Your search keyword '"Boyer, James L."' showing total 18 results

1. PPAR-Mediated Bile Acid Glucuronidation: Therapeutic Targets for the Treatment of Cholestatic Liver Diseases.

Author

Gallucci, Gina M., Hayes, Colleen M., Boyer, James L., Barbier, Olivier, Assis, David N., and Ghonem, Nisanne S.

Subjects

PEROXISOME proliferator-activated receptors, BILE acids, GLUCURONIDATION, CYTOCHROME P-450, URSODEOXYCHOLIC acid, FARNESOID X receptor

Abstract

Cholestatic liver diseases, including primary biliary cholangitis (PBC) and primary sclerosing cholangitis (PSC), result from an impairment of bile flow that leads to the hepatic retention of bile acids, causing liver injury. Until recently, the only approved treatments for PBC were ursodeoxycholic acid (UDCA) and obeticholic acid (OCA). While these therapies slow the progression of PBC in the early stage of the disease, approximately 40% of patients respond incompletely to UDCA, and advanced cases do not respond. UDCA does not improve survival in patients with PSC, and patients often have dose-limiting pruritus reactions to OCA. Left untreated, these diseases can progress to fibrosis and cirrhosis, resulting in liver failure and the need for transplantation. These shortcomings emphasize the urgent need for alternative treatment strategies. Recently, nuclear hormone receptors have been explored as pharmacological targets for adjunct therapy because they regulate enzymes involved in bile acid metabolism and detoxification. In particular, the peroxisome proliferator-activated receptor (PPAR) has emerged as a therapeutic target for patients with PBC or PSC who experience an incomplete response to UDCA. PPARα is predominantly expressed in the liver, and it plays an essential role in the regulation of cytochrome P450 (CYP) and uridine 5'-diphospho-glucuronosyltransferase (UGT) enzymes, both of which are critical enzyme families involved in the regulation of bile acid metabolism and glucuronidation, respectively. Importantly, PPARα agonists, e.g., fenofibrate, have shown therapeutic benefits in reducing elevated markers of cholestasis in patients with PBC and PSC, and elafibranor, the first PPAR (dual α, β/δ) agonist, has been FDA-approved for the second-line treatment of PBC. Additionally, newer PPAR agonists that target various PPAR isoforms (β/δ, γ) are under development as an adjunct therapy for PBC or PSC, although their impact on glucuronidation pathways are less characterized. This review will focus on PPAR-mediated bile acid glucuronidation as a therapeutic pathway to improve outcomes for patients with PBC and PSC. [ABSTRACT FROM AUTHOR]

Published

2024

2. Expression Cloning of Two Genes That Together Mediate Organic Solute and Steroid Transport in the Liver of a Marine Vertebrate

Author

Wang, Wei, Seward, David J., Li, Liqiong, Boyer, James L., and Ballatori, Nazzareno

Published

2001

3. Structural and Functional Polarity of Canalicular and Basolateral Plasma Membrane Vesicles Isolated in High Yield from Rat Liver

Author

Meier, Peter J., Sztul, Elizabeth S., Reuben, Adrian, and Boyer, James L.

Published

1984

4. Regulation of Activity and Apical Targeting of the Cl - /HCO - 3 Exchanger in Rat Hepatocytes

Author

Benedetti, Antonio, Strazzabosco, Mario, Ng, Oi Cheng, and Boyer, James L.

Published

1994

5. Phalloidin-Induced Cholestasis: A Microfilament-Mediated Change in Junctional Complex Permeability

Author

Elias, Elwyn, Hruban, Zdenek, Wade, James B., and Boyer, James L.

Published

1980

6. Adjunct Fenofibrate Up‐regulates Bile Acid Glucuronidation and Improves Treatment Response For Patients With Cholestasis.

Author

Gallucci, Gina M., Trottier, Jocelyn, Hemme, Christopher, Assis, David N., Boyer, James L., Barbier, Olivier, and Ghonem, Nisanne S.

