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[Effect of hepatocarcinogenicity of estragole on the glucocorticoid-mediated induction of liver-specific enzymes and the activity of the transcription factors FOXA and HNF4 in the liver of mouse and rat].

Authors :
Kaledin VI
Pakharukova MIu
Pivovarova EN
Kropachev KIu
Baginskaia NV
Vasil'eva ED
Il'nitskaia SI
Nikitenko EV
Kobzev VF
Merkulova TI
Source :
Biofizika [Biofizika] 2010 Mar-Apr; Vol. 55 (2), pp. 326-35.
Publication Year :
2010

Abstract

The carcinogenic effects of estragole in mice of the earlier unexplored strain ICR has been studied. It has been shown that there is a distinct correlation between the extent of inhibition of glucocorticoid-mediated induction of tyrosine aminotransferase and trypthophan oxygenase after acute administration of estragole and the frequency of liver tumors after estragole exposure. Estragole inhibits the induction of these enzymes only in female mice, but not in male mice and rats. DNA-binding activities of liver-enriched transcription factors were investigated on carcinogen-susceptible and -resistant animals. Estragole decreases the HNF4 (hepatic nuclear factor 4) and FOXA DNA-binding activities only in susceptible female mice, but not in nonsusceptible male mice and rats and does not influence the C/EBP and HNF1 activities. Pentachlorophenol, which prevents the hepatocarcinogenic effect of estragole, abolishes its inhibitory effect on tyrosine aminotransferase and trypthophan oxygenase glucocorticoid induction and restores the FOXA and HNF4 DNA-binding activities. The parallelism between the hepatocarcinogenic effects of estragole and the inhibition of FOXA and HNF4 DNA-binding activities serves as an additional argument for the involvement of these factors in the mechanisms of tumor suppression in the liver.

Details

Language :
Russian
ISSN :
0006-3029
Volume :
55
Issue :
2
Database :
MEDLINE
Journal :
Biofizika
Publication Type :
Academic Journal
Accession number :
20429289