Genotoxic effects of benzyl isothiocyanate, a natural chemopreventive agent

doi:10.1093/mutage/14.6.595

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Mutagenesis, Vol. 14, No. 6, 595-604, November 1999
© 1999 UK Environmental Mutagen Society/Oxford University Press

Genotoxic effects of benzyl isothiocyanate, a natural chemopreventive agent

Fekadu Kassie², Beatrice Pool-Zobel¹, Wolfram Parzefall and Siegfried Knasmüller

Institute for Cancer Research, Borschkegasse 8a, A-1090 Vienna, Austria and ¹ Institute of Hygiene and Toxicology, Federal Research Center for Nutrition, Karlsruhe, Germany

Benzyl isothiocyanate (BITC) is contained in cruciferous plantswhich are part of the human diet. Numerous reports indicatethat BITC prevents chemically induced cancer in laboratory animalsand it has been postulated that BITC might also be chemoprotectivein humans. On the other hand, evidence is accumulating thatthis compound is a potent genotoxin in mammalian cells by itself.To further elucidate the potential hazards of BITC, we investigatedits genotoxic effects in different in vitro genotoxicity testsand in animal models. In in vitro experiments [differentialDNA repair assay with Escherichia coli, micronucleus assay withhuman HepG2 cells and single cell gel electrophoresis (SCGE)assay with hepatocytes and gastrointestinal tract cells] pronounceddose-dependent genotoxic effects were found at low dose levels( $<=$ 5 µg/ml). In contrast, substantially weaker effects wereobtained in in vivo experiments with laboratory rodents: inthe differential DNA repair assay with E.coli cells, only moderategenotoxic effects were seen in indicator cells recovered fromvarious organs of mice after treatment with high doses (between90 and 270 mg/kg), while in SCGE assay with rats a change inthe DNA migration pattern was seen at a dose level of 220 mg/kgbody wt. These findings indicate that BITC is detoxified underin vivo test conditions. This assumption was supported by theresults of in vitro experiments which showed that the genotoxiceffects of BITC are markedly reduced by bovine serum albuminand human body fluids such as saliva and gastric juice. Additionalexperiments carried out on the mechanistic aspects of the genotoxicityof BITC showed that this compound causes formation of thiobarbituricacid-reactive substances in HepG2 cells and that its DNA damagingproperties are diminished by ${alpha}$ -tocopherol, vitamin C, sodiumbenzoate and ß-carotene, indicating the possible involvementof free radicals in the genotoxicity of BITC. The doses of BITCrequired to cause measurable DNA damage in laboratory rodentsexceeded by far the dietary exposure levels of humans, but aresimilar to those which were required to inhibit chemically inducedcancer in earlier animal experiments.

² To whom correspondence should be addressed. Tel: +43 1 427765143; Fax: +43 1 4277 65143; Email: profeka{at}yahoo.com

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