Subjects

MULTIDRUG resistance-associated proteins, FENOFIBRATE, BILE acids, LIQUID chromatography-mass spectrometry, GLUCURONIDATION

Abstract

Accumulation of cytotoxic bile acids (BAs) during cholestasis can result in liver failure. Glucuronidation, a phase II metabolism pathway responsible for BA detoxification, is regulated by peroxisome proliferator–activated receptor alpha (PPARα). This study investigates the efficacy of adjunct fenofibrate therapy to up‐regulate BA‐glucuronidation and reduce serum BA toxicity during cholestasis. Adult patients with primary biliary cholangitis (PBC, n = 32) and primary sclerosing cholangitis (PSC, n = 23), who experienced an incomplete response while receiving ursodiol monotherapy (13‐15 mg/kg/day), defined as serum alkaline phosphatase (ALP) ≥ 1.5 times the upper limit of normal, received additional fenofibrate (145‐160 mg/day) as standard of care. Serum BA and BA‐glucuronide concentrations were measured by liquid chromatography–mass spectrometry. Combination therapy with fenofibrate significantly decreased elevated serum ALP (−76%, P < 0.001), aspartate transaminase, alanine aminotransferase, bilirubin, total serum BAs (−54%), and increased serum BA‐glucuronides (+2.1‐fold, P < 0.01) versus ursodiol monotherapy. The major serum BA‐glucuronides that were favorably altered following adjunct fenofibrate include hyodeoxycholic acid–6G (+3.7‐fold, P < 0.01), hyocholic acid–6G (+2.6‐fold, P < 0.05), chenodeoxycholic acid (CDCA)–3G (−36%), and lithocholic acid (LCA)–3G (−42%) versus ursodiol monotherapy. Fenofibrate also up‐regulated the expression of uridine 5′‐diphospho‐glucuronosyltransferases and multidrug resistance–associated protein 3 messenger RNA in primary human hepatocytes. Pearson's correlation coefficients identified strong associations between serum ALP and metabolic ratios of CDCA‐3G (r2 = 0.62, P < 0.0001), deoxycholic acid (DCA)‐3G (r2 = 0.48, P < 0.0001), and LCA‐3G (r2 = 0.40, P < 0.001), in ursodiol monotherapy versus control. Receiver operating characteristic analysis identified serum BA‐glucuronides as measures of response to therapy. Conclusion: Fenofibrate favorably alters major serum BA‐glucuronides, which correlate with reduced serum ALP levels and improved outcomes. A PPARα‐mediated anti‐cholestatic mechanism is involved in detoxifying serum BAs in patients with PBC and PSC who have an incomplete response on ursodiol monotherapy and receive adjunct fenofibrate. Serum BA‐glucuronides may serve as a noninvasive measure of treatment response in PBC and PSC. [ABSTRACT FROM AUTHOR]

Published

2021

7. Fenofibrate Improves Liver Function and Reduces the Toxicity of the Bile Acid Pool in Patients With Primary Biliary Cholangitis and Primary Sclerosing Cholangitis Who Are Partial Responders to Ursodiol.

Author

Ghonem, Nisanne S., Auclair, Adam M., Hemme, Christopher L., Gallucci, Gina M., Rosa Rodriguez, Randolph, Boyer, James L., and Assis, David N.

Subjects

BILE acids, ASPARTATE aminotransferase, DEOXYCHOLIC acid, PEROXISOME proliferator-activated receptors, FENOFIBRATE, CHOLANGITIS, PRINCIPAL components analysis, ALANINE aminotransferase

Abstract

Cholestatic liver diseases result in the hepatic retention of bile acids, causing subsequent liver toxicity. Peroxisome proliferator‐activated receptor alpha (PPARα) regulates bile acid metabolism. In this retrospective observational study, we assessed the effects of fenofibrate (a PPARα agonist) therapy on bile acid metabolism when given to patients with primary biliary cholangitis (PBC) and primary sclerosing cholangitis (PSC) who have had an incomplete response to Ursodiol monotherapy. When fenofibrate was added to Ursodiol therapy there was a significant reduction and in some cases normalization of serum alkaline phosphatase, alanine aminotransferase, and aspartate aminotransferase abnormalities, as well as pro‐inflammatory cytokines. Combination fenofibrate treatment also reduced 7α‐hydroxy‐4‐cholesten‐3‐one (C4), the bile acid precursor, as well as total, primary, and conjugated bile acids. In addition, principal components analysis and heatmap analysis show that bile acid metabolites trended closer to that of healthy control subjects. These favorable effects of fenofibrate on bile acid metabolism may contribute to its beneficial clinical effects in patients with PBC and PSC experiencing a subtherapeutic response to Ursodiol monotherapy. [ABSTRACT FROM AUTHOR]

Published

2020

8. Bile acid metabolism and T cell responses in cholangiopathy: Not one-way traffic.

Author

Shetty, Shishir and Boyer, James L.

