Novel mechanisms in chemically induced hepatotoxicity
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Mehendale, Harihara M.; Roth, Robert A.; Gandolfi, A. Jay; Klaunig, James E.; Lemasters, John J.; Curtis, Lawrence R.

doi:10.1096/fasebj.8.15.8001741

Cited by 106 publications

(55 citation statements)

References 1 publication

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“…Thioacetamide-induced liver injury is a well established area of considerable pharmacological interest, since reactive oxygen species and free radicals, generated in the microsomal drug oxidation, participate in the mechanisms of cell death (Cascales et al, 1991;Mehendale et al, 1994;Sanz et al, 1998b). In the present study thioacetamide hepatotoxicity was used to investigate the e ect of a single dose of aminoguanidine on the multistep events involved in liver damage and regeneration.…”

Section: Discussionmentioning

confidence: 98%

Influence of aminoguanidine on parameters of liver injury and regeneration induced in rats by a necrogenic dose of thioacetamide

Dı́ez-Fernández

Sanz

Álvarez

et al. 1998

British J Pharmacology

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1 When aminoguanidine, a nucleophilic hydrazine compound, was administered to rats (50 mg kg 71 body wt) 30 min before a necrogenic dose of thioacetamide (500 mg kg 71 body wt), signi®cant changes related to liver injury and hepatocellular regeneration were observed. 2 The extent of necrosis was noticeably less pronounced, as detected by the peak of serum aspartate aminotransferase activity. Depletion of hepatic glutathione (GSH) and the increase in malondialdehyde concentration as markers of oxidative stress, produced by thioacetamide metabolism, were signi®cantly diminished. However, the activity of microsomal FAD monooxygenase, the system responsible for thioacetamide oxidation, did not show signi®cant alterations. Antioxidant enzyme systems involved in the glutathione redox cycle, such as glutathione reductase and glutathione peroxidase activities, slightly decreased following aminoguanidine pretreatment. 3 Primary cultures of peritoneal macrophages from control rats, when incubated in the presence of serum collected following thioacetamide intoxication, showed a signi®cant decrease in nitric oxide (NO) release at 24 h, that was more pronounced in the group pretreated with aminoguanidine. However, the sharp and progressive increase in macrophage NO release, when incubated in the presence of serum obtained at 48, 72 and 96 h, were increased by aminoguanidine-pretreatment. 4 The cell population involved in DNA synthesis sharply increased in both groups at 48 h of intoxication, although the values at 0, 24, 72 and 96 h were markedly higher in the group pre-treated with aminoguanidine. Polyploidy at 72 and 96 h of intoxication was delayed by the e ect of aminoguanidine and a progressive increase in the hypodiploid hepatocyte population, which reached 16% of the total at 96 h, was observed. 5 These results indicate that a single dose of aminoguanidine before thioacetamide administration, markedly diminished the severity of the liver injury by decreasing oxidative stress and lipoperoxidation, but hepatocellular regeneration was apparently una ected probably due to an enhanced mitogenic activity.

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Section: Discussionmentioning

confidence: 98%

Influence of aminoguanidine on parameters of liver injury and regeneration induced in rats by a necrogenic dose of thioacetamide

Dı́ez-Fernández

Sanz

Álvarez

et al. 1998

British J Pharmacology

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“…An electron is added to CCl 4 on binding to ferric cytochrome P 450 , resulting in a highly reactive trichloromethyl free radical being generated by the reductive cleavage of the carbon-chloride bond. The generated trichloromethyl free radical causes liver cell necrosis as well as destruction of the extracellular matrix, through lipid peroxidation of membranes [31,33]. In addition to its cytotoxic effects, CCl 4 activates several transcription factors [31], including NF-B [34], a transcription factor complex essentially involved in several inflammatory cytokines, including IL-6 [35].…”

Section: Discussionmentioning

confidence: 99%

Attenuated liver fibrosis and depressed serum albumin levels in carbon tetrachloride-treated IL-6-deficient mice

