Alcohol Clin Exp Res. 2014 Dec;38(12):2896-906. doi: 10.1111/acer.12576.

N-acetylcysteine inhibits the up-regulation of mitochondrial biogenesis genes in livers from rats fed ethanol chronically.

Caro AA¹, Bell M, Ejiofor S, Zurcher G, Petersen DR, Ronis MJ.

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1: Chemistry Department , Hendrix College, Conway, Arkansas.

Abstract

BACKGROUND:

Chronic ethanol (EtOH) administration to experimental animals induces hepatic oxidative stress and up-regulates mitochondrial biogenesis. The mechanisms by which chronic EtOH up-regulates mitochondrial biogenesis have not been fully explored. In this work, we hypothesized that oxidative stress is a factor that triggers mitochondrial biogenesis after chronic EtOH feeding. If our hypothesis is correct, co-administration of antioxidants should prevent up-regulation of mitochondrial biogenesis genes.

METHODS:

Rats were fed an EtOH-containing diet intragastrically by total enteral nutrition for 150 days, in the absence or presence of the antioxidant N-acetylcysteine (NAC) at 1.7 g/kg/d; control rats were administered isocaloric diets where carbohydrates substituted for EtOH calories.

RESULTS:

EtOH administration significantly increased hepatic oxidative stress, evidenced as decreased liver total glutathione and reduced glutathione/glutathione disulfide ratio. These effects were inhibited by co-administration of EtOH and NAC. Chronic EtOH increased the expression of mitochondrial biogenesis genes including peroxisome proliferator-activated receptor gamma-coactivator-1 alpha and mitochondrial transcription factor A, and mitochondrial DNA; co-administration of EtOH and NAC prevented these effects. Chronic EtOH administration was associated with decreased mitochondrial mass, inactivation and depletion of mitochondrial complex I and complex IV, and increased hepatic mitochondrial oxidative damage, effects that were not prevented by NAC.

CONCLUSIONS:

These results suggest that oxidative stress caused by chronic EtOH triggered the up-regulation of mitochondrial biogenesis genes in rat liver, because an antioxidant such as NAC prevented both effects. Because NAC did not prevent liver mitochondrial oxidative damage, extra-mitochondrial effects of reactive oxygen species may regulate mitochondrial biogenesis. In spite of the induction of hepatic mitochondrial biogenesis genes by chronic EtOH, mitochondrial mass and function decreased probably in association with mitochondrial oxidative damage. These results also predict that the effectiveness of NAC as an antioxidant therapy for chronic alcoholism will be limited by its limited antioxidant effects in mitochondria, and its inhibitory effect on mitochondrial biogenesis.

KEYWORDS:

Ethanol; Liver; Mitochondria; N-Acetylcysteine; Oxidative Stress

PMID:: 25581647
PMCID:: PMC4293075
DOI:: 10.1111/acer.12576

[Indexed for MEDLINE]

Free PMC Article

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Figure 2

Effect of ethanol and NAC on biochemical markers of mitochondrial biogenesis. Liver RNA, liver lysates and genomic DNA were isolated from rats administered ethanol (EtOH), ethanol and NAC (EtOH+NAC), NAC alone (NAC) or a control isocaloric diet (Control) by total enteral nutrition as described under Materials and Methods. (A) PGC-1α mRNA levels were quantified by real time-reverse transcriptase PCR using specific primers, normalized to β-actin and expressed as fold induction over the control group; (B) PGC-1α protein levels were quantified by western blot using specific antibodies, using beta actin as loading control. Numbers below the blots represent the relative density of the PGC-1α protein bands normalized to β-actin and expressed as fold induction over the control group; (C) TFAM mRNA levels were quantified by real time-reverse transcriptase PCR using specific primers, normalized to β-actin and expressed as fold induction over the control group; (D) TFAM protein levels were quantified by western blot using specific antibodies, using beta actin as loading control. Numbers below the blots represent the relative density of the PGC-1α protein bands normalized to β-actin and expressed as fold induction over the control group; (E) Mitochondrial DNA was quantified by real time PCR using specific primers, normalized to a nuclear DNA gene and expressed as fold induction over the control group. (F) Activation of p38 MAPK was assessed by evaluating protein levels of phosphorylated p38 (pp38) and total p38 (p38) MAPK by western blot using specific antibodies. Numbers below the blots represent the ratio of pp38 MAPK/p38 MAPK.
Data are expressed as mean ± standard error of the mean from 4 independent experiments. Shown are representative western blots. Two-way ANOVA analysis for every panel indicated a non-significant effect of ethanol (p>0.05), a significant effect of NAC (p<0.050) and a non-significant (ethanol × NAC) interaction (p>0.05).
* significantly different (p<0.05) with respect to the control group.
# significantly different (p<0.05) with respect to the same treatment, but in the absence of NAC.

N-acetylcysteine inhibits the upregulation of mitochondrial biogenesis genes in livers from rats fed ethanol chronically

Alcohol Clin Exp Res. ;38(12):2896-2906.

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N-acetylcysteine inhibits the up-regulation of mitochondrial biogenesis genes in livers from rats fed ethanol chronically.

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