Failure to demonstrate chemoprevention by the monoterpene perillyl alcohol during early rat hepatocarcinogenesis: a cautionary note

doi:10.1093/carcin/21.10.1869

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Carcinogenesis, Vol. 21, No. 10, 1869-1877, October 2000
© 2000 Oxford University Press

Carcinogenesis

Failure to demonstrate chemoprevention by the monoterpene perillyl alcohol during early rat hepatocarcinogenesis: a cautionary note

Alexandra Löw-Baselli, Wolfgang W. Huber, Monika Käfer, Krystyna Bukowska, Rolf Schulte-Hermann and Bettina Grasl-Kraupp¹

Institut für Tumorbiologie-Krebsforschung, University of Vienna, Borschkegasse 8a, A-1090 Vienna, Austria

The monoterpene perillyl alcohol (PA) is being considered asa useful chemopreventive and therapeutic agent against humancancers. However, no data are available on the effects of PAin the first stages of hepatocarcinogenesis. To study such effects,putatively initiated cells and preneoplastic foci in hepatocarcinogenesiswere used as a model. Male Wistar rats were treated with a singledose of N-nitrosomorpholine (NNM). Between days 4 and 91 afterNNM, subgroups of rats received either PA (1 g/kg body wt/day)or phenobarbital (PB) (50 mg/kg body wt/day) in the diet. SincePA treatment reduced food intake, one control group was fedad libitum, while a second control was pair fed between days4 and 91. In order to enhance any treatment effects, all groups,including the controls, were treated with the potent tumor promoterPB after day 91 until the end of the experiment at day 266.Rats were killed at multiple time points and putatively initiatedcells and preneoplastic foci were identified by staining positivelyfor placental glutathione S-transferase (G+). The followingresults were obtained. (i) A few days after NNM treatment singleG+ cells emerged; a considerable portion of which developedinto foci. (ii) Treatment with PB resulted in an increase innumber and size of G+ foci. (iii) PA treatment failed to reducethe number of G+ cells; it somewhat lowered rates of apoptosisin G+ foci and clearly increased their average size. (iv) Eighty-sevendays of PA revealed no protective effect on day 266, but, similarto PB treatment, increased the growth of foci. In conclusion,PA exerted no detectable chemopreventive effect in the earlystages of rat hepatocarcinogenesis. It rather exerted a PB-liketumor promoting activity. These data argue against a recommendationof PA as a chemopreventive agent for healthy humans.

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