Subjects

*INTERLEUKIN-7, *T cells, *BILE acids, *VASCULAR cell adhesion molecule-1, *BILIARY liver cirrhosis, *CHOLANGITIS, *CELL metabolism

Abstract

Cholangiocytes, also termed biliary epithelial cells, make a vital contribution to liver physiology and in maintaining homeostasis within the liver microenvironment.[1] They line the biliary tree and play a central role in regulating bile composition through the secretion of water, electrolytes and solutes via the expression of a range of membrane transporters. With this model they find that the transfer of T cells leads to the transcriptional downregulation of key bile acid metabolic enzymes responsible for bile acid synthesis in both the classical and alternative pathways, as well as upregulation of the BSEP. This was accompanied by a decrease in the quantity of unconjugated bile acids with an increase in conjugated bile acid in both serum and liver after T cell transfer. This study suggests that novel approaches for T cell therapy in cholangiopathies need to be designed to prevent progressive tissue injury while maintaining the beneficial effects of T cells on bile acid metabolism. [Extracted from the article]

Published

2019

9. A Novel Di-Leucine Motif at the N-Terminus of Human Organic Solute Transporter Beta Is Essential for Protein Association and Membrane Localization.

Author

Xu, Shuhua, Soroka, Carol J., Sun, An-Qiang, Backos, Donald S., Mennone, Albert, Suchy, Frederick J., and Boyer, James L.

Subjects

LEUCINE, MEMBRANE proteins, BILE acids, PROTEIN-protein interactions, IMMUNOPRECIPITATION

Abstract

The heteromeric membrane protein Organic Solute Transporter alpha/beta is the major bile acid efflux transporter in the intestine. Physical association of its alpha and beta subunits is essential for their polarized basolateral membrane localization and function in the transport of bile acids and other organic solutes. We identified a highly conserved acidic dileucine motif (-EL20L21EE) at the extracellular amino-tail of organic solute transporter beta from multiple species. To characterize the role of this protein interacting domain in the association of the human beta and alpha subunits and in membrane localization of the transporter, Leu20 and Leu21 on the amino-tail of human organic solute transporter beta were replaced with alanines by site-directed mutagenesis. Co-immunoprecipitation study in HEK293 cells demonstrated that substitution of the leucine residues with alanines prevented the interaction of the human beta mutant with the alpha subunit. Membrane biotinylation demonstrated that the LL/AA mutant eliminated membrane expression of both subunits. Computational-based modelling of human organic solute transporter beta suggested that the LL/AA mutation substantially alters both the structure and lipophilicity of the surface, thereby not only affecting the interaction with the alpha subunit but also possibly impacting the capacity of the beta subunit to traffick through the cell and interact with the membrane. In summary, our findings indicate that the dileucine motif in the extracellular N-terminal region of human organic solute transporter beta subunit plays a critical role in the association with the alpha subunit and in its polarized plasma membrane localization. [ABSTRACT FROM AUTHOR]

Published

2016

10. Biosynthesis and trafficking of the bile salt export pump, BSEP: Therapeutic implications of BSEP mutations.

Author

Soroka, Carol J. and Boyer, James L.

