Strong Inhibition of 2‐Amino‐6‐methyldipyrido[l,2‐a:3′,2′‐d]imidazole‐induced Mutagenesis and Hepatocarcinogenesis by 1‐O‐Hexyl‐2,3,5‐trimethylhydroquinone

The effects of 3‐O‐dodecylcarbomethylascorbic acid (3‐O‐DAsA), 3‐O‐ethylascorbic acid (3‐O‐EAsA) and 1‐O‐hexy1‐2,3,5‐trimethylhydroquinone (HTHQ) on 2‐amino‐6‐methyldipyrido[l,2‐a:3′,2′‐d]‐imidazole (Glu‐P‐1)‐induced mutagenesis and hepatocarcinogenesis were examined. In a Salmonella assay, addition...

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Published in:Cancer science 1993-05, Vol.84 (5), p.481-484
Main Authors: Hirose, Masao, Akagi, Keisuke, Hasegawa, Ryohei, Satoh, Toshio, Nihro, Yasunori, Miki, Tokutaro, Sugimura, Takashi, Ito, Nobuyuki
Format: Article
Language:English
Subjects:
Animals
Anticarcinogenic Agents - pharmacology
Antimutagenic Agents - pharmacology
Antioxidant
Antioxidants - pharmacology
Anti‐mutagenesis
Ascorbic Acid - pharmacology
Biological and medical sciences
Body Weight - drug effects
Carcinogenesis, carcinogens and anticarcinogens
Chemical agents
Chemoprevention
Hepatocarcinogenesis
Heterocyclic amine
Hydroquinones - pharmacology
Imidazole
Imidazoles - toxicity
Liver Neoplasms, Experimental - chemically induced
Liver Neoplasms, Experimental - prevention & control
Male
Medical sciences
Mutagenesis
Mutagens - toxicity
Rapid Communication
Rats
Rats, Inbred F344
Revertants
Salmonella
Tumors
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Summary:The effects of 3‐O‐dodecylcarbomethylascorbic acid (3‐O‐DAsA), 3‐O‐ethylascorbic acid (3‐O‐EAsA) and 1‐O‐hexy1‐2,3,5‐trimethylhydroquinone (HTHQ) on 2‐amino‐6‐methyldipyrido[l,2‐a:3′,2′‐d]‐imidazole (Glu‐P‐1)‐induced mutagenesis and hepatocarcinogenesis were examined. In a Salmonella assay, addition of 2.5 to 20.0 rag of HTHQ to Salmonella TA 98 in the presence of S‐9 mixture dose‐dependently inhibited Glu‐P‐1‐induced mutagenesis. The highest dose showed a 99% reduction in revertants. 3‐O‐DAsA and 3‐O‐EAsA were without effect. In an animal study using the medium‐term bioassay system for the detection of hepatocarcinogens or hepatopromoters in F344 male rats, treatment with Glu‐P‐1 alone was associated with a significant increase in the number and area of GST‐P‐positive foci (47.5±8.9 and 11.1±4.7, respectively). Combined treatment with 1.0% HTHQ significantly reduced the number and area of GST‐P‐positive foci (to 8.1±2.1 and 0.6±0.2) while 3‐O‐DASA exerted marginal inhibition and 3‐O‐EAsA had no effect. On the other hand, all three of these compounds slightly enhanced the numbers and areas of foci when given alone. The results indicate that HTHQ is a potent chemopreventer of Glu‐P‐1‐induced hepatocarcinogenesis.
ISSN:0910-5050
1347-9032
1349-7006
1876-4673
DOI:10.1111/j.1349-7006.1993.tb00162.x