Age-dependent modifications in rat hepatocyte antioxidant defense systems

Abstract

Background/Aims: Age-dependent changes in the hepatic antioxidant systems were studied in hepatocytes from newly weaned (21 days) to 30-month-old rats. Results: Biphasic changes were observed in superoxide dismutase (SOD), glucose-6-phosphate dehydrogenase (G6PDH) and malic enzyme (ME), in which noticeable decreases were detected in hepatocytes from newly weaned to 6-month-old rats: Cu-Zn SOD decreased to 46% ( p<0.001), Mn SOD to 41% ( p<0.001), G6PDH to 71% and ME to 19% ( p<0.001), and significant increases were observed from 6 to 30 months. In hepatocytes from 6- to 30-month-old rats the enzymes involved in antioxidant defense underwent increases in their activities as well in their mRNA: Cu-Zn SOD (142%, p<0.001), catalase (182%. p<0.001) and glutathione peroxidase (325%, p<0.001). However, chronological decreases were observed in the levels of reduced glutathione (69%, p<0.001), in the GSH/GSSG ratio (78%) and in protein thiol groups (55%, p<0.001), with concomitant increases in peroxidases (155%, p<0.001) and malondialdehyde (142%, p<0.001). DNA ploidy was also assayed by flow cytometry; a sharp increase in tetraploid (2.5–40.1%; p<0.001) and octoploid (0.1–16.1%; p<0.001) populations, and a noticeable decrease in diploid hepatocytes (92.9-34.3%; p<0.001), were observed. Populations involved in 2C→4C DNA synthesis decreased from 3.6 to 0.9% ( p<0.001), while those involved in 4C→8C increased from 0.9% to 5.2% ( p<0.001). A hypodiploid population (apoptotic cells) was detected from 12 months, increasing thereafter. Conclusions: These results show that the antioxidant cell defense system increases with age but the rate of reactive oxygen species generation exceeds the induced antioxidant ability, generating a situation that favors oxidative stress and peroxidation. The progressive polyploidization is accompanied by changes in the proliferative potential that decreases from 2C to 4C and increased from 4C to 8C. The relationship between the modifications of the oxidant/antioxidant system and increased polyploidy is not clear and may be interpreted as two independent manifestations of the aging process.