Subjects

*ATP-binding cassette transporters, *GENETIC mutation, *BILE acids, *LIVER cells, *RATE determining steps (Chemistry), *ENTEROHEPATIC circulation, *PROTEIN synthesis, *GENETIC translation

Abstract

Abstract: The bile salt export pump (BSEP, ABCB11) is the primary transporter of bile acids from the hepatocyte to the biliary system. This rate-limiting step in bile formation is essential to the formation of bile salt dependent bile flow, the enterohepatic circulation of bile acids, and the digestion of dietary fats. Mutations in BSEP are associated with cholestatic diseases such as progressive familial intrahepatic cholestasis type 2 (PFIC2), benign recurrent intrahepatic cholestasis type 2 (BRIC2), drug-induced cholestasis, and intrahepatic cholestasis of pregnancy. Development of clinical therapies for these conditions necessitates a clear understanding of the cell biology of biosynthesis, trafficking, and transcriptional and translational regulation of BSEP. This chapter will focus on the molecular and cell biological aspects of this critical hepatic membrane transporter. [Copyright &y& Elsevier]

Published

2014

11. Osta depletion protects liver from oral bile acid load.

Author

Soroka, Carol J., Velazquez, Heino, Mennone, Albert, Ballatori, Nazzareno, and Boyer, James L.

Subjects

HOMEOSTASIS, CHOLESTASIS, BILE ducts, BILE acids, TUBAL sterilization

Abstract

Bile acid homeostasis is tightly maintained through interactions between the liver, intestine, and kidney. During cholestasis, the liver is incapable of properly clearing bile acids from the circulation, and alternative excretory pathways are utilized. In obstructive cholestasis, urinary elimination is often increased, and this pathway is further enhanced after bile duct ligation in mice that are genetically deficient in the heteromeric, basolateral organic solute transporter alpha-beta (Ostα-Ostβ). In this study, we examined renal and intestinal function in Ostcs-deficient and wild-type mice in a model of bile acid overload. After 1% cholic acid feeding, Ostα-deficient mice had significantly lower serum ALT levels compared with wild-type controls, indicating partial protection from liver injury. Urinary clearance of bile acids, but not clearance of [³H]inulin, was significantly higher in cholic acid-fed Ostα-deficient mice compared with wild-type mice but was not sufficient to account for the protection. Fecal excretion of bile acids over the 5 days of cholic acid feeding was responsible for almost all of the bile acid loss in Ostα-deficient mice, suggesting that intestinal losses of bile acids accounted for the protection from liver injury. Thus fecal loss of bile acids after bile acid overload reduced the need for the kidney to filter and excrete the excess bile acids. In conclusion, Ostα-deficient mice efficiently eliminate excess bile acids via the feces. Inhibition of intestinal bile acid absorption might be an effective therapeutic target in early stages of cholestasis when bile acids are still excreted into bile. [ABSTRACT FROM AUTHOR]

Published

2011

12. Phioracetophenone-induced choleresis in rats is mediated through Mrp2.

Author

Tradtrantip, Lukmanee, Piyachaturawat, Pawinee, Soroka, Carol J., Harry, Kathy, Mennone, Albert, Mahagita, Chitrawina, Ballatori, Nazzareno, and Boyer, James L.

Subjects

BILE duct diseases, BILIARY tract, DIGESTIVE organs, LABORATORY rats, BILE acids

Abstract

Phloracetophenone (2,4,6-trihydroxyacetophenone, THA) is a potent choleretic in the bile fistula rat, although the mechanism is unknown. In the present study, we examined how THA enhances bile secretion. Stepwise infusions of THA (1-4 εmol/min) in the isolated perfused rat liver resulted in an immediate and dose-dependent increase in bile flow (BF), which reached saturation. The increase in BF was not associated with a change in the excretion of bile acids, suggesting that THA stimulated bile acid-independent bile flow. To further define the mechanism, the effect of THA on the excretion of sulfobromophthalein (BSP) and disulfobromophthalein (DBSP), typical multidrug resistance protein-2 (Mrp2) substrates was examined. THA inhibited the biliary excretion of both substrates. Because DBSP is excreted without conjugation to glutathione, in contrast to BSP, the findings suggest that THA might compete with DBSP and BSP metabolites at a common canalicular transport site, presumably Mrp2. THA infusions had no effect on the subcellular localization and distribution of either Mrp2 or the bile salt export pump (Bsep), nor the integrity of the tight junction. In contrast, the choleretic activity of THA was completely absent in the TR- rat, an animal model that lacks Mrp2, directly implicating this canalicular export pump as the mechanisms by which THA is excreted in bile. THA also partially reversed the cholestatic effects of estradiol-17β-D-glucuronide, a process also dependent on Mrp2. In conclusion, the choleretic activity of THA and its possible metabolites is dependent on Mrp2. THA appears to stimulate BF by its osmotic effects and may attenuate the cholestatic effects of hepatotoxins undergoing biotransformation and excretion via similar pathways. [ABSTRACT FROM AUTHOR]

Published

2007

13. Upregulation of a basolateral FXR-dependent bile acid efflux transporter OSTα-OSTβ in cholestasis in humans and rodents.

