [3H]aflatoxin B1 into rats yielded covalently bound derivatives in hepatic DNA, rRNA, and protein. Mild acid hydrolysis of the DNA and rRNA adducts formed a derivative indistinguishable from 2,3-dihydro-2,3-dihydroxy-aflatoxin B1. The data indicate that approximately 60% of the nucleic acid adducts were derived from reactions with aflatoxin B1-2,3-oxide. Acid hydrolysis of rRNA-[3Haflatoxin B1 adduct formed by human liver microsomes also liberated the dihydrodiol in significant amount. The 2,3-oxide of aflatoxin B1 is a probable ultimate carcinogenic metabolite. |
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Keywords: | rRNA ribosomal RNA DMSO dimethylsulfoxide EDTA ethylenediamine tetraacetic acid TLC thin layer chromatography |
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