1992
DOI: 10.1016/0273-2300(92)90044-a
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An analysis of exposure rate effects for benzene using a physiologically based pharmacokinetic model

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Cited by 28 publications
(19 citation statements)
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“…The amount of metabolites (hydroquinone, catechol, and muconaldehyde) formed was 20% higher after the 15-min exposure at the higher level than after the 8-h exposure at the lower level. Differences between the model predictions (Bois and Paxman, 1992) and the empirical data of Sabourin, et al (1989a,b) may be related, at least in part, to the higher benzene exposure levels (50, 150, and 600 ppm) used by Sabourin, et al A number of investigators have suggested that covalent binding of benzene metabolites to cellular macromolecules is related to benzene's mechanism of toxicity, although the relationship between adduct formation and toxicity is not clear. Benzene metabolites have been found to form covalent adducts with proteins from blood in humans (Bechtold, et al, 1992b).…”
Section: Metabolismmentioning
confidence: 86%
“…The amount of metabolites (hydroquinone, catechol, and muconaldehyde) formed was 20% higher after the 15-min exposure at the higher level than after the 8-h exposure at the lower level. Differences between the model predictions (Bois and Paxman, 1992) and the empirical data of Sabourin, et al (1989a,b) may be related, at least in part, to the higher benzene exposure levels (50, 150, and 600 ppm) used by Sabourin, et al A number of investigators have suggested that covalent binding of benzene metabolites to cellular macromolecules is related to benzene's mechanism of toxicity, although the relationship between adduct formation and toxicity is not clear. Benzene metabolites have been found to form covalent adducts with proteins from blood in humans (Bechtold, et al, 1992b).…”
Section: Metabolismmentioning
confidence: 86%
“…Parameters k 1 and k 2 were sampled from wide uniform distributions, with informative bounds given by Segel (1975, p. 32). For k 3 we used a narrower range because we had reasonable prior values for benzene, toluene, ethylbenzene, and m -xylene V max (Bois and Paxman 1992; Dennison et al 2003; Tardif et al 1997) and for the total quantity of CYP2E1 in liver, hence for its total liver concentration [CYP2E1] total (Carlile et al 1997; Seaton et al 1995). …”
Section: Methodsmentioning
confidence: 99%
“…We again used Monte Carlo simulations and reverted to a continuous measure of fit, log-likelihood, which has several disadvantages as men- Observed Dat Value Figure 10. Predictions made by the best-fitting simulation run versus observed experimental values (3,4,(11)(12)(13). For a perfect fit, the points would fall on the identity line.…”
Section: Methodological Versus Biological Accomplishmentsmentioning
confidence: 99%