Author

Boyer, James L., Trauner, Michael, Mennone, Albert, Soroka, Carol J., Shi-ying Cai, Moustafa, Tarek, Zollner, Gernot, Un Young Lee, and Ballatori, Nazzareno

Subjects

*BILE acids, *STEROID-binding proteins, *CHOLESTASIS, *KIDNEYS, *URINARY organs

Abstract

Organic solute transporter (OSTα-OSTβ) is a novel heteromeric bile acid and sterol transporter expressed at the basolateral membranes of epithelium in the ileum, kidney, and liver. To determine whether OSTα-OSTβ undergoes farnesoid X receptor (FXR)-dependent adaptive regulation following cholestatic liver injury, mRNA and protein expression levels were analyzed in patients with primary biliary cirrhosis (PBC) and following common bile duct ligation (CBDL) in rats and Fxr null and wild-type mice. Hepatic OSTα and OSTβ mRNA increased 3- and 32-fold, respectively, in patients with PBC com- pared with controls, whereas expression of Ostα and Ostβ also increased in the liver of rats and mice following CBDL. In contrast, expression of Ostα and Ostβ mRNA was generally lower in Fxr null mice, and CBDL failed to enhance expression of Ostαr and Ostβ compared with wild-type mice. HepG2 cells treated for 24 h with chenodeoxycholic acid, a selective FXR ligand, had higher levels of OSTα and OSTβ mRNA and protein. Increases in OST protein were visualized by confocal microscopy at the plasma membrane. These results indicate that expression of Ostα and Ostβ are highly regulated in response to cholestasis and that this response is dependent on the FXR bile acid receptor. [ABSTRACT FROM AUTHOR]

Published

2006

14. Mechanisms of bile acid mediated inflammation in the liver.

Author

Li, Man, Cai, Shi-Ying, and Boyer, James L.

Subjects

*BILE acids, *HEPATITIS, *CHOLESTASIS, *LIVER cells, *BLOOD serum analysis

Abstract

Bile acids are synthesized in the liver and are the major component in bile. Impaired bile flow leads to cholestasis that is characterized by elevated levels of bile acid in the liver and serum, followed by hepatocyte and biliary injury. Although the causes of cholestasis have been extensively studied, the molecular mechanisms as to how bile acids initiate liver injury remain controversial. In this chapter, we summarize recent advances in the pathogenesis of bile acid induced liver injury. These include bile acid signaling pathways in hepatocytes as well as the response of cholangiocytes and innate immune cells in the liver in both patients with cholestasis and cholestatic animal models. We focus on how bile acids trigger the production of molecular mediators of neutrophil recruitment and the role of the inflammatory response in this pathological process. These advances point to a number of novel targets where drugs might be judged to be effective therapies for cholestatic liver injury. [ABSTRACT FROM AUTHOR]

Published

2017

15. Hepatic NFAT signaling regulates the expression of inflammatory cytokines in cholestasis.

Author

Cai, Shi-Ying, Yu, Dongke, Soroka, Carol J., Wang, Jing, and Boyer, James L.

Subjects

*NUCLEAR factor of activated T-cells, *BILIARY atresia, *BILE ducts, *CHOLESTASIS, *BILE acids

