Physiologically Based Biokinetic (PBBK) Model for Safrole Bioactivation and Detoxification in Rats
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作者:
Martati, E.
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Wageningen Univ, Div Toxicol, NL-6703 HE Wageningen, Netherlands
Brawijaya Univ, Dept Food Sci & Technol, Jl Veteran Malang 65145, IndonesiaWageningen Univ, Div Toxicol, NL-6703 HE Wageningen, Netherlands
Martati, E.
[1
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Boersma, M. G.
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Wageningen Univ, Div Toxicol, NL-6703 HE Wageningen, NetherlandsWageningen Univ, Div Toxicol, NL-6703 HE Wageningen, Netherlands
Boersma, M. G.
[1
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Spenkelink, A.
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Wageningen Univ, Div Toxicol, NL-6703 HE Wageningen, NetherlandsWageningen Univ, Div Toxicol, NL-6703 HE Wageningen, Netherlands
Spenkelink, A.
[1
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Khadka, D. B.
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Wageningen Univ, Div Toxicol, NL-6703 HE Wageningen, NetherlandsWageningen Univ, Div Toxicol, NL-6703 HE Wageningen, Netherlands
Khadka, D. B.
[1
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Punt, A.
[1
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Vervoort, J.
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Wageningen Univ, Dept Biochem, NL-6703 HA Wageningen, NetherlandsWageningen Univ, Div Toxicol, NL-6703 HE Wageningen, Netherlands
Vervoort, J.
[3
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van Bladeren, P. J.
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Wageningen Univ, Div Toxicol, NL-6703 HE Wageningen, Netherlands
Nestle Res Ctr, CH-1000 Lausanne, SwitzerlandWageningen Univ, Div Toxicol, NL-6703 HE Wageningen, Netherlands
van Bladeren, P. J.
[1
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Rietjens, I. M. C. M.
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Wageningen Univ, Div Toxicol, NL-6703 HE Wageningen, NetherlandsWageningen Univ, Div Toxicol, NL-6703 HE Wageningen, Netherlands
Rietjens, I. M. C. M.
[1
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机构:
[1] Wageningen Univ, Div Toxicol, NL-6703 HE Wageningen, Netherlands
A physiologically based biokinetic (PBBK) model for alkenylbenzene safrole in rats was developed using in vitro metabolic parameters determined using relevant tissue fractions. The performance of the model was evaluated by comparison of the predicted levels of 1,2-dihydroxy-4-allylbenzene and 1'-hydroxysafrole glucuronide to levels of these metabolites reported in the literature to be excreted in the urine of rats exposed to safrole and by comparison of the predicted amount of total urinary safrole metabolites to the reported levels of safrole metabolites in the urine of safrole exposed rats. These comparisons revealed that the predictions adequately match observed experimental values. Next, the model was used to predict the relative extent of bioactivation and detoxification of safrole at different oral doses. At low as well as high doses, P450 mediated oxidation of safrole mainly occurs in the liver in which 1,2-dihydroxy-4-allylbenzene was predicted to be the major P450 metabolite of safrole. A dose dependent shift in P450 mediated oxidation leading to a relative increase in bioactivation at high doses was not observed. Comparison of the results obtained for safrole with the results previously obtained with PBBK models for the related alkenylbenzenes estragole and methyleugenol revealed that the overall differences in bioactivation of the three alkenylbenzenes to their ultimate carcinogenic 1'-sulfooxy metabolites are limited. This is in line with the generally less than 4-fold difference in their level of DNA binding in in vitro and in vivo studies and their almost similar BMDL(10) values (lower confidence limit of the benchmark dose that gives 10% increase in tumor incidence over background level) obtained in in vivo carcinogenicity studies. It is concluded that in spite of differences in the rates of specific metabolic conversions, overall the levels of bioactivation of the three alkenylbenzenes are comparable which is in line with their comparable carcinogenic potential.
机构:
Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Einsteinweg 55, NL-2333 CC Leiden, NetherlandsLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Einsteinweg 55, NL-2333 CC Leiden, Netherlands
Sharma, Raju Prasad
Burgers, Elsje J.
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Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Einsteinweg 55, NL-2333 CC Leiden, NetherlandsLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Einsteinweg 55, NL-2333 CC Leiden, Netherlands
Burgers, Elsje J.
Beltman, Joost B.
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Leiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Einsteinweg 55, NL-2333 CC Leiden, NetherlandsLeiden Univ, Leiden Acad Ctr Drug Res, Div Drug Discovery & Safety, Einsteinweg 55, NL-2333 CC Leiden, Netherlands
机构:
Certara UK Ltd, Simcyp Div, Sheffield, S Yorkshire, EnglandCertara UK Ltd, Simcyp Div, Sheffield, S Yorkshire, England
Fisher, C. P.
Hatley, O.
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Certara UK Ltd, Simcyp Div, Sheffield, S Yorkshire, EnglandCertara UK Ltd, Simcyp Div, Sheffield, S Yorkshire, England
Hatley, O.
van Vugt, B.
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BioDetect Syst BV, Amsterdam, NetherlandsCertara UK Ltd, Simcyp Div, Sheffield, S Yorkshire, England
van Vugt, B.
Bois, F.
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Inst Natl Envirom Ind & Risques INERIS, Models Ecotoxicol & Toxicol Unit, Verneuil En Halatte, FranceCertara UK Ltd, Simcyp Div, Sheffield, S Yorkshire, England
Bois, F.
Escher, S.
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Fraunhofer Inst Toxicol & Expt Med ITEM, Dept Chem Risk Assessment Databases & Expert Syst, Hannover, GermanyCertara UK Ltd, Simcyp Div, Sheffield, S Yorkshire, England
Escher, S.
Gardner, I.
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Certara UK Ltd, Simcyp Div, Sheffield, S Yorkshire, EnglandCertara UK Ltd, Simcyp Div, Sheffield, S Yorkshire, England
机构:
Kyoto Univ, Grad Sch Engn, Dept Global Environm Engn, Sakyo Ku, Kyoto 6068501, JapanKyoto Univ, Grad Sch Engn, Dept Global Environm Engn, Sakyo Ku, Kyoto 6068501, Japan
Chan, Melissa R. L.
Morisawa, Shinsuke
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机构:Kyoto Univ, Grad Sch Engn, Dept Global Environm Engn, Sakyo Ku, Kyoto 6068501, Japan
Morisawa, Shinsuke
Nakayama, Aki
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机构:Kyoto Univ, Grad Sch Engn, Dept Global Environm Engn, Sakyo Ku, Kyoto 6068501, Japan
Nakayama, Aki
Kawamoto, Yuko
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机构:Kyoto Univ, Grad Sch Engn, Dept Global Environm Engn, Sakyo Ku, Kyoto 6068501, Japan
Kawamoto, Yuko
Sugimoto, Miki
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机构:Kyoto Univ, Grad Sch Engn, Dept Global Environm Engn, Sakyo Ku, Kyoto 6068501, Japan
Sugimoto, Miki
Yoneda, Minoru
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机构:Kyoto Univ, Grad Sch Engn, Dept Global Environm Engn, Sakyo Ku, Kyoto 6068501, Japan