The role of 9-hydroxybenzo(a)pyrene in the microsome mediated binding of benzo(a)pyrene to dna

## Abstract Individual metabolites of benzo (a)pyrene were isolated from rat liver microsomal incubation of the parent hydrocarbon, and subsequently bound to DNA in separate incubations with microsomes. Of the metabolites examined, by far the greatest binding resulted with 7,8‐dihydro‐7,8‐dihydroxy

## Abstract A rat liver microsome‐mediated bacterial mutagenicity test showed 9‐hydroxybenzo (__a__) pyrene to be significantly more effective as a pre‐mutagen than benzo (__a__) pyrene. Experiments measuring the ability of these compounds to be metabolically activated to moieties that alky late ex

## Abstract Chemical conversion of generally tritiated benzo (a) pyrene to 6 and 1,6‐substituted derivatives resulted in 30% and 48% loss of tritium respectively. Metabolism of [^3^H], [^14^C]‐benzo (a) pyrene by rat liver microsomes yielded 3‐hydroxybenzo (a) pyrene with 30% loss of tritium, a mix

## Abstract An examination has been made of the binding, both __in vitro__ and __in vivo__ of the benzo(__a__)pyrene (BP) adduct to DNA components of differing sequence complexity. Annealing was performed at low renaturation temperatures in the presence of high concentrations of formamide to minimi

## Abstract The toxicokinetics of benzo(a)pyrene (BaP) and 3‐hydroxybenzo(a)pyrene (3‐OHBaP) were assessed in 36 male Sprague–Dawley rats injected intravenously with 40 µmol kg^1^ of BaP to explain the reported atypical urinary excretion profile of 3‐OHBaP. Blood, liver, kidney, lung, adipose tissu