Carcinogenesis, Vol 19, 1369-1375, Copyright © 1998 by Oxford University Press
C Cavin, D Holzhauser, A Constable, AC Huggett and B Schilter
The diterpenes cafestol and kahweol (C&K) have been identified in
animal models as two potentially chemoprotective agents present in green
and roasted coffee beans. It has been postulated that these compounds may
act as blocking agents by producing a co-ordinated modulation of multiple
enzymes involved in carcinogen detoxification. In this study, we
investigated the effects of C&K against the covalent binding of
aflatoxin B1 (AFB1) metabolites to DNA. Male Sprague-Dawley rats were
treated with increasing amounts of a mixture of C&K in the diet (0-6200
p.p.m.) for 28 and 90 days. A dose-dependent inhibition of AFB1 DNA-binding
was observed using S9 and microsomal subcellular fractions from
C&K-treated rat liver in an in vitro binding assay. Significant
inhibition was detected at 2300 p.p.m. and maximal reduction of DNA adduct
formation to nearly 50% of the control value was achieved with 6200 p.p.m.
of dietary C&K. Two complementary mechanisms may account for the
chemopreventive action of cafestol and kahweol against aflatoxin B1 in
rats. A decrease in the expression of the rat activating cytochrome P450s
(CYP2C11 and CYP3A2) was observed, as well as a strong induction of the
expression of the glutathione-S- transferase (GST) subunit GST Yc2, which
is known to detoxify highly the most genotoxic metabolite of AFB1. These
data and the previously demonstrated effects of C&K against the
development of 7,12- dimethylbenz[a]anthracene (DMBA)-induced
carcinogenesis at various tissue sites suggest the potential widespread
effect of these coffee components against chemical carcinogenesis.
ARTICLES
The coffee-specific diterpenes cafestol and kahweol protect against aflatoxin B1-induced genotoxicity through a dual mechanism
Nestle Research Center, Lausanne, Switzerland.
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