Age‐related differences in TGF‐α and proto‐oncogenes expression in rat liver after a low dose of carbon tetrachloride

1 October 1995

journal article
research article
Published by Wiley in Journal of Biochemical Toxicology

Vol. 10 (5) , 259-264
https://doi.org/10.1002/jbt.2570100506

Abstract

The resiliency of rats during early postnatal development to CCl₄ or to an interactive hepatotoxicity of chlordecone (CD) + CCl₄ has been shown to be due to an efficient stimulation of tissue repair. The objective of the current study was to investigate if this is due to efficient expression of transforming growth factor-α (TGF-α) and proto-oncogenes. Postnatally developing (20 day old) and adult (60 day old) male Sprague–Dawley rats were challenged with a single low dose of CCl₄ (100 μL/kg, ip) or corn oil. Liver samples were collected during a time course (0–96 h) after the administration of CCl₄ and used to examine TGF-α and early (c-fos) and late (H-ras and K-ras) proto-oncogenes mRNA expressions. Significant increases in TGF-α, H-ras, and K-ras gene expressions were evident as early as 12 hours after CCl₄ and peaked between 24 and 48 hours in an age-dependent manner as detected by slot-blot analysis. Results of the study revealed three- and twofold increases in TGF-α gene expression in 20 and 60 day old rats, respectively, after CCl₄. There were 3.5- and 2.5-fold increases in H-ras and 4.4- and 3.4-fold increases in K-ras in 20 and 60 day old rats, respectively. In contrast, a 10-fold increase in c-fos mRNA expression was evident in 20 day old rats 1 hour after CCl₄ treatment, returning to the baseline value by 3 hours, whereas in 60 day old rats, this increase was less than twofold. The overall findings of this study indicate that TGF-α and the early and late proto-oncogene mRNA expressions were enhanced in an age- and time-dependent manner in response to a low dose of CCl₄. These results further strengthen the view that the remarkable resiliency of rats to hepatotoxicants during early postnatal development is due to substantial increases in stimulation of hepatocellular regeneration and tissue repair mechanisms, leading to regression of liver injury and recovery. © 1996 John Wiley & Sons, Inc.

Keywords

This publication has 28 references indexed in Scilit:

Age-Related Susceptibility to Chlordecone-Potentiated Carbon Tetrachloride Hepatotoxicity and Lethality Is Due to Hepatic Quiescence
Pediatric Research, 1995
Resiliency to Amplification of Carbon Tetrachloride Hepatotoxicity by Chlordecone during Postnatal Development in Rats
Pediatric Research, 1993
Ongoing hepatocellular regeneration and resiliency toward galactosamine hepatotoxicity
Archives of Toxicology, 1992
Increased production of transforming growth factor α following acute gastric injury
Gastroenterology, 1992
Influence of Aging on Chemically Induced Hepato-Toxicity: Role of Age-Related Changes in Metabolism
Drug Metabolism Reviews, 1989
Developmental expression of transforming growth factors alpha and beta in mouse fetus.
Molecular and Cellular Biology, 1988
Developmental expression of rat transforming growth factor-alpha mRNA.
Molecular and Cellular Biology, 1985
Regulated transcription of c-Ki-ras and c-myc during compensatory growth of rat liver.
Molecular and Cellular Biology, 1984
Hepatotoxicity of carbon tetrachloride in developing rats
Toxicology and Applied Pharmacology, 1979
Carbon tetrachloride poisoning in the liver of the new-born rat
The Journal of Pathology and Bacteriology, 1963