Natsume

Tsuji

Harada

et al. 1999

Journal of Leukocyte Biology

105

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Chronic intermittent injection of carbon tetrachloride (CCl 4 ) for more than 10 weeks induced liver fibrosis in mice, as evidenced by positive Azan staining and increased intrahepatic collagen content. Preceding the onset of liver fibrosis, interleukin-6 (IL-6) gene expression was enhanced in liver and immunoreactive IL-6 was detected in infiltrating inflammatory cells. To delineate the role of IL-6 in this process, we treated IL-6-deficient mice with CCl 4 in a similar manner for 12 weeks, after which fibrotic changes were less evident and serum albumin levels were lower in IL-6-deficient than wild-type mice. Moreover, CCl 4 -induced expression of transforming growth factor ␤ 1 and hepatocyte growth factor genes in liver was significantly reduced in IL-6-deficient mice. Thus, IL-6 may be vitally involved in fibrotic changes and maintenance of serum albumin levels, partly by modulating intrahepatic expression of these cytokines. J. Leukoc. Biol. 66: 601-608; 1999.

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“…24 In contrast, liver damage caused by hepatotoxic chemicals induces compensatory hepatic hyperplasia after severe liver necrosis due to direct damage of hepatocytes and subsequent inflammation. 25 To determine if Nrf2 is also protective under these more harmful conditions, we utilized CCl 4 as a model hepatotoxic agent that allowed the evaluation of both necrosis and subsequent inflammation 26 and fibrosis. 17 Furthermore, acute CCl 4 treatment had recently been shown to induce nuclear translocation of Nrf2 and activation of the Nrf2 target gene heme oxygenase-1.…”

Section: Nrf2 Protects From Acute CCL 4 -Induced Liver Damagementioning

confidence: 99%

The Nrf2 transcription factor protects from toxin-induced liver injury and fibrosis

Hellerbrand

Köhler

et al. 2008

Laboratory Investigation

180

116

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The liver is frequently exposed to insults, including toxic chemicals and alcohol, viral infection or metabolic overload. Although it can fully regenerate after acute injury, chronic liver damage causes liver fibrosis and cirrhosis, which can result in complete liver failure. In this study, we demonstrate that the NF-E2-related factor 2 (Nrf2) transcription factor protects the liver from acute and chronic toxin-mediated damage. Repair of the liver injury that occurs after a single treatment with the hepatotoxin carbon tetrachloride (CCl 4 ) was severely delayed in Nrf2-deficient mice. The defect in repair was accompanied by an enhanced and prolonged inflammatory and profibrotic response. After long-term CCl 4 treatment, liver fibrosis was strongly aggravated in the Nrf2 knockout mice and inflammation was enhanced. We demonstrate that these abnormalities are at least in part due to the reduced expression of known and novel Nrf2 target genes in hepatocytes, which encode enzymes involved in the detoxification of CCl 4 and its metabolites. These results suggest that activation of Nrf2 may be a novel strategy to prevent or ameliorate toxin-induced liver injury and fibrosis.

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Novel mechanisms in chemically induced hepatotoxicity ¹

Cited by 106 publications

References 1 publication

Influence of aminoguanidine on parameters of liver injury and regeneration induced in rats by a necrogenic dose of thioacetamide

Influence of aminoguanidine on parameters of liver injury and regeneration induced in rats by a necrogenic dose of thioacetamide

Attenuated liver fibrosis and depressed serum albumin levels in carbon tetrachloride-treated IL-6-deficient mice

The Nrf2 transcription factor protects from toxin-induced liver injury and fibrosis

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Novel mechanisms in chemically induced hepatotoxicity 1

Cited by 106 publications

References 1 publication

Influence of aminoguanidine on parameters of liver injury and regeneration induced in rats by a necrogenic dose of thioacetamide

Influence of aminoguanidine on parameters of liver injury and regeneration induced in rats by a necrogenic dose of thioacetamide

Attenuated liver fibrosis and depressed serum albumin levels in carbon tetrachloride-treated IL-6-deficient mice

The Nrf2 transcription factor protects from toxin-induced liver injury and fibrosis

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Product

Resources

About

Novel mechanisms in chemically induced hepatotoxicity ¹