Effect of PSC 833, an inhibitor of P-glycoprotein, on 1,2-dimethylhydrazine-induced liver carcinogenesis in rats

doi:10.1093/carcin/bgg159

Carcinogenesis Advance Access originally published online on September 11, 2003

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Carcinogenesis, Vol. 24, No. 12, 1977-1984, December 2003
© Oxford University Press; all rights reserved

CARCINOGENESIS

Effect of PSC 833, an inhibitor of P-glycoprotein, on 1,2-dimethylhydrazine-induced liver carcinogenesis in rats

Janarthanan Kankesan¹^,*, Aroon Yusuf¹^,*, Ezio Laconi⁴^,*, Ramesh Vanama¹, Grace Bradley², Jake J. Thiessen³, Victor Ling⁵, Prema M. Rao¹, Srinivasan Rajalakshmi¹ and Dittakavi S. R. Sarma¹^,6

¹ Departments of Laboratory Medicine and Pathobiology, ² Medical Biophysics and ³ Pharmacy, University of Toronto, Toronto, Ontario, Canada, ⁴ Department of Experimental Pathology, University of Cagliari, Cagliari, Italy and ⁵ BC Cancer Agency and University of British Columbia, Vancouver, British Columbia, Canada

The present study explores the hypothesis that over-expressionof P-glycoprotein (Pgp, product of mdr1) is intimately associatedwith liver cancer development and therefore inhibitors of Pgpshould inhibit the development of liver cancer. Accordingly,we determined the effect of PSC833 (PSC), a potent inhibitorof Pgp, on experimental liver carcinogenesis in rats. To studythe effects of PSC on liver cancer development, a daily doseof 30 mg PSC/kg body wt (PSC30) was chosen based on an initialdose–response experiment. Accordingly in experiment 1,PSC30 was fed to rats initiated by 1,2-dimethylhydrazine coupledwith two-thirds partial hepatectomy and promoted for 22 weekswith 1% dietary orotic acid. Surprisingly, in contrast to ourearlier observations in rats without hepatic nodules, in ratsbearing hepatic nodules, PSC30 was found to be toxic. Becauseof this, PSC30 diet was discontinued after 5 weeks and the ratswere transferred to basal diet (BD). The rats were killed 10and 25 weeks thereafter. Cumulative results indicate that PSC30exhibited a 40% decrease in the incidence of hepatocellularcarcinoma (HCC; 15 of 18 in the BD group compared with eightof 17 in the PSC30 group; P = 0.08) coupled with significantreduction of tumor multiplicity (54%; P < 0.05) and tumorburden (61%; P < 0.005) compared with controls. In experiment2, 15 mg PSC/kg body wt (PSC15) was fed for 20 weeks to ratssimilarly initiated and promoted for 35 weeks. PSC15 inhibitedthe incidence of HCC by 75% (four of four in the BD group comparedto one of four in the PSC30 group; P = 0.15) and significantlyreduced tumor burden by 55% (P < 0.05). The lack of statisticalsignificance of inhibition on tumor incidence reflects the smallsample size. Taken together the results indicate a possibleintrinsic role for Pgp in liver cancer development and introduceanother promising unexplored therapeutic approach in liver cancertreatment.

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