Effects of chemoprotective agents on the metabolic activation of the carcinogenic arylamines PhIP and 4-aminobiphenyl in human and rat liver microsomes

Carcinogenic aromatic amines, including the heterocyclic amines, may pose a significant health risk to humans. To determine the potential for chemoprotective intervention against the carcinogenicity of these arylamines and to better understand their mechanism of action, a range of agents, most of th...

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Bibliographic Details
Published in:Nutrition and cancer 1999, Vol.33 (1), p.46-52
Main Authors: Hammons, G.J, Fletcher, J.V, Stepps, K.R, Smith, E.A, Balentine, D.A, Harbowy, M.E, Kadlubar, F.F
Format: Article
Language:English
Subjects:
amines
Aminobiphenyl Compounds - metabolism
animal models
Animals
Anticarcinogenic Agents - pharmacology
antineoplastic agents
Antioxidants - pharmacology
aromatic compounds
Biological and medical sciences
Carcinogenesis, carcinogens and anticarcinogens
carcinogens
Carcinogens - metabolism
Diterpenes - pharmacology
Estrogens, Non-Steroidal - pharmacology
Flavonoids - pharmacology
Foods and miscellaneous
Gastroenterology. Liver. Pancreas. Abdomen
Humans
Imidazoles - metabolism
inhibition
Isoflavones
liver
Liver Neoplasms - chemically induced
Liver Neoplasms - metabolism
Liver Neoplasms - prevention & control
Liver. Biliary tract. Portal circulation. Exocrine pancreas
Male
Medical sciences
microsomes
Microsomes, Liver - drug effects
Microsomes, Liver - metabolism
Phenols - pharmacology
Phytoestrogens
Plant Preparations
Polymers - pharmacology
Rats
Rats, Inbred F344
Tumors
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Summary:Carcinogenic aromatic amines, including the heterocyclic amines, may pose a significant health risk to humans. To determine the potential for chemoprotective intervention against the carcinogenicity of these arylamines and to better understand their mechanism of action, a range of agents, most of them natural dietary constituents, was examined in vitro for their ability to modulate the N-hydroxylation of 2-amino-1-methyl-6-phenylimidazo[4,5-b]pyridine (PhIP) and 4-aminobiphenyl (ABP), an initial step in their bioactivation. Experiments were conducted with rat and human liver microsomes. The agents (diallyl sulfide, indole-3-carbinol, alpha-angelicalactone, cafestol/kahweol palmitates, cafestol, kahweol, benzylisothiocyanate, genistin, formononetin, daidzin, equol, biochanin A, Oltipraz, tannic acid, quercetin, ethoxyquin, green tea, and black tea) comprised a variety of chemical classes that included sulfur-containing compounds, antioxidants, flavonoids, phytoestrogens, diterpenes, and polyphenols. Several of these agents, quercetin, ethoxyquin, and black tea, were found to strongly inhibit PhIP N-hydroxylation in rat liver microsomes, resulting in a nearly 85-90% decrease in activity at 100 micromolar or 0.2%. Tannic acid and green tea, in addition to these agents, were also strong inhibitors of ABP N-hydroxylation. In human liver microsomes, each of these agents was strongly inhibitory (approx 85-95% at 100 micromolar or 0.02%) of PhIP and ABP N-hydroxylation. Theaflavins and polyphenols were judged to be the primary inhibiting components in the teas, the theaflavins showing the most potent effect. These results demonstrate that chemoprotective agents can inhibit the bioactivation of carcinogenic arylamines, and this is likely to be one of the mechanisms of protection.
ISSN:0163-5581
1532-7914
DOI:10.1080/01635589909514747