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Effect of toremifene on antipyrine elimination in the isolated perfused rat liver

  • Original Articles
  • Toremifene, Antipyrine, Isolated Liver Perfusion
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Summary

Toremifene is a triphenylethylene antioestrogen with significant antitumour activity. It is structurally very similar to tamoxifen. Both drugs undergo extensive hepatic metabolism and tamoxifen is known to inhibit hepatic mixed-function oxidases (MFO). Using the isolated perfused rat-liver model, we investigated the effect of toremifene on the elimination of antipyrine, a standard marker of MFO activity. Perfusate consisted of 20% red cells in a modified Krebs-Henseleit buffer, and 80 ml was recirculated at 14 ml/min for 3 h. High but clinically relevant steady-state toremifene levels of 3 and 10 μg/ml were achieved using bolus plus constant infusion into the reservoir. Elimination of 2.5 mg antipyrine was not inhibited by steady-state toremifene, but methanol (maximal perfusate concentration, 1.29%), the vehicle used for toremifene administration, caused a statistically significant increase in the antipyrine elimination half-life (mean, 1.4±0.2 h for controls vs 2.2±0.3 h for methanol;P<0.05,n=4). Whereas the methanol had no apparent effect on liver viability as assessed by bile flow and perfusate back-pressure, toremifene at a steady-state concentration of 10 μg/ml caused a statistically significant decrease in bile flow (value at 180 min, 0,22±0.05 ml/h as compared with 0.52±0.06 ml/h in the methanol control;P<0.05) and a statistically significant increase in perfusate back-pressure (value at 180 min, 17.5±1.8 cm vs 11.0±2.6 cm in the methanol control;P<0.05). Therefore, toremifene used at high doses can impair liver function in the isolated perfused rat liver, but it does not have any effect on antipyrine elimination.

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Authors and Affiliations

  1. Pharmacology Unit, Peter MacCallum Cancer Institute, Melbourne, Victoria, Australia

    Lorraine K. Webster, Andrew G. Ellis & James F. Bishop

  2. Experimental Chemotherapy Unit, Peter MacCallum Cancer Institute, 481 Little Lonsdale St., 3000, Melbourne, Victoria, Australia

    Lorraine K. Webster, Andrew G. Ellis & James F. Bishop

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  1. Lorraine K. Webster
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  2. Andrew G. Ellis
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  3. James F. Bishop
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Webster, L.K., Ellis, A.G. & Bishop, J.F. Effect of toremifene on antipyrine elimination in the isolated perfused rat liver. Cancer Chemother. Pharmacol. 31, 319–323 (1993). https://doi.org/10.1007/BF00685678

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  • DOI: https://doi.org/10.1007/BF00685678

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