Ursodeoxycholic acid stimulates Nrf2-mediated hepatocellular transport, detoxification, and antioxidative stress systems in mice

Okada, Kōsuke; Shoda, Junichi; Taguchi, Keiko; Maher, Jonathan; Ishizaki, Kaoru; Inoue, Yoshimi; Ohtsuki, M; Gotô, Nobuharu; Takeda, Koichi; Utsunomiya, Hirotoshi; Oda, Koji; Warabi, Eiji; Ishii, Tetsuro; Osaka, Keiko; Hyodo, Ichinosuke; Yamamoto, Masayuki

doi:10.1152/ajpgi.90321.2008

Cited by 128 publications

(106 citation statements)

References 41 publications

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“…Our data are in agreement with the observation that CDCA treatment activated Nrf2 and induced its target genes in the liver and intestinal cells (Tan et al, 2007). Ursodeoxycholic acid, another bile acid, has been used in clinical studies to treat liver diseases including primary biliary cirrhosis, and a large part of its beneficial aspect may be attributable to its property of Nrf2 activation (Okada et al, 2008;Kawata et al, 2010). Hence, it is presumed that an enhanceosome complex containing C/EBP␤ and Nrf2 may work together in inducing target genes by CDCA.…”

Section: Noh Et Alsupporting

confidence: 91%

Farnesoid X Receptor Activation by Chenodeoxycholic Acid Induces Detoxifying Enzymes through AMP-Activated Protein Kinase and Extracellular Signal-Regulated Kinase 1/2-Mediated Phosphorylation of CCAAT/Enhancer Binding Protein β

Noh

Kim

et al. 2011

Drug Metab Dispos

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Section: Noh Et Alsupporting

confidence: 91%

Farnesoid X Receptor Activation by Chenodeoxycholic Acid Induces Detoxifying Enzymes through AMP-Activated Protein Kinase and Extracellular Signal-Regulated Kinase 1/2-Mediated Phosphorylation of CCAAT/Enhancer Binding Protein β

Noh

Kim

et al. 2011

Drug Metab Dispos

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“…Of note, in our previous experience (unpublished), such systemic effects on any of these systems were not observed when sulforaphane, another potent Nrf2 activator, was topically administered under similar experimental conditions. MRP4 participates in the export of nucleoside monophosphate analogs (41)(42)(43), and its inducible gene expression is known to be regulated by Nrf2 (40,44,45). Furthermore, silencing of mrp4 increases the 6-TG incorporation in DNA of Hepa1c1c7 cells treated with this thiopurine (36).…”

Section: Resultsmentioning

confidence: 99%

“…The primers and probe used to measure mRNA for MRP4 (40) were synthesized by MWG-Biotech UK Ltd. Total RNA from mouse liver and skin was extracted using RNeasy and RNeasy Fibrous Tissue Kit (Qiagen Ltd.), respectively. Total RNA (500 ng) was reverse transcribed into cDNA with Omniscript Reverse Transcription Kit (Qiagen Ltd.).…”

Section: Quantitative Reverse Transcriptase Pcrmentioning

confidence: 99%

Highly Potent Activation of Nrf2 by Topical Tricyclic Bis(Cyano Enone): Implications for Protection against UV Radiation during Thiopurine Therapy

Kalra

Knatko

Zhang

et al. 2012

Cancer Prevention Research

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Chronic treatment with azathioprine, a highly effective anti-inflammatory and immunosuppressive agent, profoundly increases the risk for development of unusually aggressive cutaneous squamous cell carcinoma. Its ultimate metabolite, 6-thioguanine (6-TG) nucleotide, is incorporated in DNA of skin cells, and upon exposure to UVA radiation, causes oxidative stress, followed by damage of DNA and associated proteins. The acetylenic tricyclic bis(cyano enone) TBE-31 is a strong inhibitor of inflammation and a potent inducer of the Keap1/Nrf2/ARE pathway, which orchestrates the expression of a large network of cytoprotective genes. We now report that long-term (five days per week for four weeks) topical daily applications of small (200 nmol) quantities of TBE-31 cause a robust systemic induction of the Keap1/Nrf2/ ARE pathway and decreases the 6-TG incorporation in DNA of skin, blood, and liver of azathioprine-treated mice, indicating extraordinary bioavailability and efficacy. In addition, TBE-31, at nanomolar concentrations, protects cells with 6-TG in their genomic DNA against oxidative stress caused by UVA radiation through induction of the Keap1/Nrf2/ARE pathway. At the same 6-TG DNA levels, Keap1-knockout cells, in which the pathway is constitutively upregulated, are highly resistant to UVA radiation-induced oxidative stress. The protective effects of both the Keap1-knockout genotype and TBE-31 are completely lost in the absence of transcription factor Nrf2. Our findings suggest that compounds of this kind are excellent candidates for mechanism-based chemoprotective agents against conditions in which oxidative stress and inflammation underlie disease pathogenesis. Moreover, their potential skin patch incorporation for transdermal delivery is an exciting possibility. Cancer Prev Res; 5(7); 973-81. Ó2012 AACR.

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“…Bile duct ligation or lipopolysaccharide (LPS) treatment resulted in an IL-1b-mediated RARa/RXRa downregulation, which in turn decreased ABCC2 transcription in rats (Denson et al, 2002). Oxidative stress (e.g., via toxic bile acids) can increase ABCC2 transcription via nuclear factor erythroid 2-related factor 2 in rodents (Maher et al, 2007;Okada et al, 2008). Posttranscriptional mechanisms fine tune the canalicular ABCC2 expression.…”

Section: Abcc2mentioning

confidence: 99%

The Role of Canalicular ABC Transporters in Cholestasis

et al. 2014

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Cholestasis, a hallmark feature of hepatobiliary disease, is characterized by the retention of biliary constituents. Some of these constituents, such as bile acids, inflict damage to hepatocytes and bile duct cells. This damage may lead to inflammation, fibrosis, cirrhosis, and eventually carcinogenesis, sequelae that aggravate the underlying disease and deteriorate clinical outcome. Canalicular ATP-binding cassette (ABC) transporters, which mediate the excretion of individual bile constituents, play a key role in bile formation and cholestasis. The study of these transporters and their regulatory nuclear receptors has revolutionized our understanding of cholestatic disease. This knowledge has served as a template to develop novel treatment strategies, some of which are currently already undergoing phase III clinical trials. In this review we aim to provide an overview of the structure, function, and regulation of canalicular ABC transporters. In addition, we will focus on the role of these transporters in the pathogenesis and treatment of cholestatic bile duct and liver diseases.

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Ursodeoxycholic acid stimulates Nrf2-mediated hepatocellular transport, detoxification, and antioxidative stress systems in mice

Cited by 128 publications

References 41 publications

Farnesoid X Receptor Activation by Chenodeoxycholic Acid Induces Detoxifying Enzymes through AMP-Activated Protein Kinase and Extracellular Signal-Regulated Kinase 1/2-Mediated Phosphorylation of CCAAT/Enhancer Binding Protein β

Farnesoid X Receptor Activation by Chenodeoxycholic Acid Induces Detoxifying Enzymes through AMP-Activated Protein Kinase and Extracellular Signal-Regulated Kinase 1/2-Mediated Phosphorylation of CCAAT/Enhancer Binding Protein β

Highly Potent Activation of Nrf2 by Topical Tricyclic Bis(Cyano Enone): Implications for Protection against UV Radiation during Thiopurine Therapy

The Role of Canalicular ABC Transporters in Cholestasis

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