Abstract

The nuclear factor of activated T-cells (NFAT) plays an important role in immune responses by regulating the expression of inflammatory genes. However, it is not known whether NFAT plays any role in the bile acid (BA)-induced hepatic inflammatory response. Thus, we aimed to examine the functional role of NFATc3 in cholestatic liver injury in mice and humans. Gene and protein expression and cellular localization were assessed in primary hepatocyte cultures (mouse and human) and cholestatic liver tissues (murine models and patients with primary biliary cholangitis [PBC] or primary sclerosing cholangitis [PSC]) by quantitative PCR, western blot and immunohistochemistry. Specific NFAT inhibitors were used in vivo and in vitro. Gene reporter assays and ChIP-PCR were used to determine promoter activity. NFAT isoforms c1 and c3 were expressed in human and mouse hepatocytes. When treated with cholestatic levels of BAs, nuclear translocation of NFATc3 was increased in both human and mouse hepatocytes and was associated with elevated mRNA levels of IL-8 , CXCL2 , and CXCL10 in these cells. Blocking NFAT activation with pathway-specific inhibitors or knocking down Nfatc3 expression significantly decreased BA-driven induction of these cytokines in mouse hepatocytes. Nuclear expression of NFATc3/Nfatc3 protein was increased in cholestatic livers, both in mouse models (bile duct ligation or Abcb4 -/- mice) and in patients with PBC and PSC in association with elevated tissue levels of Cxcl2 (mice) or IL-8 (humans). Gene reporter assays and ChIP-PCR demonstrated that the NFAT response element in the IL-8 promoter played a key role in BA-induced human IL-8 expression. Finally, blocking NFAT activation in vivo in Abcb4 -/- mice reduced cholestatic liver injury. NFAT plays an important role in BA-stimulated hepatic cytokine expression in cholestasis. Blocking hepatic NFAT activation may reduce cholestatic liver injury in humans. Bile acid induces liver injury by stimulating the expression of inflammatory genes in hepatocytes through activation of the transcription factor NFAT. Blocking this activation in vitro (in hepatocyte cultures) and in vivo (in cholestatic mice) decreased the expression of inflammatory genes and reduced liver injury. • Bile acids activate the transcription factor NFATc3 in mouse and human hepatocytes. • This activation increases the expression of inflammatory genes in hepatocytes. • Increased nuclear expression of NFATc3 expression is also seen in cholestatic livers. • Blocking this activation reduced cholestatic liver injury in mice. [ABSTRACT FROM AUTHOR]

Published

2021

16. NHERF-1 Binds to Mrp2 and Regulates Hepatic Mrp2 Expression and Function.

Author

Man Li, Wen Wang, Soroka, Carol J., Mennone, Albert, Harry, Kathy, Weinman, Edward J., and Boyer, James L.

Subjects

*PROTEIN binding, *MULTIDRUG resistance, *ADENOSINE triphosphate, *LIVER cells, *BILE acids

Abstract

Multidrug resistance-associated protein 2 (Mrp2, Abcc2) is an ATP-binding cassette transporter localized at the canalicular membrane of hepatocytes that plays an important role in bile formation and detoxification. Prior in vitro studies suggest that Mrp2 can bind to Na+/H+ exchanger regulatory factor 1 (NHERF-1), a PDZ protein that cross-links membrane proteins to actin filaments. However the role of NHERF-1 in the expression and functional regulation of Mrp2 remains largely unknown. Here we examine the interaction of Mrp2 and NHERF-1 and its physiological significance in HEK293 cells and NHERF-1 knock-out mice. Mrp2 co-precipitated with NHERF-1 in co-transfected HEK293 cells, an interaction that required the PDZ-binding motif of Mrp2. In NHERF-1-/- mouse liver, Mrp2 mRNA was unchanged but Mrp2 protein was reduced in whole cell lysates and membrane-enriched fractions to ~50%(p< 1 x 10-6) and ~70% (p < 0.05), respectively, compared with wild-type mice, suggesting that the down-regulation of Mrp2 expression was caused by post-transcriptional events. Mrp2 remained localized at the apical/canalicular membrane of NHERF-1-/- mouse hepatocytes, although its immunofluorescent labeling was noticeably weaker. Bile flow in NHERF-1-/- mice was reduced to ~70% (p < 0.001) in association with a 50% reduction in glutathione excretion (p < 0.05) and a 60% reduction in glutathione-methylfluorescein (GS-MF) excretion in isolated mouse hepatocyte (p < 0.01). Bile acid and bilirubin excretion remained unchanged compared with wildtype mice. These findings strongly suggest that NH ERF-1 binds to Mrp2, and plays a critical role in the canalicular expression of Mrp2 and its function as a determinant of glutathione-dependent, bile acid-independent bile flow. [ABSTRACT FROM AUTHOR]

Published

2010

17. Multidrug resistance-associated protein 4 is up-regulated in liver but down-regulated in kidney in obstructive cholestasis in the rat

Author

Denk, Gerald U., Soroka, Carol J., Takeyama, Yasuaki, Chen, Wen-Sheng, Schuetz, John D., and Boyer, James L.

Subjects

*ADENOSINE monophosphate, *CYCLIC nucleotides, *MULTIDRUG resistance, *BILE ducts

Abstract

: Background/AimsMultidrug resistance-associated protein 4 (Mrp4, ABCC4) transports cyclic nucleotides, anti-retroviral compounds, and sulfated bile acids. Mrp4 expression is increased in farnesyl/bile acid receptor knockout mice. Our aim was to investigate Mrp4 expression and function in rat liver and kidney in obstructive cholestasis.: MethodsMale Sprague–Dawley rats were subjected to bile duct ligation (BDL) or sham-surgery. Animals were sacrificed after 3, 7, and 14 days and tissues were harvested for Western blot analysis, real-time reverse transcriptase-mediated polymerase chain reaction (RT-PCR), and immunohistochemistry.: ResultsWestern blot analysis revealed a progressive, more than seven-fold increase (P<0.05) of Mrp4 expression in cholestatic livers, 14 days after BDL. In contrast, Mrp4 in 14-day BDL kidneys decreased to 26±4% of controls (P<0.005). Immunohistochemistry localized Mrp4 to the basolateral hepatocyte membrane and corroborated its hepatic up-regulation after BDL. Real-time RT-PCR demonstrated no major changes of Mrp4 mRNA levels in liver and kidney after BDL. Cyclic adenosine monophosphate, an MRP4 substrate, was increased in plasma and urine, consistent with these findings.: ConclusionsObstructive cholestasis in rats results in progressive up-regulation of Mrp4 protein in liver but down-regulation in kidney. The absence of corresponding changes in Mrp4 mRNA suggests posttranscriptional mechanisms as predominant regulators of Mrp4 expression in BDL rats. [Copyright &y& Elsevier]

Published

2004

18. Down-regulation of the Na+/taurocholate cotransporting polypeptide during pregnancy in the rat

Author

Arrese, Marco, Trauner, Michael, Ananthanarayanan, Meenakshisundaram, Pizarro, Margarita, Solıs, Nancy, Accatino, Luigi, Soroka, Carol, Boyer, James L., Karpen, Saul J., Miquel, Juan Francisco, and Suchy, Frederick J.

Subjects

*BILE acids, *CARRIER proteins

Abstract

Background: Experimental studies have shown decreased bile acid (BA) uptake and reduced excretion of cholephilic compounds in pregnant rodents.Aim: To assess the expression and function of the main BA importer, the Na+/taurocholate cotransporting polypeptide (Ntcp) in pregnant rats.Methods: BA uptake and Ntcp expression were studied in control and timed-pregnant rats in late gestation. Ntcp protein, messenger RNA (mRNA) expression, and Ntcp tissue localization were determined by Northern blotting, Western analysis, and tissue immunofluorescence. The activity of three transactivators of the Ntcp promoter: hepatocyte nuclear factor 1-α (HNF1-α), nuclear receptor heterodimer retinoid X receptor:retinoid acid receptor (RXR:RAR) and signal transducer and activator of transcription 5 (Stat5) was assessed using gel electrophoretic mobility shift assays.Results: A significantly reduced BA uptake and decreased Ntcp mRNA levels (−40%) and protein mass (−60%) was observed in pregnant rats. Nuclear extracts from pregnant rats showed a marked decrease of HNF1-α and RXR:RAR binding activities by −80 and −40% of basal activity, respectively. In contrast, binding activity of Stat-5 was increased by 50% in nuclear extracts from pregnant rats.Conclusions: Pregnancy is associated with reduced Ntcp expression and function in the rat. Our findings suggest that Ntcp down-regulation during pregnancy occurs primarily at the transcriptional level. [Copyright &y& Elsevier]

Published

2003